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Thanks to our network of collaborators who help us promote open science.
By supporting an open access policy, we facilitate the rapid and free exchange of scientific ideas, ensuring that the research we fund can be leveraged for future discoveries.
The Aligning Science Across Parkinson’s (ASAP) initiative is devoted to accelerating the pace of discovery and informing the path to a cure for Parkinson’s disease through collaboration, research-enabling resources, and data sharing.
Fund international multidisciplinary teams to encourage the exchange of ideas, foster innovation, and catalyze new experimental approaches.
Build infrastructure to support the next generation of Parkinson’s research through genetic analysis efforts, training support, natural history studies, and other research tools.
Implement open science policies to ensure that ASAP-funded research, outputs, and tools can be leveraged by the broader community.
Learn about the work of the fourteen awarded teams.
The research discoveries largely centered around 4 categories:
Dysfunction of selective autophagic mechanisms have been directly linked to PD. ASAP teams published articles that centered on understanding autophagosome biogenesis, elongation, and downstream mechanisms, with specific insights on mitophagy and lysophagy.
Protein aggregation has been implicated in the progression of neurodegenerative disorders, such as PD. Focusing specifically on the proteins alpha-synuclein and tau, ASAP teams explored how protein aggregation begins and how it can be hindered or enhanced.
LRRK2 mutations are the most common genetic causes for PD. ASAP teams focused on understanding the LRRK2 interactome and how LRRK2 mutations impact downstream signaling pathways.
Diseases are often complex and multi-systemic, and as such can have shared pathophysiology. ASAP teams explored PD in the context of other diseases and created tools to better evaluate risk loci.
By supporting an Open Science policy, we facilitate the rapid and free exchange of scientific ideas, ensuring that the research we fund can be leveraged for future discoveries. Our guiding principles are modified from the Panton Principles for Open Data in Science. We believe that:
ASAP is guided by the belief that research outcomes will be improved through the following principles:
Given the multifactorial nature of Parkinson’s disease, charting a new path will require multidisciplinary cooperation from investigators with and without a previous record of PD research.
Philanthropic capital has the most impact in areas that are deemed unpopular, high-risk, or out-of-scope for government funding, requiring creative and thoughtful consideration of research.
As roadmap goals are implemented, we will be responsive to the evolving nature of research and adjust focus as deemed appropriate.
To accelerate research, we’ll support the free flow of data and resources within our collaborative network and make findings available to the broader community.
The ASAP-sponsored video series, Discover ASAP, highlights top findings and tools connected to our ASAP network, including datasets, code & software, protocols, and lab materials. Featured videos include interviews of authors, grantees, and key opinion leaders in Parkinson’s research.
Discover ASAP is designed to further the spread of knowledge and enhance equity across the scientific community by promoting transparent research practices. We are excited to share these interviews and videos with the research community, in hopes that they will help to accelerate discoveries for Parkinson’s disease.
Watch Discover ASAP videos. You can receive notifications when there are new interviews to watch. Subscribe to ASAP’s YouTube channel.
We’re enabling science to go further, faster, and at a greater scale. Follow @ASAP_Research across our social media channels and join our mailing list for exciting updates as our work matures.
Sign up for updates here.
Huw Morris leads the Cohort Integration working group (CIWG). In this blog post, Huw provides an outline of the research on Parkinson’s disease over the last 25 years and shares the plans of the CIWG to harmonize clinical data from research participants to enable large clinical outcomes research.
As a follow-up to the last blog post on Understanding GWAS, the GP2 Complex Disease Data Analysis Working Group has provided practical tips and insights for running your own GWAS.
Adding a layer of compute to connect two massive datasets is where we are headed. Mike Nalls, Hampton Leonard, Matt Bookman, and Eline Appelmans outline the partnership between The Global Parkinson’s Genetics Program (GP2) and Accelerating Medicines Partnership: Parkinson's Disease (AMP PD) to be your one-stop shop for PD genetic and genomic data in this new blog post.
Members of the GP2 Operations and Compliance working group provide an overview of what compliance is and why it is important in GP2.
Members of the GP2 Complex Disease Data Analysis working group provide an overview of Genome-Wide Association Studies (GWAS), including statistical formulae, workflows, and examples from the most recent Parkinson’s disease GWAS.
Christine Klein leads the GP2 Monogenic Hub. In this post Christine shares how her interest in Parkinson’s disease genetics was sparked, which genes have been discovered so far, and the questions which are still to be answered.
The ASAP Collaborative Research Network is an international, multidisciplinary, and multi-institutional network of 35 teams working to address research and knowledge gaps in the development and progression of PD.
ASAP is launching a new video series, Discover ASAP, which highlights interviews of authors, grantees, and key opinion leaders in Parkinson’s research discussing top findings and tools connected to our ASAP network.
ASAP is announcing two open competitive funding opportunities for the research community. These new grants will provide additional capital to spur discovery and inform the path to a cure for Parkinson’s disease research.
Aligning Science Across Parkinson’s (ASAP) is pleased to share the impact that our initiative, network, and supported programs have had on providing new insights into Parkinson’s disease (PD) while offering opportunities to collaborate, generate resources, and share data. Together, we are uncovering novel discoveries and making progress toward our vision of advancing collaborative, transparent research processes and environments that deliver faster and better outcomes in PD research.
The ASAP Collaborative Research Network (CRN) continues to expand, attracting new investigators across multiple disciplines, institutions, career stages, and geographies. Working together, the CRN addresses gaps in the development and progression of Parkinson’s disease. This year, we welcome 14 new research teams who will focus their work on circuitry and brain-body interactions.
The effect of genetic alterations on disease biology
The molecular and cellular contributions of the neuro-immune system
The underlying neuronal circuit dynamics and interface with the periphery
The role of heredity, neuro-immune factors, and circuit-level alterations on disease progression
The cause is unknown; however, there are a number of known risk factors. Men are 50 percent more likely than women to develop Parkinson’s disease; exposure to pesticides and other toxins increases risk. Head trauma and depression are also thought to increase a person’s chances of developing Parkinson’s disease. A number of recently discovered genetic risk variants are reported to increase a person’s risk as well – these may prove scientifically useful in identifying the underlying mechanisms of Parkinson’s disease.
Although there are some therapies that help with the symptoms of Parkinson’s disease, none can address the underlying cause of the disease. Levodopa is a drug that replaces dopamine, the main chemical produced by the neurons that Parkinson’s disease attacks. However, its effect tends to wear off after four to seven years and can cause unwanted side effects. Other drug treatments try to mimic the action of dopamine, protect it from breakdown or preserve motor function through other molecular pathways. And for some people with Parkinson’s disease, surgically implanted electrodes can relieve symptoms.
Because we currently have little understanding of how Parkinson’s disease starts and progresses, the challenge of developing a disease-modifying drug is formidable. Researchers and clinicians lack a reliable diagnostic or biomarkers that can be used to determine whether a candidate drug affects disease progression at a cellular level.
Aligning Science Across Parkinson’s (ASAP) is fostering collaboration and resources to better understand the underlying causes of Parkinson’s disease. With scale, transparency, and open access data sharing, we believe we can accelerate the pace of discovery, and inform the path to a cure.
From 2020 to 2024, the ASAP CRN supported 35 multidisciplinary, international teams across 14 countries. See how the CRN has accelerated breakthroughs in PD research through collaboration and open science.
In this blog, ASAP highlights its transformation since its inception and shares insight into new programs and discoveries.
ASAP’s 2025 Collaborative Meeting welcomed representatives from our 35 CRN teams to share impactful findings on the PD landscape, promote the cross-fertilization of ideas, and provide opportunities to engage the broader CRN across different levels of training.
Meet the new members of ASAP’s Collaborative Research Network. Multidisciplinary investigators in 21 teams from 60 institutions across 11 countries, seek to accelerate targeted basic research and move us toward more meaningful advancements for Parkinson’s Disease. Get to know these talented scientists, their projects and how their outcomes will contribute to the field of PD.
GP2’s new online learning platform makes development opportunities accessible and enables learners from around the world to explore courses on topics related to Parkinson’s disease genetics and a range of related areas. It is easy to register and available to everyone interested.
Collaborative and transparent research processes and environments that deliver faster and better outcomes for Parkinson’s disease.
Accelerating the pace of discovery and informing the path to a cure for Parkinson’s disease through collaboration, research-enabling resources, and data sharing.
Human genetics and epidemiological studies are valuable tools for understanding Parkinson’s disease, but research has found that known genetic factors identified in European populations play an insignificant role in the development of PD in Latinos. LARGE-PD, an ASAP partner and multicenter collaboration across Latin America, is working to increase Latino and Hispanic representation in this field of research. Read GP2’s latest blog post.
The Aligning Science Across Parkinson’s (ASAP) initiative invites applications from collaborative teams to join the ASAP Collaborative Research Network (CRN), an international, multidisciplinary, multi-institutional network of research teams working to address high-priority research questions in an effort to advance our understanding of Parkinson’s disease (PD) and drive new ideas into the R&D pipeline. For this cycle, applications within the Scientific Track that focus on dissecting the mechanisms that contribute to PD heterogeneity will be considered in six key focus areas.
We’re enabling science to go further, faster, and at a greater scale. Join us to receive updates.
iNDI-PD has developed tools and research outputs that can be utilized by the scientific community to support research endeavors. To learn more about iNDI-PD outputs visit the ASAP Catalog, which lists the publicly available, ASAP-funded research outputs produced through the ASAP initiative.
CLN5
GBA1LP
PARK7/DJ1
STING1
CLU
GPNMB
PGK1
SYNJ1
CTSB
HLA-DRB5
PLA2G15
TREM2
DNAJC6
ITSN1
PSMF1
USP30
FBXO7
LRP1
RIMS2
VPS13C
Study Rationale: Genetic mutations that lead to the activation of the enzyme LRRK2 are a major cause of inherited Parkinson’s disease. Team Alessi aims to combine the complementary expertise of its four research laboratories to perform fundamental, state-of-the-art experimentation to better comprehend the biology that is controlled by LRRK2. Team Alessi’s goal is to gain a much better understanding of LRRK2-driven Parkinson’s disease, hopefully providing a foundation for the development of future therapies.
Hypothesis: LRRK2 targets and modifies a set of enzymes known as Rab GTPases, triggering new biological events by creating new protein: protein interactions. Team Alessi aims to decipher what controls the activity of LRRK2 and to explore, in precise molecular detail, how this enzyme affects three major cellular structures (cilia, lysosomes, and mitochondria) implicated in Parkinson’s disease.
Study Design: Team Alessi showed that mutant LRRK2 triggers a series of molecular changes that cause new sets of proteins to interact. Team Alessi’s goal is to use a combination of state-of-the-art approaches to understand the consequences of these new interactions on the biology of three important subcellular compartments: primary cilia, lysosomes, and mitochondria.
Impact on Diagnosis/Treatment of Parkinson’s Disease: Team Alessi’s findings will provide novel, fundamental information of relevance to understanding the origin and progression of Parkinson’s that they hope will lead to new ideas to better diagnose, treat, and even prevent this malady in the future.
The project will provide fundamental information regarding how mutations in LRRK2 cause Parkinson's disease. View Team Outcomes.
Study Rationale: Geneticists have made great progress in identifying gene mutations that either cause Parkinson’s or increase disease risk. The critical next step is to determine how some of these mutations perturb the function of brain cells involved in Parkinson’s disease. By advancing knowledge of these processes, Team De Camilli’s research will help to identify new opportunities for reversing the vulnerabilities that cause the disease.
Hypothesis: Team De Camilli hypothesizes that the functions of multiple Parkinson’s disease genes converge on common biochemical pathways involving endocytic organelles and/or mitochondria within vulnerable cell types.
Study Design: Team De Camilli will use a comprehensive cell biology tool kit including cutting-edge biochemistry, structural biology, microscopy at different scales, and genome editing tools to elucidate the function of selected Parkinson’s disease genes and the effects produced by their dysfunction both in cellular models in vitro and in mouse and rat models. By defining the molecular and cellular networks in which the products of these genes operate, Team De Camilli hopes to identify strategies for reversing the cellular vulnerabilities that cause Parkinson’s disease or increase disease risk.
Impact on Diagnosis/Treatment of Parkinson’s Disease: Similar to assembling the pieces of a puzzle, the project has the potential to reveal interconnections between the functions of distinct Parkinson’s disease genes, thus helping to build an understanding of Parkinson’s disease cell biology. This is a critical step towards the development of therapeutic strategies to make neurons resistant to the dysfunctions that cause Parkinson’s disease.
The project hopes to reveal interconnections between the functions of distinct Parkinson’s disease genes, thus helping to identify cellular processes whose dysfunction confers Parkinson’s disease vulnerability and which may be targeted for therapeutic intervention. View Team Outcomes.
Study Rationale: The progression of Parkinson’s disease is very variable, with some individuals having a rapid course and others having a longer and more benign course. Team Hardy believes that by understanding the genetics and the mechanistic basis of this variability, they will be able to design therapies to slow Parkinson’s progression. Team Hardy has already found that GBA mutations lead to a rapid disease course and that LRRK2, linked to familial forms of Parkinson’s, influences the course of parkinsonism in another disease: progressive supranuclear palsy. They will test whether modulating these enzymes influences the course of pathology spread in a pre-clinical model of progression as a validation of this approach to disease treatment.
Hypothesis: Team Hardy wants to find and understand the genes that are involved in Parkinson’s progression and test whether modulating them pharmacologically influences disease progression.
Study Design: Through genetic analysis, Team Hardy will find genes that influence the progression of parkinsonism, and then assess the mechanisms by which they affect disease development. They have already found that GBA and LRRK2 influence clinical rates of decline so Team Hardy will test, in a mouse model of pathology progression, whether inhibiting these enzymes influences pathology spread and thereby develop a relevant platform to test drugs for slowing disease progression.
Impact on Diagnosis/Treatment of Parkinson’s Disease: This research will impact Parkinson’s care in three ways. First, by understanding the genetics of rate of decline, these data can be factored into clinical trial design and possibly more generally into clinical practice. Second, the identification of pathways involved in disease progression is likely to reveal further drug targets. And thirdly, the testing of GBA and LRRK2 inhibitors in a mouse model of disease progression will test this as a valid approach to treatment development.
Team Hardy will dissect the genetic and gene expression variability underlying differences in the rate of decline inherent in PD and move towards therapies which slow this decline. View Team Outcomes.
Study Rationale: Abnormal protein aggregation and prion-like aggregate spreading are hallmarks of the degenerative cascades of sporadic and familial Parkinson’s disease (PD) and can damage cells, including neurons. Multiple mechanisms of aggregate toxicity have been implicated in cellular PD pathology, and PD risk alleles may have the potential to illuminate additional underlying biological mechanisms.
Hypothesis: Parkinson’s disease, at the molecular level, results from the failure of cellular quality control (QC) mechanisms, and finding ways to maintain (or augment) QC capacity will provide new therapeutic strategies for PD and possibly other neurodegenerative disorders.
Study Design: Using powerful molecular visualization and discovery tools in disease-relevant cells, Team Harper will elucidate how individual types of protein aggregates linked with PD strains (including patient-derived aggregates) alter cellular pathways, including effects on cell survival and function. Team Harper will also use genetic approaches to understand what cellular proteins promote the processing of PD-related aggregates.
Impact on Diagnosis/Treatment of Parkinson’s Disease: Team Harper’s expectation is that this work will identify those critical cellular functions that are disrupted by protein aggregates and will help define how mutations alter the underlying mechanisms of dysfunctional proteostasis.
Through biochemical reconstitution, in situ structural analysis, and genetic perturbations, this project will directly visualize pathogenic mechanisms in cells and in reconstituted systems at nanometer and subnanometer resolution, providing an unprecedented understanding of how a-synuclein strains and other PD mutants promote cellular dysfunction. View Team Outcomes.
Study Rationale: Mitochondria are tiny power-generating stations within all cells, including neurons. They are vital energy producers, but when things go wrong, they can spew toxic materials and sicken or kill neurons. The clean-up crew for mitochondria gone wrong is called “mitophagy” (as in “eating mitochondria”) and is directed by two proteins called PINK1 and parkin. Studies of Parkinson’s disease have taught researchers that PINK1, parkin and mitophagy are very important in preventing disease.
Hypothesis: The purpose of this project is to figure out how PINK1, parkin and mitophagy work together to prevent disease. Once Team Hurley knows how they work together, they hope to figure out how to make them work faster and better, so that they can prevent Parkinson’s disease from ever starting.
Study Design: Team Hurley thinks of PINK1, parkin and the proteins of mitophagy as nanomachines. They call their type of research “mechanistic” because it seeks to understand how these machines work. Team Hurley relies heavily on the most powerful light and electron microscopes available, and they also use genome engineering of stem cells to make versions of neurons that are easier to study.
Impact on Diagnosis/Treatment of Parkinson’s Disease: Team Hurley’s dream is to understand PINK1, parkin, and mitophagy so well that they can build a computerized description of the pathway that will be able to predict which drugs and treatments will help the mitochondrial clean-up crew enough to prevent or cure disease.
If successful, the project will provide a therapeutically actionable basis for where and how mitophagy can best be activated to promote the health and longevity of the dopaminergic neurons affected in Parkinson's Disease. View Team Outcomes.
Study Rationale: Several genes are known to be associated with Parkinson’s disease, although how they impact the disease process is not fully understood. Team Kirik will use stem cells from patients in whom the genetic cause is known and perform mechanistic studies to elucidate the interactions between three key genes and how they impact the function of cells in the brain.
Hypothesis: This project will provide new insights into the role specific gene mutations play in the development of disease features in cell types known to be affected in Parkinson’s disease.
Study Design: Stem cells generated from patients with neurological disease, including Parkinson’s disease, provide a tool for researchers to study and understand mechanisms underlying the disease. One limitation of this approach is that the cells are maintained in culture dishes in the laboratory in an artificial environment that does not closely model that of the disease. This project proposes a unique approach involving the transplantation of the human cells into mice in order to study them in the living brain and thus reveal new insights into disease mechanisms.
Impact on Diagnosis/Treatment of Parkinson’s Disease: Researchers’ ability to design better treatments for Parkinson’s is directly related to the level of understanding on the basic biological processes governing the initiation of the disease process and how the disease progresses from that point onward. This information is critical in efforts to intervene with the disease process.
This project will use patient-derived cells from genetic forms of PD, studied in the environment of the living brain, as a unique paradigm to reveal cellular components of PD pathobiology. View Team Outcomes.
Study Rationale: While aging is the greatest risk factor for the development of Parkinson’s disease (PD), how aging promotes PD is not fully understood. Examining the role of cellular senescence (deterioration of function), a major driver of aging, in PD represents a completely novel approach to understanding disease pathophysiology and may lead to new therapeutic approaches.
Hypothesis: Senescence and PD-linked gene mutations have reciprocal pathological interactions where (i) senescence causes PD-relevant neuropathology; (ii) PD-linked mutant genes (alpha-synuclein, LRRK2, Vps35) cause premature senescence; and (iii) senescence participates in neuropathology caused by PD-linked genes.
Study Design: First, Team Lee will use novel mouse models of premature senescence to test whether premature senescence in specific cell types causes PD-like neuropathology. Second, they will combine mouse models of senescence and familial PD to test whether senescence participates in neuropathology caused by mutant PD-linked genes. Specifically, Team Lee will determine if pathology in a PD mouse model causes premature senescence and whether removing senescent cells from brain can prevent PD pathology. Finally, Team Lee will perform gene expression analysis of PD brains and mouse brains, at a single-cell level, to gain high-resolution insights about cellular processes that link aging and PD pathology.
Impact on Diagnosis/Treatment of Parkinson’s Disease: Team Lee’s results will support the use of senolytics (drugs that selectively kill senescent cells and are currently in Phase II clinical trials) as novel disease-modifying therapies for PD. In addition, Team Lee’s studies may identify new biomarkers of senescence in PD.
This project will determine if cellular senescence is a pathogenic component of Parkinson’s disease and test if drugs targeting senescent cells can be used as a disease-modifying therapy for PD. View Team Outcomes.
Study Rationale: Leucine Rich Repeat Kinase 2 (LRRK2) is the most commonly mutated gene in inherited forms of Parkinson’s disease (PD). The LRRK2 gene codes for a protein kinase, an enzyme that adds chemical groups to other proteins to change their activity inside cells. However, researchers currently do not understand how LRRK2 normally works and why its malfunction causes PD. Importantly, LRRK2 has also been shown to function abnormally in PD patients that have the sporadic form of the disease, making LRRK2 one of the most promising targets for drug development.
Hypothesis: Team Reck-Peterson recently discovered that chains of the LRRK2 protein can wrap around cellular highways called “microtubules”. Their work suggests that LRRK2 blocks the cellular machines that move on these highways. Team Reck-Peterson will explore the idea that mutations in LRRK2 cause PD by acting as roadblocks that change the normal transport of chemical information inside cells. They will test additional ideas that arise from the experiments they perform.
Study Design: The collaborative team includes experts in cryo-electron microscopy (Cryo-EM), cryo-electron tomography (Cryo-ET), small molecule synthesis, proteomics, and single-molecule and live-cell imaging. The team will use their expertise to solve structures of multiple conformations and variants of LRRK2 to manipulate these different pools of LRRK2 and understand their cellular functions. Team Reck-Peterson will determine how LRRK2 binds to microtubules and affects microtubule-based motors. They will also identify the protein interaction landscape of LRRK2 and test emergent cellular hypotheses resulting from this work, including whether LRRK2 regulates the transport of chemical information on microtubules.
Impact on Diagnosis/Treatment of Parkinson’s Disease: A major barrier to developing LRRK2-based PD therapy has been the lack of a blueprint of LRRK2’s three-dimensional shape, alone or interacting with other molecules it comes into contact with inside human cells. Team Reck-Peterson expects that the work will reveal what LRRK2 looks like, what it does in cells, and why its malfunction causes PD. The work will be critical for the design of drugs targeting LRRK2.
Team Reck-Peterson's work on LRRK2 will provide a comprehensive understanding of the structure and conformation-dependent association with cellular partners of this key target for the development of Parkinson’s disease therapeutics. View Team Outcomes.
Study Rationale: Parkinson’s disease can have multiple complex causes, including genetic and environmental, that are not fully understood. Team Rio will combine modern genetic and human stem cell-based approaches to determine how heritable genetic changes affect Parkinson’s disease predisposition. By identifying how even small genetic changes can compound the risk of developing Parkinson’s disease, Team Rio hopes to identify new ways to detect and treat the disease in the future.
Hypothesis: Team Rio hypothesizes that combining complex human cell culture models such as 3-dimensional brain organoids with sophisticated genome-scale functional analysis will allow the team to elucidate how diverse genetic factors interact and contribute to the risk of developing Parkinson’s disease, thereby informing the development of early detection diagnostics and advanced treatment options.
Study Design: Team Rio will genetically engineer human embryonic stem cells to model the genetic alterations known to increase risk for Parkinson’s disease and turn those cells into disease-relevant cell types such as dopamine neurons. By profiling the gene expression changes caused by these known Parkinson’s disease risk variants, the team will decipher the key molecular signatures that contribute to Parkinson’s disease. Once identified, the team will confirm these genetic signatures in patient samples and validate their effects in animal models.
Impact on Diagnosis/Treatment of Parkinson’s Disease: Elucidating how Parkinson’s disease genetic risk variants affect cell biology has promise to identify disease-specific biomarkers and novel treatment options.
This project uses state-of-the-art functional genomics approaches to identify gene expression and RNA splicing signatures that may lead to the development of novel pharmacological interventions for Parkinson’s disease or biomarkers for early diagnosis and disease progression. View Team Outcomes.
Study Rationale: Genome-wide association studies (GWAS) have unequivocally linked thousands of noncoding variants in ninety independent GWAS signals to susceptibility for common, genetically complex Parkinson’s disease (PD) that affects more than 7 million people around the world. Why have these breakthroughs not uncovered the mechanism(s) of PD? Researchers do not know how disease-associated variants cause neurodegeneration and why they impair some brain cells but not others. Team Scherzer’s research will tackle the critical task of clarifying the precise mechanisms through which this wealth of genetic variation regulates onset and progression of PD.
Hypothesis: Team Scherzer hypothesizes that most GWAS variants function through cell-, space-, and stage-dependent gene-regulatory mechanisms.
Study Design: Here Team Scherzer will develop a molecular atlas of PD that reveals how GWAS/familial genetics control proximal disease mechanisms in five dimensions: brain cells (1D), brain space (3D), and disease stage (1D). The team will reveal how genetic variants modulate mechanisms in specific brain cells in specific topographic locations of midbrain and cortex during the progression of neuropathology from healthy brains to prodromal to symptomatic disease. Massively parallel analysis of hundreds of thousands of single human brain cells with genetic transcriptomics, high-resolution spatial transcriptomics, and fine-mapping of causal alleles with allelic imbalance in human brains will be combined with the prodigious power of cell- and stage-specific mechanistic analyses in brain of Drosophila avatars and in vitro in human pluripotent stem cells.
Impact on Diagnosis/Treatment of Parkinson’s Disease: Team Scherzer’s collaborative and integrative project will translate the complex human genetics of PD into a dynamic, five-dimensional view of proximal cellular mechanisms. It will begin to reveal how single nucleotide variation in a person’s universal DNA code regulates gene activity (without changing protein sequence) in situ in billions of physiologically specialized neurons and glia cells, and determines, how, when, which, and where brain cells are destined to malfunction.
Parkinson5D will translate the complex human genetics of Parkinson’s disease into a dynamic, spatiotemporal understanding of proximal mechanisms in specific brain cells --- in situ in patients’ brains, in vivo in Drosophila, and in vitro using human pluripotent stem cell genetics. It will begin to reveal how single nucleotide variation in a person’s universal DNA code regulates gene activity in situ in billions of physiologically specialized neurons and glia cells, and determines, how, when, which, and where brain cells are destined to malfunction. View Team Outcomes.
Study Rationale: Why do some people develop Parkinson’s disease (PD) while others do not? Although many genetic risk factors have been identified, researchers still cannot confidently answer this question, or explain how certain cells in the brain go from being healthy early in life to diseased in old age. Clearly, numerous complex factors are involved, and a systematic investigation of the key cellular and molecular players is necessary to understand and effectively treat this disease.
Hypothesis: Team Studer hypothesizes that single genetic factors are insufficient to cause PD — rather, that it is triggered by a combination of genetics, age-related factors, and their effects in different brain cells.
Study Design: Here, Team Studer proposes to dissect the genetic, age-related, and cell-type-specific factors that lead to PD using a collection of genetically diverse stem cells derived from patients. Using advanced methods pioneered by the team, they will convert these stem cells into the different types of brain cells implicated in PD — neurons, microglia, and astrocytes — allowing the team to investigate how genetic risk factors, the aging process, and these different cell types interact to trigger disease. Team Studer will assess how various combinations of these factors disrupt the function of brain cells using detailed molecular studies, microscopy, genetic manipulations, and biochemical measurements — building a computational network model of the factors that cause PD.
Impact on Diagnosis/Treatment of Parkinson’s Disease: This richer, fully human cell model of PD will provide an entirely new level of understanding of how the interplay between genetics, different brain cells, and aging shapes individual disease risk, enabling early diagnosis, prediction of therapeutic targets that could halt or reverse the disease, and stratification of patients into therapeutically meaningful subgroups.
The project will not only help address the question of variable penetrance — why some individuals with genetic risk factors develop Parkinson’s disease while others do not — but may also lead to improved tools for early diagnosis, prediction of effective therapeutic targets, and stratification of patients into therapeutically meaningful subgroups. View Team Outcomes.
Study Rationale: Mutations in the genes ATP13A2 (PARK9) and ATP10B trigger Parkinson’s disease (PD) and cause dysfunction of lysosomes, the recycling compartments of the cell. Team Vangheluwe explained these defects by impaired transport of polyamines and glucosylceramide out of the lysosome, respectively. Polyamines are cell protective agents, whereas the levels of the lipid glucosylceramide are controlled by GBA1, the major genetic risk factor of PD. However, there is a clear knowledge gap regarding the biology of polyamine and glucosylceramide transport systems in neurons and their supporting cells of the brain, and how an impaired polyamine and glucosylceramide distribution in these cells leads to neurodegeneration.
Hypothesis: Team Vangheluwe hypothesizes that an impaired polyamine and glucosylceramide transport activity causes toxic accumulation of these substances in lysosomes and leads to a shortage elsewhere in the cell. Together, this may cause lysosomal and mitochondrial dysfunction, and lead to α-synuclein toxicity, three major hallmarks of PD.
Study Design: First, Team Vangheluwe will investigate the molecular architecture of polyamine and glucosylceramide transporters and identify mechanisms to modulate their activity. Second, the team will examine how these transporters influence the intracellular distribution of polyamine and glucosylceramide, and how this affects the cross-talk between lysosomes and mitochondria. Third, they will investigate how dysfunctional polyamine and glucosylceramide transporters affect other PD pathways, such as mitophagy, GBA1 and alpha-synuclein aggregation, and whether the modulation of these transporters can be validated as therapeutic approach for PD. Finally, Team Vangheluwe will collect evidence for disturbed polyamine and glucosylceramide transport in PD patients.
Impact on Diagnosis/Treatment of Parkinson’s Disease: Team Vangheluwe will validate the neuroprotective effect of polyamine and glucosylceramide transporters and investigate their potential to reverse α-synuclein and GBA1 pathology. This may offer new therapeutic strategies that correct aberrant lysosomal and mitochondrial dysfunction in Parkinson’s disease. The team will analyze whether alterations in the polyamine and glucosylceramide levels together may be considered as biomarkers for PD.
By dissecting the neuroprotective effect of lysosomal polyamine and glucosylceramide transporters at the molecular level, Team Vangheluwe will establish new pathways implicated in Parkinson’s disease that may serve as novel therapeutic targets to restore lysosomal dysfunction in Parkinson’s disease. View Team Outcomes.
Study Rationale: Parkinson’s disease (PD) is a disorder that not only affects the function of the brain, but also of the gut, which are both complex tissues composed of functionally diverse types of cells that need to cooperate for organ function. Around 90 regions of the DNA that we inherit from our parents, show differences between people with and without PD. Furthermore, as we develop and age, new, non-inherited DNA mutations may also be acquired in part of our body cells. How such inherited and newly acquired DNA variants function in increasing the risk of developing PD remains however largely unknown.
Hypothesis: Team Voet hypothesizes that these DNA variants can increase or decrease the activity of key (un)known genes in particular types of cells of the brain and the gut, which in turn increases the risk of developing PD.
Study Design: Team Voet will use the expertise of their consortium in analyzing single cells to study the brain and gut from individuals who lived with and without PD. Specifically, gene expression profiling of over 4,500,000 single cells will allow the team to discover the genes of which the expression is altered by the DNA variants, and importantly, also in which type of brain and/or gut cells the expression of the gene is disturbed. Team Voet will next analyze how these DNA variants change the functioning of these specific cell types, by using their existing models of the fruitfly, and of cultured human nerve and immune gut cells.
Impact on Diagnosis/Treatment of Parkinson’s Disease: This study will provide crucial mechanistic insights into how faults in our DNA change the functioning of specific cells in our brains and guts, and thus cause a predisposition to PD.
By disclosing the Parkinson's disease (PD)-relevant genes and cell (sub)types in the brain and gut, and the molecular mechanisms of their gene expression (dys)regulation in the normal condition, with aging and in PD, Team Voet will advance their understanding of the etiopathogenesis of the disease and pave the path for devising new treatment modalities. View Team Outcomes.
Study Rationale: To determine the molecular and cellular process that lead to PD, a powerful approach is to single out and study the cells where the disease originates. To achieve this goal, Team Wood uses alpha-synuclein oligomers as a cellular biomarker to identify the right cells. The team will then apply state-of-the-art genomic and genetic analyses to identify genes and proteins that form the disease pathways. Team Wood can then determine the difference between cause and effect by using human cell models derived from induced pluripotent stem cells.
Hypothesis: Team Wood hypothesizes that alpha-synuclein oligomers can be used as cellular biomarkers to identify the specific cells where the disease processes begin, thus making their targeted study possible.
Study Design: By detecting the presence of alpha-synuclein oligomers, Team Wood will identify neuronal and non-neuronal cells in the human brain at different stages of disease, which the team will then study using state of the art single cell genomic and transcriptomic methods. This will allow the team to build a comprehensive and detailed picture of the genes and molecular processes that underlie the disease, which the team will then prioritize using network theory and their knowledge of the current and emerging genetic factors. Using a human model system (iPSC), Team Wood will be able to distinguish cause and effect and deliver new targets for therapeutics, diagnostics, and biomarkers of disease.
Impact on Diagnosis/Treatment of Parkinson’s Disease: This interdisciplinary program, combining physical chemistry, computational modeling, genetics, and neurobiology, will allow researchers to much more fully understand the reasons behind why some cells succumb and others resist the pathological processes. Team Wood findings will offer opportunities for accurate markers of disease status, progression, and validated targets for biopharma to develop novel therapies.
Team Wood's project addresses the fundamental mechanisms underlying oligomerization of alpha-synuclein and the impact of genetic risk factors in these processes by harnessing single cell transcriptomics and genomics to delineate molecular pathways to disease. View Team Outcomes.
Study Rationale: The motor symptoms of Parkinson’s disease (PD) result from the degeneration of the dopamine-producing neurons in a brain area called the substantia nigra pars compacta (SNc). Recent findings suggest that the SNc is diverse and is comprised of dopamine neurons with distinct properties. How these dopamine neuron “subtypes” contribute to movement, how they are affected in PD, and how they are modified by deep brain stimulation (DBS) remains unknown.
Hypothesis: Team Awatramani will determine whether (a) the SNc is comprised of pro-motor and anti-motor dopamine neuron subtypes and (b) selective loss of pro-motor neurons in PD causes an imbalance in dopamine neuron subtypes that underlies the motor symptoms of PD.
Study Design: Team Awatramani will separate these neurons into their distinct genetic subtypes, which will allow the team to study their specific physiological, anatomical, and functional properties. The team will also determine the molecular and circuit mechanisms underlying the dysfunction of dopamine neurons in a mouse model of PD (LRRK2 model). Additionally, they will explore whether deep brain stimulation of dopamine neuron inputs contributes to the therapeutic efficacy of this treatment.
Impact on Diagnosis: First, Team Awatramani work will identify which dopamine neuron subtypes degenerate and which circuits are dysregulated in PD. This knowledge will be important for understanding the pattern of SNc neuron loss in PD and efficacy of DBS in patients. By using a LRRK2 model, Team Awatramani’s studies also will identify the molecular targets of the hyperactive LRRK2 enzyme, which will be critical for the optimization of LRRK2 inhibitor drugs and their application in patients.
Team Awatramani aims to provide a detailed understanding of the diverse dopamine neurons that exist in the substantia nigra in terms of their molecular signatures, unique anatomical circuits, functional contributions to motor behavior, and how this circuitry is disrupted in Parkinson's disease models. View Team Outcomes.
Study Rationale: Many people with Parkinson’s disease (PD) develop untreatable cognitive symptoms, including problems with attention, decision-making, and dementia at late stages of the disease, due to changes in a crucial part of the brain, the cerebral cortex. Evidence suggests that aggregation of the protein alpha-synuclein in vulnerable nerve cells interferes with their health and damages the cellular networks required for normal brain function. However, the relationships between alpha-synuclein, vulnerable cells, and network activity are not understood. By identifying and understanding the causes and effects of this damage in brain networks, and affected nerve cells and their connections, Team Biederer aims to enable therapies that directly target this disorder.
Hypothesis: Team Biederer hypothesizes that networks of nerve cells in the cortex of the brain become dysfunctional because of damage caused by pathological deposits of the protein alpha-synuclein in vulnerable cells.
Study Design: Team Biederer will assess how alpha-synuclein pathology progressively impairs network function in the brain cortex and identify the features distinguishing vulnerable from resilient cells using innovative technologies, including imaging of activity in the live brain, measurements of attention, profiling of different cell types and their contents, and high-resolution microscopy of neuronal connections. The team will integrate these data using advanced computational methods to design and test cell-specific interventions to restore the function of the disrupted networks. This study will reveal mechanisms of cortical network damage in Parkinson’s disease and will identify the types of nerve cells suited for therapeutic intervention.
Impact on Diagnosis: Diagnostic biomarkers for PD can leverage Team Biederer’s findings of which types of neurons, their connections, and molecular markers are most affected. For treatment, Team Biederer’s work will define novel mechanisms that can directly restore network function by targeting specific types of cortical nerve cells and their connections.
Team Biederer's project will gain mechanistic insight into PD pathology linked to progression to dementia. The team will integrate information across molecular, anatomical, and circuit domains, using mathematical modeling, to reveal and manipulate underlying cellular and network vulnerabilities in the cortex. View Team Outcomes.
Study Rationale: While neurodegeneration in Parkinson’s disease (PD) affects many cells, dopamine neurons are particularly vulnerable, and their loss drives many of the major motor difficulties in PD. To date, the inner workings of the dopamine neurons themselves have been extensively studied to identify sources for this selective vulnerability. However, neurons in the brain are heavily interconnected and interdependent with their surrounding cells and circuitry. Understanding how the “neighborhood” in which dopamine neurons live and function influences their well-being is a critical missing piece in the puzzle of PD.
Hypothesis: Team Calakos hypothesizes that circuit properties of incoming neuronal connections (synapses), surrounding non-neuronal cells (glial cells), and key modulatory cells (those that produce the chemical signal, acetylcholine) contribute to dopamine neuron loss in PD.
Study Design: Team Calakos will evaluate circuit contributions to dopamine neuron dysfunction in PD using state-of-the-art mouse genetic models and patient-derived stem cell models (organoids). Team Calakos members bring unique, specialized expertise that allows the team to isolate and manipulate each of these three components (synapses, glia, and neuromodulators) individually to test its role in dopamine neuron degeneration. In addition to functional manipulations, the team will capture the molecular signatures of the connections dopamine neurons make with each of its “neighbors” to determine which are most disrupted in PD.
Impact on Diagnosis: Recognizing new processes that cause dopamine neuron demise in PD creates new opportunities for intervention. Team Calakos’ bidirectional tests of function may identify not only circuit properties that accelerate disease, but also identify factors that promote resistance to cell death.
Team Calakos' collective team efforts will reveal the extent to which circuit components outside of the dopamine neurons themselves can serve as new targets to slow the progression of dopamine neuron death in Parkinson’s disease. View Team Outcomes.
Study Rationale: Nerve cells that produce the brain chemical dopamine die in people with Parkinson’s disease (PD). These nerve cells extend long and thin fibers called axons that release dopamine from thousands of different points, sending signals to other nerve cells in a brain area called the striatum. Many different types of cells and molecules in the striatum can directly control how dopamine is released, but researchers have not yet discovered which ones are the most important and how they are affected in Parkinson’s. By better understanding this cooperation between striatum and the release of dopamine from axons, the team could provide new knowledge toward ways to restore normal function.
Hypothesis: Team Cragg thinks that other molecules in the striatum play a very important role in controlling the release of dopamine, particularly for the types of dopamine axons that are most vulnerable in PD. The team believes that this role is disrupted in the disease and could be targeted to rescue symptoms.
Study Design: Team Cragg’s international team will combine cutting-edge research methods in mice and human cells that allow the team to study the biology behind Parkinson’s. The team will measure dopamine and other signaling molecules in different areas of the striatum and work out what they do. This work will reveal the biological differences between vulnerable and resistant areas. Team Cragg will use this knowledge to study the most promising molecules in mice that develop PD and in cells from people with PD, to then suggest new ways that might fix the problems with dopamine in the disease.
Impact on Diagnosis: Team Cragg’s discoveries will provide knowledge that may help to find new ways of treating Parkinson’s using medicines that target the key signaling molecules in striatum that control dopamine release.
Team Cragg expects their collaboration to unravel the modulators and circuits within striatum that govern dopamine function for vulnerable versus resistant neurons, and the related dysfunction in these key circuits during disease progression, to provide fresh mechanistic rationale for new therapies for Parkinson’s disease. View Team Outcomes.
Study Rationale: Previous work has shown how the loss of dopamine neurons affects brain activity. In this program, Team Edwards will determine how brain activity influences the neurodegeneration that causes Parkinson’s disease (PD). To understand the onset of disease, the team will identify the earliest changes in brain activity and use them to infer the mechanisms involved. Team Edwards will also manipulate activity directly and determine how it interacts with known genes to produce degeneration.
Hypothesis: Team Edwards hypothesizes that abnormalities in neural activity do not simply reflect PD but actually cause the disease. Researchers’ lack of knowledge about the role of neural activity in Parkinson’s makes it difficult to understand how other, identified factors contribute to disease.
Study Design: Team Edwards will use two models of PD, one based on over-expression of the pathogenic protein alpha-synuclein and the other based on a direct increase in activity. The strategy is to (a) identify the earliest events along the pathway to degeneration and to (b) correlate these with the selective vulnerability of particular neurons to PD. These approaches will reveal the processes specifically affected by PD. Team Edwards will also determine how neural activity intersects with factors previously implicated in PD, providing a foundation to understand how they cause degeneration.
Impact on Diagnosis: With greater understanding around the onset of disease, Team Edwards can further investigate how genetic and environmental factors conspire to produce PD. This will open entirely new areas to arrest and prevent the underlying degeneration.
By identifying the earliest changes leading to degeneration, the physiology will indicate mechanisms involved in disease onset. View Team Outcomes.
Study Rationale: Team Mobley recently discovered that it is possible to generate new neurons to rebuild the damaged neural circuitries in a Parkinson’s disease model. This establishes a new foundation for developing strategies to reverse the disease. Team Mobley’s proposed project will investigate how to change a cell’s identity to encourage it to become a neuron, how to make the right new type of neurons in the brain to rebuild different circuitries, and how to make new neurons that will not become sick again.
Hypothesis: Team Mobley hypothesizes that astrocytes, an abundant population of non-neuronal cells in the brain, store a latent program that allows them to become neurons if the right types of inducing signals are provided.
Study Design: Team Mobley has designed five sets of experiments to address a series of fundamental questions on cell fate determination and reprogramming. The team will analyze individual cells to elucidate key regulatory events responsible for those cells to become neurons. Team Mobley will search for critical genes that make cell fate change less efficient so that the team can improve the reprogramming efficiency by inhibiting the function of those genes. The team will examine reprogramming in different brain regions to test their benefits to both motor and non-motor symptoms and develop strategies to make new and disease-resistant neurons.
Impact on Diagnosis: More information on cellular reprogramming will pave the way to rebuilding the neural circuitries lost to degeneration. If successful, this will lead to the development of a completely new cell replacement therapy against Parkinson’s disease.
Team Mobley anticipates that their findings will establish the foundation for developing a cell replacement therapy for the disease based on the initial proof-of-concept study. Once fully developed, the team hopes to be able to effectively reverse the disease phenotype in PD patients. View Team Outcomes.
Study Rationale: Although clinicians have long reported that Parkinson’s disease (PD) does not affect the brain alone, the field has only recently started to investigate gut dysfunction in experimental models of PD. Consequently, the anatomical and functional basis of gut-to-brain circuitry dysfunction in PD—such as network activity and dopamine signaling—remain poorly understood. Team Gradinaru will characterize circuit mechanisms underlying gut-to-brain disease spread and progression in the earliest appearance of Parkinson’s symptoms.
Hypothesis: Team Gradinaru’s hypothesis is that environmental and genetic factors impact the connections between neurons in the enteric nervous system (ENS), which regulates the gastrointestinal tract. This disruption may increase susceptibility to PD triggers—including aggregation of alpha-synuclein, which is toxic to cells and can trigger PD symptoms and gut inflammation. This inflammation could, in turn, augment the toxic form of alpha-synuclein that circulates to the brain and causes dysfunctions in neural circuits and motor deficits.
Study Design: Team Gradinaru will determine PD-relevant gut and brain anatomic and physiologic profiles in rodents, primates, and human cells by clarifying the anatomic pathways underlying gut-to-brain propagation of aggregated alpha-synuclein in mice, and by constructing anatomic and functional maps of macaque ENS and central nervous system PD-relevant circuits at single-cell resolution. The team also will test whether disruption of ENS circuitry mitigates gut-brain disease outcome and evaluate whether spiny mice (a rodent model that can repair damaged tissue) show protection from PD-related gut-brain degeneration.
Impact on Diagnosis: Using powerful new technologies across multiple PD-relevant model systems, this project could uncover novel circuit mechanisms that mediate symptoms, and embolden new therapeutic options to slow, halt, or perhaps reverse peripheral symptoms of PD.
This project will use powerful sensor, actuator, and gene delivery technologies across multiple model systems to characterize the anatomical and functional bases of gut-brain circuitry dysfunction in PD, enabling new therapeutic options to slow, halt, or perhaps even reverse peripheral symptoms of PD. View Team Outcomes.
Study Rationale: A hallmark of Parkinson’s disease (PD) is the development of abnormal deposits throughout the brain composed of the alpha-synuclein protein. This pathology can be found in the gut too. Increasing evidence indicates that, in some patients, alpha-synuclein pathology may begin in the gut and spread to the brain through a nerve called the vagus, which directly connects the gut to the brain. An animal model developed by Team Kaplitt’s members reproduces many of these features seen in humans to allow study of these pathways and consequences of this advancing disease as it spreads throughout the brain.
Hypothesis: Team Kaplitt hypothesizes that specific vagus nerve cells are responsible for disease spread from gut to brain, with both vagus nerve activity and other factors such as gender and menopause affecting this spread, resulting in early symptoms such as sleep disorders seen in humans before development of movement problems.
Study Design: The first two goals will use genetic manipulation to study (a) what cells may be responsible for gut-to-brain spread of abnormal alpha-synuclein, (b) how disease spread affects normal vagus functions, and (c) how different levels of vagus activity influence disease spread. Team Kaplitt will also study the consequences of this type of gut-brain spread on development of early symptoms that may occur before the movement problems, particularly sleep disorders. Given the reduced risk of PD in women prior to menopause, Team Kaplitt’s final goal is to study these same problems in a novel animal model that mimics human menopause.
Impact on Diagnosis: The gene therapy methods used to block gut-brain spread in Team Kaplitt’s studies could be applied non-invasively to patients with diagnosed presence of gut alpha-synuclein pathology to prevent disease spread. Team Kaplitt’s sleep and menopause studies will further identify opportunities for early intervention and possible hormonal approaches to limiting effects of disease spread.
Team Kaplitt anticipates that their findings will advance our collective understanding of how pathology spreads from the gut to the brain in PD, and the consequences of that pathology on early PD symptoms, with the potential for new targeted interventions to block spread and improve neuronal function. View Team Outcomes.
Study Rationale: Emerging evidence supports the concept that alpha-synuclein pathology, a hallmark of Parkinson’s disease (PD), might originate in the gastrointestinal tract and spread to the brain. However, where and how pathological alpha-synuclein initially forms remains unclear. Certain gut microbiota and some environmental toxins have been associated with PD. Team Liddle recently discovered that specialized sensory cells in the gut known as enteroendocrine cells (EECs), in direct contact with gut microbiota and different environmental toxins, might transfer misfolded alpha-synuclein to the nervous system in disease.
Hypothesis: Team Liddle hypothesizes that gut microbes and environmental toxins, alone or in combination, corrupt alpha-synuclein protein expressed in EECs to misfolded pathological forms that might spread to the nervous system in a novel circuit important in PD.
Study Design: Using a unique, large, and well-characterized collection of human data, Team Liddle will identify potential triggers and alterations in gut microbiota and neuroinflammatory pathways that are associated with PD. The team will test known and experimental triggers (toxins and microorganisms) in two complementary model systems (ex vivo cultures, and in vivo in mice) to determine effects on the formation and spread of pathological alpha-synuclein within a predictable circuit of interconnected cells vulnerable to disease.
Impact on Diagnosis: These studies will (a) establish how EECs are involved in the formation of pathological alpha-synuclein at the earliest stages of disease, (b) identify gut-associated toxins and microbes that contribute to PD, (c) develop novel “humanized” pre-clinical model systems, and (d) test two particularly promising experimental therapeutic approaches in the novel model systems.
Team Liddle's project will characterize specialized sensory cells of the gut, known as enteroendocrine cells, as a target for Parkinson’s disease-associated toxicant, gut microbiome, and immune interactions leading to alpha-synuclein pathology, and as a conduit to vagal, enteric, and spinal neurons. View Team Outcomes.
Study Rationale: To slow the progression of Parkinson’s disease (PD), researchers need to know more about how it starts. It is well known now that many individuals with PD have had a significant reduction in their ability to smell years before their movement disorder starts. Here, Team Schlossmacher will study the role of a PD-linked gene, alpha-synuclein, in odor processing, and how viruses in the nose may change how alpha-synuclein is handled within the odor-signaling cells of the brain in people with PD.
Hypothesis: Team Schlossmacher hypothesizes that certain environmental triggers, including viruses, can start a chain reaction inside the nasal cavity by which a protein called alpha-synuclein begins to form insoluble clumps. This happens inside the nerve circuits that specifically process scent and then gradually spreads further inside the brain, thereby promoting Parkinson’s disease.
Study Design: Team Schlossmacher will first define the normal role of the alpha-synuclein protein in the scent-processing circuits of mice and humans. The team will then answer whether so called Lewy bodies (i.e., alpha-synuclein clumps in nerve cells) contribute to the inability to smell. Third, they will study the areas of the human brain that are responsible for smell, including using MRI imaging. Lastly, Team Schlossmacher will perform studies with nasal fluids from people with PD and introduce these (and viruses) into mice, to see if these start a reaction that cause changes in the mouse olfactory system like what is seen in humans with PD, including loss of smell and changes in the alpha-synuclein protein. The team will see if the inability to smell can progress to motor deficits.
Impact on Diagnosis: This study will delineate what causes the loss of sense of smell in PD. That will help researchers to develop new drugs to treat it and explore new ways to diagnose the disease, hopefully at a stage before the movement symptoms appear. Team Schlossmacher may also gain insights into risk factors for PD, which could lead to strategies to help people reduce their risk. The team will also create new animal models that can be used by others.
Team Schlossmacher will determine whether environment-a-synuclein interactions and inflammation in the nasal cavity can act as triggers for disease initiation, for a-synuclein aggregate formation and associated neuronal circuit dysfunction, thus informing risk and progression of disease and biomarker development in humans. View Team Outcomes.
Study Rationale: People with Parkinson’s disease have long been known to display remarkable motor abilities under special circumstances, such as smooth walking with certain visual or auditory cues. This phenomenon is called paradoxical kinesia. In addition, placebos can be surprisingly effective in treating the motor signs of the disease. Team Strick hypothesizes that a specific neuroanatomical substrate supports paradoxical kinesia and the placebo effect. The team plans to define this substrate and investigate its functional organization.
Hypothesis: Team Strick hypothesizes that a specific neural circuit supports paradoxical kinesia and the placebo effect.
Study Design: Team Strick will use cutting-edge techniques to reveal the two distinct brain circuits that enable the basal ganglia to influence the control of voluntary movement in primates. Next, the team will record the electrical and chemical activity of basal ganglia neurons in the best animal model of Parkinson’s disease. In addition, Team Strick will determine the molecular signatures of basal ganglia neurons that are affected by the disease and those that are left intact. Finally, the team will image neural activity in human subjects affected by the disease to determine the full range of strategies that could be used to improve basal ganglia function.
Impact on Diagnosis: Team Strick’s results could re-shape paradigms for therapeutic development and attempts to influence disease progression. Importantly, the team’s results have the potential to use basal ganglia circuits that are untouched by the disease to promote recovery of more normal motor function..
Team Strick's project will perform a multidisciplinary characterization of the networks that link the basal ganglia with the cortical motor areas. The information from the team's studies could lead to new therapeutic targets to delay disease progression and new approaches to ameliorate the motor dysfunction that is so disabling for PD patients. View Team Outcomes.
Study Rationale: Parkinson’s disease (PD) begins decades before it compromises the ability to move about in the world and sleep through the night. Understanding how the dysfunction of brain circuits begins and then evolves to cause difficulty in moving and sleeping will allow researchers to diagnose PD earlier—increasing the chances of halting disease progression—and to better treat the disease once it appears.
Hypothesis: The progressive damage to dopamine-releasing neurons results in staged disruption of neural circuits in larger and larger parts of the brain, ultimately leading to both motor and sleep deficits characteristic of PD.
Study Design: Team Surmeier’s plan is to study a new genetically engineered mouse model that manifests a progressive, levodopa-responsive parkinsonism. Importantly, this mouse faithfully reproduces the human staging of pathology in key brain circuits. Using the most advanced methods available for studying and manipulating genetically defined brain circuits, the causal linkage between circuit dysfunction and motor and sleep behavior will be determined.
Impact on Diagnosis: A better understanding of how the circuit dysfunction underlying PD is staged should allow earlier diagnosis—enhancing the potential benefit of disease-modifying therapies—and better treatment strategies for later-stage patients.
Team Surmeier's project will provide fundamental insight into the relationship between progressive dopamine depletion and distributed circuit dysfunction underlying motor and sleep symptoms of Parkinson’s disease. View Team Outcomes.
Study Rationale: Specific brain circuits that are highly melanized (build-up of the dark pigment neuromelanin) with age are primarily affected, particularly early, in Parkinson’s disease (PD). Models incorporating this aspect of PD have only been developed recently and show that increased neuromelanin production causes neurodegenerative changes consistent with Parkinson’s. The regulators of cellular neuromelanin metabolism have not been determined, the effect of neuromelanin on normal activity in these pathways has not been defined, the potential for neuromelanin aggregates to increase alpha-synuclein accumulation has not been evaluated, and the impact of extracellular neuromelanin on detrimental inflammatory processes has not been assessed.
Hypothesis: Activity in melanized brain circuits is a dominant factor in the initiation of PD and sustains its progression by seeding pathology in connected regions and providing the stimulus for chronic inflammation. Manipulating neuromelanin production and/or brain circuit activity can ameliorate these deficits.
Study Design: Parallel experiments will be performed in mice and non-human primates in which neuromelanin production has been induced for comparison with neuromelanin-producing neurons in people with prodromal and early Parkinson’s. To test whether activity in melanized brain circuits is a dominant factor in the initiation of PD, spatiotemporal activity mapping, imaging, and other techniques will be used, and manipulating neuromelanin production and/or brain circuit activity will be assessed as potential treatments. To determine if neurons spread PD pathology through their connectivity, seeding experiments will be performed and impacts on behavior and neurodegeneration assessed. To determine how non-neuronal mechanisms are involved in disease progression, high-resolution microscopy and cell-specific details of changes in extracellular spaces and infiltration of non-neuronal cells into the brain will be assessed.
Impact on Diagnosis: Diagnosis of neuromelanin changes in the brain are already being assessed for their diagnostic potential, but this study will determine their focus and rate of change with respect to neural activity and clinical features. Team Vila will also identify if reducing neuromelanin levels stabilizes pathology and restores brain activity.
The project will unravel molecular mechanisms linking brain circuit activity to PD vulnerability, identify brain circuits through which PD pathology spreads across the brain and periphery, establish non-neuronal mechanisms of PD progression and determine whether modulation of neuromelanin levels and/or brain circuit activity can restore PD circuit dysfunction & pathology. View Team Outcomes.
Study Rationale: The outer mantle of the brain, the cerebral cortex, plays a significant role in selecting and controlling movements. Changes in the activity of cortical neurons are key to disorders of movement, especially Parkinson’s disease (PD). It is unknown, however, which specific cell types are involved and how their activity changes during the course of the disease. In these experiments, Team Wichmann will use new technologies to study large groups of specific types of cortical neurons (for example, those that send fibers to the spinal cord) and explore how their activity and morphology change in animal models of chronic PD.
Hypothesis: Team Wichmann’s hypothesis is that groups of cortical neurons that send fibers to the spinal cord—unlike those that send projections to the striatum—start to show abnormal activity and undergo morphological changes in connections that provide inputs to them when parkinsonism develops.
Study Design: Team Wichmann will measure the anatomical and functional characteristics of neurons in the motor cortex in animal models of slowly progressive PD. Optical imaging methods as well as electrophysiologic recordings will allow the team to measure the activity patterns of large groups of individual cortical neurons, while parallel anatomical studies will identify the reshaping of connections to different families of cortical neurons before and during the development of parkinsonism. Computational analysis will allow Team Wichmann to put the findings together in computer simulations that will help them to understand the cortical circuit abnormalities that contribute to PD.
Impact on Diagnosis: A better understanding of how movement problems in PD develop is key to developing more effective methods to control them. Characterizing the abnormalities in specific families of cortical neurons may allow researchers to develop new therapies that target the affected circuits through deep brain stimulation, pharmacologic, or genetic methods.
The activity and anatomy of neurons in the brain’s outer mantle, the cortex, are abnormal in Parkinson’s disease. Team Wichmann's studies will help researchers to understand which specific cells or connections are involved in parkinsonism. This knowledge may allow researchers to therapeutically target these circuits through stimulation, pharmacologic, or genetic methods. View Team Outcomes.
Several studies suggest mitochondrial impairment in PD, although it is still unclear whether such mitochondrial defects are primary causes of neurodegeneration or secondary causes. Furthermore, impairment of mitochondrial metabolism and dynamics has been observed in a variety of cellular models of GCase deficiency and patient neurons. However, the mechanisms leading to mitochondrial dysfunction in these models are unknown. A novel function for GCase outside of the lysosome is presented. The team shows that a fraction of GCase can be imported into the mitochondria where it can impact mitochondrial quality control mechanisms. This data presents a role for GCase outside of the lysosome.
CLN5
GBA1LP
PARK7/DJ1
STING1
CLU
GPNMB
PGK1
SYNJ1
CTSB
HLA-DRB5
PLA2G15
TREM2
DNAJC6
ITSN1
PSMF1
USP30
FBXO7
LRP1
RIMS2
VPS13C
Parkinson’s disease is the second most common neurodegenerative disease after Alzheimer’s.
With rapid advances in areas like genomics, single-cell technologies, and data analytics, we’re at a tipping point to better understand this devastating disease – but we can’t do it alone.
ASAP builds on the significant strides made by the research community, funders, other experts and strategists around the world. With input across sectors and disciplines, we’ve developed a strategic roadmap to collectively tackle field-wide challenges together.
ASAP is guided by the belief that research outcomes will be improved through the following principles:
Given the multifactorial nature of Parkinson’s disease, charting a new path will require multidisciplinary cooperation from investigators with and without a previous record of PD research.
Philanthropic capital has the most impact in areas that are deemed unpopular, high-risk, or out-of-scope for government funding, requiring creative and thoughtful consideration of research.
As roadmap goals are implemented, we will be responsive to the evolving nature of research and adjust focus as deemed appropriate.
To accelerate research, we’ll support the free flow of data and resources within our collaborative network and make findings available to the broader community.
Scientific progress can be accelerated when researchers exchange ideas early and often, in a collaborative rather than competitive manner.
By supporting resource development, we are building an infrastructure, available to the larger scientific community, that improves access to research tools, reproducibility of studies, and process efficiency to accelerate discoveries.
By sharing research outputs like data, code, and protocols, we are allowing researchers to build upon the work of others. This facilitates collaboration among investigators, attracts new talent and expertise to the field, and allows us to increase the power of our studies through meta-analysis.
We believe that by supporting collaboration, facilitating research, enabling resource generation, and creating a culture of data sharing, we can deliver faster and better outcomes for Parkinson’s disease research.
For the last two years, we’ve engaged more than 100 multidisciplinary experts and strategists to inform our strategic roadmap and thoughtfully guide future investments in scientific discovery.
This meeting brought the ASAP Planning Advisory Council together to kick off the two-year planning process. The Planning Council comprised both PD and non-PD experts from academia, industry, government, and the patient community to guide strategic roadmap development through a multi-disciplinary and multi-stakeholder lens. We focused on candidate scientific themes, as well as opportunities, challenges, and considerations for the path ahead.
James Beck, Parkinson’s Foundation
Patrik Brundin, Van Andel Research Institute (VARI)
Marie-Francoise Chesselet, University of California, Los Angeles
Martin Citron, UCB Pharma
Ted Dawson, Johns Hopkins University School of Medicine
Pietro De Camilli, Yale School of Medicine
David Dexter, Imperial College London
Thomas Gasser, German Center for Neurodegenerative Diseases
Magali Haas, Cohen Veterans Bioscience
Karl Kieburtz, University of Rochester Medical Center
Walter Koroshetz, National Institute of Neurological Disease and Stroke
Kelsey Martin, University of California, Los Angeles
Karoly Nikolich, Alkahest
C. Warren Olanow, Mount Sinai School of Medicine
Bernardo Sabatini, Harvard Medical School
Darryle Schoepp, Merck and Company
Todd Sherer, The Micheal J. Fox Foundation for Parkinson’s Research
Andrew Singleton, National Institute on Aging, NIH
Beth Stevens, Harvard Medical School
David Sulzer, Columbia University Medical Center
This meeting convened the ASAP Planning Advisory Council to discuss a framework by which key knowledge gaps within the candidate scientific themes could be addressed. Strategically, it was recommended that we build on known areas (i.e., candidate scientific themes) by filling in the gaps left by public funding and uncover unknown areas through large, unbiased data collection and analysis.
James Beck, Parkinson’s Foundation
Patrik Brundin, Van Andel Research Institute (VARI)
Marie-Francoise Chesselet, University of California, Los Angeles
Ted Dawson, Johns Hopkins University School of Medicine
David Dexter, Imperial College London
Thomas Gasser, German Center for Neurodegnerative Diseases
Magali Haas, Cohen Veterans Bioscience
Karl Kieburtz, University of Rochester Medical Center
Walter Koroshetz, National Institute of Neurological Disease and Stroke
Robert Malenka, Stanford University School of Medicine
Kelsey Martin, University of California, Los Angeles
Karoly Nikolich, Alkahest
C. Warren Olanow, Mount Sinai School of Medicine
Bernardo Sabatini, Harvard Medical School
Randy Schekman, University Of California, Berkeley
Darryle Schoepp, Merck and Company
Todd Sherer, The Micheal J. Fox Foundation for Parkinson’s Research
Andrew Singleton, National Institute on Aging, NIH
David Sulzer, Columbia University Medical Center
Huda Zoghbi, Baylor College of Medicine
We hosted over 100 attendees during this reception held at the Society for Neuroscience Annual Meeting. A feature fireside chat between Melissa Stevens of the Milken Institute Center for Strategic Philanthropy, and George Pavlov of the Sergey Brin Family Foundation, publicly introduced the ASAP initiative to the broader neuroscience community, discussed intent and the role that philanthropy can play to propel discovery, and sought feedback from attendees.
Primed with months of advance preparation in working groups, this international workshop brought together over 70 academic and industry investigators, public and private funders, as well as patients and advocates from across disciplines to design conceptual research programs that addressed a prioritized list of knowledge gaps within the selected scientific themes. A discussion of resource and infrastructure needs was a key component of each program.
Matthew Ackerman, MBA
Dario Alessi, University of Dundee
James Beck, Parkinson’s Foundation
Elizabeth Bradshaw, Columbia University
Latese Briggs, Milken Institute Center For Stragetig Philanthropy
Katja Brose, Chan Zuckerberg Initiative (CZI)
Patrik Brundin, Van Andel Research Institute (VARI)
Edward Callaway, The Salk Institute
Paul Cannon, 23andMe, Inc.
Honglei Chen, Michigan State University
Joanne Chory, The Salk Institute
Martin Citron, UCB Pharma
Mark Cookson, National Inistitute on Aging (NIA)
Ted Dawson, John Hopkins University School of Medicine
Pietro De Camilli, Yale School of Medicine
Michel Desjardins, University of Montreal
Steve Finkbeiner, University of California San Francisco
Thomas Gasser, German Center of Neurodegenerative Diseases
Viviana Gardinaru, Caltech
Tim Greenamyre, University of Pittsburgh School of Medicine
Magali Haas, Cohen Veterans Bioscience
Erika Holzbaur-Howland, University of Pennsylvania School of Medicine
Elaine Hsiao, University of California, Los Angeles
Anthony Hyman, Max Planck Institute of Molecular Cell Biology and Genetics
H. Shawn Je, Duke-National University of Singapore Medical School
Kirstie Keller, Milken Institute Center For Strategic Philanthropy
Johnathan Kipnis, University of Virginia Medical School
Jeffrey Kordower, Rush Medical College
Dimitri Krainc, Feinberg School of Medicine at Northwestern University
Anatol Kreitzer, University of California, San Francisco
Arnold Kriegstein, University of California, San Francisco
Thomas Kukar, Emory University School of Medicine
Jin Hyung Lee, Stanford University School of Medicine
Shane Liddlelow, New York University Neurosciences Institute
Byungkook Lim, University of California, San Diego
Robert Malenka, Stanford University School of Medicine
Kenneth Marek, Institute of Neurodegenerative Disorders
Kelsey Martin, University of California, Los Angeles
Sarkis Mazmanian, Caltech
Heidi McBride, McGill University
K. Kimberly McCleary, Center of the Milken Institute
Miratul Muqit, University of Dundee
Karoly Nikolich, Alkahest
Alastair Reith, GlaxoSmithKline Pharmaceuticals
Ekemini Riley, Milken Institute Center of Strategic Philanthropy
Randy Schekman, University of California, Berkeley
Clemens Scherzer, Harvard Medical School
John Siebyl, inviCRO, LLC.
Alessandro Sette, La Jolla Institute for Allergy and Immunology
Todd Sherer, The Michael J. Fox Foundation for Parkinson’s Research
Andrew Singleton, National Insititute on Aging, NIH
Frank Soldner, Massachusetts Institute of Technology (MIT)
Benjamin Stecher, Tomorrow Edition Blog
Melissa Stevens, Milken Institute Center for Strategic Philanthropy
David Sulzer, Columbia University Medical Center
D. James Surmeier, Northwestern University
Margaret Sutherland, National Institute for Neurological Disease and Stroke (NINDS)
Caroline Tanner, University of California, San Francisco School of Medicine
Malú Tansey, Emory University School of Medicine
Daniel Wesson, University of Florida College of Medicine
Su-Chun Zhang, Duke-National University of Singapore Medical School
This forum sought to cultivate a learning community of peer funders and program leaders in neuroscience to explore ways that we can all work together to address this neurological disease. We discussed funding priorities and gleaned lessons learned to avoid unnecessary duplication of efforts.
James Beck, Parkinson’s Foundation
Niranjan Bose, Gates Ventures
Patrick Brannelly, Rainwater Charitable Foundation
Latese Briggs, Milken Institute Center For Strategic Philanthropy
Katja Brose, Chan Zuckerberg Initiative (CZI)
Rosa Canet-Avilés, Foundation for the NIH
Valerie Conn, Science Philanthropy Alliance
Jonah Cool, Chan Zuckerberg Initiative
Rick Howitz, Allen Institute for Cell Science
Brett Holleman, Van Andel Research Institute
Ehud Isacoff, University of California, Berkeley
John Lehr, Parkinson’s Foundation
Karoly Nikolich, Alkahest
George Pavlov, Bayshore Global Management
Louis Reichardt, Simons Foundation for Autism Research Initiative (SFARI)
Ekemini Riley, Milken Institute Center For Strategic Philanthropy
Amy Rommel, Rainwater Charitable Foundation
Randy Schekman, University of California, Berkeley
Todd Sherer, The Micheal J. Fox Foundation for Parkinson’s Research
Thomas Snyder, Verily Life Sciences
Melissa Stevens, Milken Institute Center For Strategic Philanthropy
Margaret Sutherland, National Institute for Neurological Disease and Stroke (NINDS)
Jason Tung, Science Philanthropy Alliance
This meeting brought the ASAP Planning Advisory Council together to kick off the two-year planning process. The Planning Council comprised both PD and non-PD experts from academia, industry, government, and the patient community to guide strategic roadmap development through a multi-disciplinary and multi-stakeholder lens. We focused on candidate scientific themes, as well as opportunities, challenges, and considerations for the path ahead.
James Beck, Parkinson’s Foundation
Patrik Brundin, Van Andel Research Institute (VARI)
Marie-Francoise Chesselet, University of California at Los Angeles
Martin Citron, UCB Pharma
Ted Dawson, Johns Hopkins University School of Medicine
Pietro De Camilli, Yale School of Medicine
David Dexter, Imperial College London
Thomas Gasser, German Center for Neurodegenerative Diseases
Magali Haas, Cohen Veterans Bioscience
Karl Kieburtz, University of Rochester Medical Center
Walter Koroshetz, National Institute of Neurological Disease and Stroke
Kelsey Martin, University of California at Los Angeles
Karoly Nikolich, Alkahest
C. Warren Olanow, Mount Sinai School of Medicine
Bernardo Sabatini, Harvard Medical School
Darryle Schoepp, Merck and Company
Todd Sherer, The Micheal J. Fox Foundation for Parkinson’s Research
Andrew Singleton, National Institute on Aging, NIH
Beth Stevens, Harvard Medical School
David Sulzer, Columbia University Medical Center
This meeting convened the ASAP Planning Advisory Council to discuss a framework by which key knowledge gaps within the candidate scientific themes could be addressed. Strategically, it was recommended that we build on known areas (i.e., candidate scientific themes) by filling in the gaps left by public funding and uncover unknown areas through large, unbiased data collection and analysis.
James Beck, Parkinson’s Foundation
Patrik Brundin, Van Andel Research Institute (VARI)
Marie-Francoise Chesselet, University of California, Los Angeles
Ted Dawson, Johns Hopkins University School of Medicine
David Dexter, Imperial College London
Thomas Gasser, German Center for Neurodegnerative Diseases
Magali Haas, Cohen Veterans Bioscience
Karl Kieburtz, University of Rochester Medical Center
Walter Koroshetz, National Institute of Neurological Disease and Stroke
Robert Malenka, Stanford University School of Medicine
Kelsey Martin, University of California, Los Angeles
Karoly Nikolich, Alkahest
C. Warren Olanow, Mount Sinai School of Medicine
Bernardo Sabatini, Harvard Medical School
Randy Schekman, University Of California, Berkeley
Darryle Schoepp, Merck and Company
Todd Sherer, The Micheal J. Fox Foundation for Parkinson’s Research
Andrew Singleton, National Institute on Aging, NIH
David Sulzer, Columbia University Medical Center
Huda Zoghbi, Baylor College of Medicine
We hosted over 100 attendees during this reception held at the Society for Neuroscience Annual Meeting. A feature fireside chat between Melissa Stevens of the Milken Institute Center for Strategic Philanthropy, and George Pavlov of the Sergey Brin Family Foundation, publicly introduced the ASAP initiative to the broader neuroscience community, discussed intent and the role that philanthropy can play to propel discovery, and sought feedback from attendees.
Primed with months of advance preparation in working groups, this international workshop brought together over 70 academic and industry investigators, public and private funders, as well as patients and advocates from across disciplines to design conceptual research programs that addressed a prioritized list of knowledge gaps within the selected scientific themes. A discussion of resource and infrastructure needs was a key component of each program.
Matthew Ackerman, MBA
Dario Alessi, University of Dundee
James Beck, Parkinson’s Foundation
Elizabeth Bradshaw, Columbia University
Latese Briggs, Milken Institute Center For Stragetig Philanthropy
Katja Brose, Chan Zuckerberg Initiative (CZI)
Patrik Brundin, Van Andel Research Institute (VARI)
Edward Callaway, The Salk Institute
Paul Cannon, 23andMe, Inc.
Honglei Chen, Michigan State University
Joanne Chory, The Salk Institute
Martin Citron, UCB Pharma
Mark Cookson, National Institute on Aging (NIA)
Ted Dawson, John Hopkins University School of Medicine
Pietro De Camilli, Yale School of Medicine
Michel Desjardins, University of Montreal
Steve Finkbeiner, University of California, San Francisco
Thomas Gasser, German Center of Neurodegenerative Diseases
Viviana Gardinaru, California Institute of Technology
Tim Greenamyre, University of Pittsburgh School of Medicine
Magali Haas, Cohen Veterans Bioscience
Erika Holzbaur-Howland, University of Pennsylvania School of Medicine
Elaine Hsiao, University of California at Los Angeles
Anthony Hyman, Max Planck Institute of Molecular Cell Biology and Genetics
H. Shawn Je, Duke-National University of Singapore Medical School
Kirstie Keller, Milken Institute Center For Strategic Philanthropy
Johnathan Kipnis, University of Virginia Medical School
Jeffrey Kordower, Rush Medical College
Dimitri Krainc, Feinberg School of Medicine at Northwestern University
Anatol Kreitzer, University of California at San Francisco
Arnold Kriegstein, University of California at San Francisco
Thomas Kukar, Emory University School of Medicine
Jin Hyung Lee, Stanford University School of Medicine
Shane Liddlelow, New York University Neurosciences Institute
Byungkook Lim, University of California at San Diego
Robert Malenka, Stanford University School of Medicine
Kenneth Marek, Institute of Neurodegenerative Disorders
Kelsey Martin, University of California at Los Angeles
Sarkis Mazmanian, California Institute of Technology
Heidi McBride, McGill University
K. Kimberly McCleary, Center of the Milken Institute
Miratul Muqit, University of Dundee
Karoly Nikolich, Alkahest
Alastair Reith, GlaxoSmithKline Pharmaceuticals
Ekemini Riley, Milken Institute Center of Strategic Philanthropy
Randy Schekman, University of California at Berkeley
Clemens Scherzer, Harvard Medical School
John Siebyl, inviCRO, LLC.
Alessandro Sette, La Jolla Institute for Allergy and Immunology
Todd Sherer, The Michael J. Fox Foundation for Parkinson’s Research
Andrew Singleton, National Insititute on Aging, NIH
Frank Soldner, Massachusetts Institute of Technology (MIT)
Benjamin Stecher, Tomorrow Edition Blog
Melissa Stevens, Milken Institute Center for Strategic Philanthropy
David Sulzer, Columbia University Medical Center
D. James Surmeier, Northwestern University
Margaret Sutherland, National Institute for Neurological Disease and Stroke (NINDS)
Caroline Tanner, University of California, San Francisco School of Medicine
Malú Tansey, Emory University School of Medicine
Daniel Wesson, University of Florida College of Medicine
Su-Chun Zhang, Duke-National University of Singapore Medical School
This forum sought to cultivate a learning community of peer funders and program leaders in neuroscience to explore ways that we can all work together to address this neurological disease. We discussed funding priorities and gleaned lessons learned to avoid unnecessary duplication of efforts.
James Beck, Parkinson’s Foundation
Niranjan Bose, Gates Ventures
Patrick Brannelly, Rainwater Charitable Foundation
Latese Briggs, Milken Institute Center For Strategic Philanthropy
Katja Brose, Chan Zuckerberg Initiative (CZI)
Rosa Canet-Avilés, Foundation for the NIH
Valerie Conn, Science Philanthropy Alliance
Jonah Cool, Chan Zuckerberg Initiative
Rick Howitz, Allen Institute for Cell Science
Brett Holleman, Van Andel Research Institute
Ehud Isacoff, University of California at Berkeley
John Lehr, Parkinson’s Foundation
Karoly Nikolich, Alkahest
George Pavlov, Bayshore Global Management
Louis Reichardt, Simons Foundation for Autism Research Initiative (SFARI)
Ekemini Riley, Milken Institute Center For Strategic Philanthropy
Amy Rommel, Rainwater Charitable Foundation
Randy Schekman, University of California at Berkeley
Todd Sherer, The Micheal J. Fox Foundation for Parkinson’s Research
Thomas Snyder, Verily Life Sciences
Melissa Stevens, Milken Institute Center For Strategic Philanthropy
Margaret Sutherland, National Institute for Neurological Disease and Stroke (NINDS)
Jason Tung, Science Philanthropy Alliance
The ASAP initiative is a global, multi-institutional community of researchers who are committed to accelerating the pace of discovery in Parkinson’s disease through collaboration, generation of resources, and data sharing. View our Honors & Awards to learn more about the people, labs, and teams who exemplify ASAP’s mission.
This series celebrates individuals and labs that have been recognized for their outstanding contributions to ASAP’s mission.
Recognizing labs or individuals within the ASAP network who have demonstrated a strong commitment to open science in their work to advance PD research.
Congratulations to GP2 for winning The Neuro (Montreal Neurological Institute-Hospital) Irv and Helga Cooper Foundation Open Science Prize!
Accelerating the pace of discovery and informing the path to a cure for Parkinson’s disease through collaboration, research-enabling resources, and data sharing.
Collaborative and transparent research processes and environments that deliver faster and better outcomes for Parkinson’s disease.
