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An open approach to Huntington’s disease research : Scientific Data

Oct 19 2016

Notable achievements

Chemical biology of human proteins

Structural biology of human proteins – The SGC has so far contributed over 2000 protein structures of human proteins of potential relevance for drug discovery into the public domain since 2003.¹⁷ Structures that constitute complexes with synthetic small molecules is aided by a partnership with the Diamond synchrotron in Oxfordshire.¹⁸ The chemical probe program prioritizes (members of) protein families that are relatively understudied, or which may be currently relevant to human biology and drug discovery. These families include epigenetic signaling,¹⁹²⁰ solute transport,²¹²² protein proteostasis,^2324252627 and protein phosphorylation.²⁸²⁹³⁰ The protein family approach is supported by publicly available bioinformatics tools (ChromoHub,³¹ UbiHub³²), family-based protein production and biochemistry, crystallography and structure determination, biophysics, and cell biology (for example target engagement assays). The SGC has (so far) contributed ~120 chemical probes³³³⁴³⁵ into the public domain over the past decade, and >25,000 samples of these probes have been distributed to the scientific community. The chemical probes conform to the now community-standard quality criteria created by the SGC and its collaborative network.^363738394041

1. Epigenetic chemical probes that have generated clinical interest in their targets include PFI-1⁴² and JQ1⁴³ for the BET family, UNC0642⁴⁴ for G9a/GLP, UNC1999⁴⁵ for EZH2/H1, LLY-283⁴⁶ and GSK591⁴⁷ for PRMT5, and OICR-9429⁴⁸ for WDR5. The WDR5 chemical probe was optimized (by a company external to the SGC) for clinical amenability and is the subject of investment from Celgene.
2. Kinases have seen 50 drugs approved by the FDA for treatment of cancer, inflammation, and fibrosis.⁴⁹ A review⁵⁰ from two and a half years ago, a recent preprint,⁵¹ and peer-reviewed publication⁵² highlight low coverage of kinases both by peer-reviewed publications and 3D structures. In the last 4 years laboratories in Frankfurt, North Carolina and Oxford have developed chemical matter to help biologists study underrepresented kinases. In collaboration with pharmaceutical companies and academia, 15 chemical probes, and version 1.0 of 187 chemogenomic inhibitors (aka KCGS) for 215 kinases⁵³⁵⁴ have been co-developed.
3. Integral membrane proteins are permanently attached to the cell membrane. The family includes the solute carrier (SLC) proteins. The SLCs are largely unexplored therapeutically ~30% are considered ‘orphaned’ because their substrate specificity and biological function are unknown. In 2019 a public-private partnership comprising 13 partners, including the SGC, formed The RESOLUTE Consortium⁵⁵ with funding from the IMI. RESOLUTE’s goal is to encourage research on SLCs .
4. The Target Enabling Package (TEP) is a collection reagents and knowledge on a protein target aimed to catalyze biochemical and chemical exploration, and characterization of proteins with genetic linkage to key disease areas. The SGC has opened target nominations to the public.⁵⁶
5. The Unrestricted Leveraging of Targets for Research Advancement and Drug Discovery (ULTRA-DD) program, funded by the European Commission’s Innovative Medicines Initiative (IMI), aims to identify and validate under-explored targets in auto-immune and inflammatory disease models. Patient-derived cell lines are screened against chemical modulators (including chemical probes and chemogenomic compounds) with the intention of obtaining phenotypic read-outs in a disease relevant context.⁵⁷
6. The Enabling and Unlocking biology in the Open (EUbOPEN) program, funded by the IMI, aims to assemble a chemogenomic library for ~1,000 proteins, discover ~100 high-quality, chemical probes, establish infrastructure to characterize these compounds, disseminate robust protocols for primary patient cell-based assays, while establishing the infrastructure to seed a global effort on addressing the entire druggable genome.

Non-human proteins

The Structure-guided Drug Discovery Coalition (SDDC) comprises the Seattle Structural Genomics Center for Infectious Disease (SSGCID), the Midwest Center for Structural Genomics, the Center for Structural Genomics of Infectious Diseases (CSGID), and drug discovery teams from academia and industry has resulted in 7 early drug leads for tuberculosis (TB), malaria, and cryptosporidiosis. The SDDC receives funding from participating academic initiatives and the Bill & Melinda Gates Foundation.

The University of North Carolina at Chapel Hill and the Eshelman Institute for Innovation, launched Rapidly Emerging Antiviral Drug Development Initiative (READDI™) and Viral Interruption to Medicines Initiative (VIMI™). REDDI™ is modelled after the non-profit drug research and development Drugs for Neglected Diseases Initiative (DNDi). READDI™ and VIMI™ are non-profit, open science initiatives that focus on developing therapeutics for all pandemic-capable viruses.⁵⁸

Open Science

Open science is a key operating principle.⁵⁹ A Trust Agreement^60616263 is signed before reagents are shared with researchers. These reagents include cDNA clones (Addgene), chemical probes,⁶⁴ and 3D structures.⁶⁵ Tools to promote open science include open lab notebooks.⁶⁶ The latter platform is being used to share research on (for example) Diffuse intrinsic pontine glioma (DIPG), Fibrodysplasia ossificans progressiva, Huntington’s disease,⁶⁷⁶⁸ Parkinson’s disease, and Chordoma.

Open Drug Discovery

The for-profit spin-off companies M4K Pharma (Medicines for Kids), M4ND Pharma (Medicines for Neurological Diseases) and M4ID Pharma (Medicines for Infectious Diseases) do not file patents and practise open science. The M4 companies are wholly owned by a Canadian charity Agora Open Science Trust whose mandate is to share scientific knowledge and ensure affordable access to all medicines. M4K Pharma has the most advanced open drug discovery program⁶⁹ and is supported with funding from the Ontario Institute for Cancer Research, The Brain Tumour Charity, Charles River Laboratories and Reaction Biology, and with contributions from scientists at the Universities of McGill, North Carolina, Oxford, Pennsylvania, and Toronto and in the Sant Joan de Déu hospital, the University Health Network hospitals, the Hospital for Sick Children, and The Institute for Cancer Research. M4K Pharma is developing a selective inhibitor of ALK2 for DIPG, a uniformly fatal pediatric brain tumour.⁷⁰

History

The Concept

In 2000, a group of companies and Wellcome conceptualized forming a Structural Genomics Consortium to focus on determining the three-dimensional structures of human proteins.⁷¹ The consortium must place all structural information and supporting reagents into the public domain without restriction. This effort was designed to complement other structural genomics programs in the world.

Phase I (2004-2007)

The SGC scientific program was launched, with activities at the Universities of Oxford and Toronto, and with a mandate to contribute >350 human protein structures into the public domain. To be counted toward these goals, the proteins had to derive from a pre-defined list and the protein structures were required to meet pre-defined quality criteria. The quality of protein structures was and continues to be adjudicated by a committee of independent academic scientists. Michael Morgan was the Chair of the SGC Board, and the scientific activities were led by Cheryl Arrowsmith (Toronto) and Michael Sundstrom (Oxford). In mid 2005, VINNOVA, the Knut and Alice Wallenberg Foundation and the Foundation for Strategic Research (SSF) established the Swedish research node of the SGC. Experimental activities started at the Karolinska Institutet in Stockholm, led by Pär Nordlund and Johan Weigelt. Together, the three SGC laboratories contributed 392 human protein structures into the public domain. A pilot program in the structural biology of proteins in the malaria parasite was also initiated.⁷²

Phase II (2007-2011)

The new goal for structures was 650. The SGC focused considerable activities in the areas of ubiquitination, protein phosphorylation, small G-proteins and epigenetics, and also initiated an effort in the structural biology of integral membrane proteins. In this phase, the SGC determined the structures of 665 human proteins from its Target List. With support from Wellcome and GSK, the SGC launched a program to develop freely-available chemical probes to proteins involved in epigenetic signalling which at the time were under studied.⁷³⁷⁴ The quality of each chemical probe was subject to two levels of review prior to their dissemination to the public. The first was internal, through a Joint Management Committee comprising representatives from each member organization. The second was provided by a group of independent experts selected from academia. This level of oversight is aimed at developing reagents that support reproducible research.⁷⁵⁷⁶⁷⁷ It ultimately led to the creation of the Chemical Probes Portal. The SGC Memberships expanded to include Merck, Sharpe and Dohme, and Novartis. Wayne Hendrickson served as the Chair of the SGC Board.

Phase III (2011-2015)

The SGC mandate diversified to include 200 human proteins including 5 integral membrane proteins and chemical probes (30). Many of the chemical probes’ programs were undertaken in partnership with scientists in the pharmaceutical companies, which made the commitment to contribute the collaborative chemical probe into the public domain, without restriction. In Phase III, the SGC, along with the SSGCID (https://www.ssgcid.org/) and the CSGID (https://csgid.org/) launched the SDDC. SGC Memberships: AbbVie, Bayer AG, Boehringer Ingelheim, Eli Lilly and Janssen. Merck, Sharpe and Dohme and the Canadian Institutes for Health Research left the consortium. Markus Gruetter became the Chair of the SGC Board.⁷⁸

Phase IV (2015-2020)

This phase built on the goals of previous phases but included well-characterized antibodies to human proteins. The SGC initiated a concerted effort to develop disease-relevant, cell-based assays using (primary) cells or tissue from patients. This phase saw the launch of research activities at Goethe University in Frankfurt, at McGill University, and at the Universities of Campinas and North Carolina, and participation in ULTRADD and RESOLUTE⁷⁹⁸⁰ within IMI. SGC Memberships: Merck KGaA, the Eshelman Institute for Innovation, Merck, Sharpe and Dohme joined while GSK and Eli Lilly left. Tetsuyuki Maruyama became the Chair of the Board.

The Future - Target 2035

Target 2035 is an open science movement with the goal of creating chemical^8182838485 and/or biological⁸⁶⁸⁷ tools for the entire proteome by 2035.⁸⁸ The launch in November 2020 and monthly webinars have and continue to be free to attend. Supporting projects currently underway include the SGC’s epigenetics chemical probe program,⁸⁹⁹⁰⁹¹ the NIH’s Illuminating the Druggable Genome initiative for under-explored kinases, GPCR’s and ion channels,⁹²⁹³⁹⁴ IMI’s RESOLUTE project on human SLCs,⁹⁵ and IMI's Enabling and Unlocking Biology in the Open (EUbOPEN). These teams are linked to SGC’s global collaborative network.^{96979899100101102}

Selected publications

Chemogenomics, protein degradation

• Carter, AJ; Kraemer, O; Zwick, M; Mueller-Farhnow, A; Arrowsmith, CH; Edwards, AM (November 2019). "Target 2035: probing the human proteome". Drug Discovery Today. 24 (11): 2111–2115. doi:10.1016/j.drudis.2019.06.020. PMID 31278990.
• Wells, CI (2021). "The Kinase Chemogenomic Set (KCGS): An Open Science Resource for Kinase Vulnerability Identification". International Journal of Molecular Sciences. 22 (2): 566. doi:10.3390/ijms22020566. PMC 7826789. PMID 33429995.
• Schapira, M; Calabrese, MF; Bullock, AN; Crews, CM (December 2019). "Targeted protein degradation: expanding the toolbox". Nature Reviews Drug Discovery. 18 (12): 949–963. doi:10.1038/s41573-019-0047-y. PMID 31666732. S2CID 204942300.
• Superti-Furga, G; et, al. (July 2020). "The RESOLUTE consortium: unlocking SLC transporters for drug discovery". Nature Reviews Drug Discovery. 19 (7): 429–430. doi:10.1038/d41573-020-00056-6. hdl:21.11116/0000-0006-0FF1-A. PMID 32265506. S2CID 215406274.

Patient-derived cell assays

• Edwards, AM; et, al. (March 2015). "Preclinical target validation using patient-derived cells". Nature Reviews Drug Discovery. 14 (3): 149–50. doi:10.1038/nrd4565. PMID 25722227. S2CID 2423838.
• Lan, X; et, al (September 2017). "Fate mapping of human glioblastoma reveals an invariant stem cell hierarchy". Nature. 549 (7671): 227–232. Bibcode:2017Natur.549..227L. doi:10.1038/nature23666. PMC 5608080. PMID 28854171.
• Kulandaimanuvel, AM; et, al. (June 2020). "Metabolic Regulation of the Epigenome Drives Lethal Infantile Ependymoma". Cell. 181 (6): 1329–1345.e24. doi:10.1016/j.cell.2020.04.047. PMC 10782558. PMID 32445698. S2CID 218842162.

Open science

• Muller, S; et, al. (April 2018). "Donated chemical probes for open science". eLife. 7. doi:10.7554/eLife.34311. PMC 5910019. PMID 29676732. S2CID 4976020.
• Harding, RJ (January 2019). "Open notebook science can maximize impact for rare disease projects". PLOS Biol. 17 (1): e3000120. doi:10.1371/journal.pbio.3000120. PMC 6366684. PMID 30689629. S2CID 59338390.

Reproducibility

• Frye, SV; Arkin, MR; Arrowsmith, CH; Conn, PJ; Glicksman, MA; Hull-Ryde, EA; Slusher, BS (November 2015). "Tackling reproducibility in academic preclinical drug discovery". Nature Reviews Drug Discovery. 14 (11): 733–4. doi:10.1038/nrd4737. PMID 26388229. S2CID 205478934.
• Marcon, E; et, al. (August 2015). "Assessment of a method to characterize antibody selectivity and specificity for use in immunoprecipitation". Nature Methods. 12 (8): 725–31. doi:10.1038/nmeth.3472. PMID 26121405. S2CID 205423964.
• Laflamme, C; et, al. (October 2019). "Implementation of an antibody characterization procedure and application to the major ALS/FTD disease gene C9ORF72". eLife. 8. doi:10.7554/eLife.48363. PMC 6794092. PMID 31612854. S2CID 204704632.

External links

• Partner List
• Global SGC website
• SGC UNC
• SGC Frankfurt
• SGC Karolinska
• SGC Toronto
• Chemical probe resources: Chemical Probes Portal, Probe Miner, SGC Chemical Probes, SGC Donated Chemical Probes Program
• Chemogenomics: Kinase Chemogenomic Set v1.0
• Centre for Medicines Discovery
• University of Campinas

References

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12. Wells, Carrow I.; Al-Ali, Hassan; Andrews, David M.; Asquith, Christopher R. M.; Axtman, Alison D.; Dikic, Ivan; Ebner, Daniel; Ettmayer, Peter; Fischer, Christian; Frederiksen, Mathias; Futrell, Robert E. (2021-01-08). "The Kinase Chemogenomic Set (KCGS): An Open Science Resource for Kinase Vulnerability Identification". International Journal of Molecular Sciences. 22 (2): 566. doi:10.3390/ijms22020566. ISSN 1422-0067. PMC 7826789. PMID 33429995. https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7826789 ↩

13. Laflamme, Carl; McKeever, Paul M.; Kumar, Rahul; Schwartz, Julie; Kolahdouzan, Mahshad; Chen, Carol X.; You, Zhipeng; Benaliouad, Faiza; Gileadi, Opher; McBride, Heidi M.; Durcan, Thomas M. (15 October 2019). "Implementation of an antibody characterization procedure and application to the major ALS/FTD disease gene C9ORF72". eLife. 8. doi:10.7554/eLife.48363. ISSN 2050-084X. PMC 6794092. PMID 31612854. https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6794092 ↩

14. Ensan, Deeba; Smil, David; Zepeda-Velázquez, Carlos A.; Panagopoulos, Dimitrios; Wong, Jong Fu; Williams, Eleanor P.; Adamson, Roslin; Bullock, Alex N.; Kiyota, Taira; Aman, Ahmed; Roberts, Owen G. (2020-05-14). "Targeting ALK2: An Open Science Approach to Developing Therapeutics for the Treatment of Diffuse Intrinsic Pontine Glioma". Journal of Medicinal Chemistry. 63 (9): 4978–4996. doi:10.1021/acs.jmedchem.0c00395. ISSN 1520-4804. PMC 8213057. PMID 32369358. https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8213057 ↩

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25. Harding, Rachel J.; Ferreira de Freitas, Renato; Collins, Patrick; Franzoni, Ivan; Ravichandran, Mani; Ouyang, Hui; Juarez-Ornelas, Kevin A.; Lautens, Mark; Schapira, Matthieu; von Delft, Frank; Santhakumar, Vjayaratnam (9 November 2017). "Small Molecule Antagonists of the Interaction between the Histone Deacetylase 6 Zinc-Finger Domain and Ubiquitin". Journal of Medicinal Chemistry. 60 (21): 9090–9096. doi:10.1021/acs.jmedchem.7b00933. ISSN 1520-4804. PMID 29019676. /wiki/Doi_(identifier) ↩

26. Ferreira de Freitas, Renato; Harding, Rachel J.; Franzoni, Ivan; Ravichandran, Mani; Mann, Mandeep K.; Ouyang, Hui; Lautens, Mark; Santhakumar, Vijayaratnam; Arrowsmith, Cheryl H.; Schapira, Matthieu (24 May 2018). "Identification and Structure-Activity Relationship of HDAC6 Zinc-Finger Ubiquitin Binding Domain Inhibitors". Journal of Medicinal Chemistry. 61 (10): 4517–4527. doi:10.1021/acs.jmedchem.8b00258. ISSN 1520-4804. PMID 29741882. /wiki/Doi_(identifier) ↩

27. Mann, Mandeep K.; Franzoni, Ivan; de Freitas, Renato Ferreira; Tempel, Wolfram; Houliston, Scott; Smith, Leanna; Vedadi, Masoud; Arrowsmith, Cheryl H.; Harding, Rachel J.; Schapira, Matthieu (27 November 2019). "Discovery of Small Molecule Antagonists of the USP5 Zinc Finger Ubiquitin-Binding Domain" (PDF). Journal of Medicinal Chemistry. 62 (22): 10144–10155. doi:10.1021/acs.jmedchem.9b00988. ISSN 1520-4804. PMID 31663737. S2CID 204975079. https://www.biorxiv.org/content/biorxiv/early/2019/06/22/676668.full.pdf ↩

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29. Knapp, Stefan; Arruda, Paulo; Blagg, Julian; Burley, Stephen; Drewry, David H.; Edwards, Aled; Fabbro, Doriano; Gillespie, Paul; Gray, Nathanael S.; Kuster, Bernhard; Lackey, Karen E. (January 2013). "A public-private partnership to unlock the untargeted kinome". Nature Chemical Biology. 9 (1): 3–6. doi:10.1038/nchembio.1113. ISSN 1552-4469. PMID 23238671. /wiki/Doi_(identifier) ↩

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