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Human Genetics in Rheumatoid Arthritis Guides a High-Throughput Drug Screen of the CD40 Signaling Pathway
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نویسنده
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li g. ,diogo d. ,wu d. ,spoonamore j. ,dancik v. ,franke l. ,kurreeman f. ,rossin e.j. ,duclos g. ,hartland c. ,zhou x. ,li k. ,liu j. ,de jager p.l. ,siminovitch k.a. ,zhernakova a. ,raychaudhuri s. ,bowes j. ,eyre s. ,padyukov l. ,gregersen p.k. ,worthington j. ,gupta n. ,clemons p.a. ,stahl e. ,tolliday n. ,plenge r.m.
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منبع
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plos genetics - 2013 - دوره : 9 - شماره : 5
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چکیده
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Although genetic and non-genetic studies in mouse and human implicate the cd40 pathway in rheumatoid arthritis (ra),there are no approved drugs that inhibit cd40 signaling for clinical care in ra or any other disease. here,we sought to understand the biological consequences of a cd40 risk variant in ra discovered by a previous genome-wide association study (gwas) and to perform a high-throughput drug screen for modulators of cd40 signaling based on human genetic findings. first,we fine-map the cd40 risk locus in 7,222 seropositive ra patients and 15,870 controls,together with deep sequencing of cd40 coding exons in 500 ra cases and 650 controls,to identify a single snp that explains the entire signal of association (rs4810485,p = 1.4×10-9). second,we demonstrate that subjects homozygous for the ra risk allele have ∼33% more cd40 on the surface of primary human cd19+ b lymphocytes than subjects homozygous for the non-risk allele (p = 10-9),a finding corroborated by expression quantitative trait loci (eqtl) analysis in peripheral blood mononuclear cells from 1,469 healthy control individuals. third,we use retroviral shrna infection to perturb the amount of cd40 on the surface of a human b lymphocyte cell line (bl2) and observe a direct correlation between amount of cd40 protein and phosphorylation of rela (p65),a subunit of the nf-κb transcription factor. finally,we develop a high-throughput nf-κb luciferase reporter assay in bl2 cells activated with trimerized cd40 ligand (tcd40l) and conduct an hts of 1,982 chemical compounds and fda-approved drugs. after a series of counter-screens and testing in primary human cd19+ b cells,we identify 2 novel chemical inhibitors not previously implicated in inflammation or cd40-mediated nf-κb signaling. our study demonstrates proof-of-concept that human genetics can be used to guide the development of phenotype-based,high-throughput small-molecule screens to identify potential novel therapies in complex traits such as ra. © 2013 li et al.
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آدرس
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division of rheumatology,immunology,and allergy and division of genetics,brigham and women's hospital,harvard medical school,boston,ma, United States, division of rheumatology,immunology,and allergy and division of genetics,brigham and women's hospital,harvard medical school,boston,ma,united states,medical and population genetics program,chemical biology program,broad institute,cambridge,ma, United States, division of rheumatology,immunology,and allergy and division of genetics,brigham and women's hospital,harvard medical school,boston,ma,united states,medical and population genetics program,chemical biology program,broad institute,cambridge,ma,united states,department of statistics,harvard university,cambridge,ma, United States, chemical biology platform,broad institute,cambridge,ma, United States, chemical biology program,broad institute,cambridge,ma, United States, department of genetics,university medical center groningen and university of groningen,groningen, Netherlands, division of rheumatology,immunology,and allergy and division of genetics,brigham and women's hospital,harvard medical school,boston,ma,united states,medical and population genetics program,chemical biology program,broad institute,cambridge,ma, United States, medical and population genetics program,chemical biology program,broad institute,cambridge,ma,united states,biological and biomedical sciences program,health sciences and technology program,harvard medical school,boston,ma,united states,analytical and translational genetics unit,massachusetts general hospital,boston,ma, United States, division of rheumatology,immunology,and allergy and division of genetics,brigham and women's hospital,harvard medical school,boston,ma, United States, chemical biology platform,broad institute,cambridge,ma, United States, school of computer and information technology,beijing jiaotong university,beijing, China, chemical biology program,broad institute,cambridge,ma, United States, department of statistics,harvard university,cambridge,ma, United States, medical and population genetics program,chemical biology program,broad institute,cambridge,ma,united states,program in translational neuropsychiatric genomics,institute for the neurosciences department of neurology,brigham and women's hospital,boston,ma, United States, department of medicine,university of toronto,toronto,on,canada,mount sinai hospital,samuel lunenfeld research institute and toronto general research institute,toronto,on, Canada, department of genetics,university medical center groningen and university of groningen,groningen,netherlands,department of rheumatology,leiden university medical centre,leiden, Netherlands, division of rheumatology,immunology,and allergy and division of genetics,brigham and women's hospital,harvard medical school,boston,ma,united states,medical and population genetics program,chemical biology program,broad institute,cambridge,ma, United States, arthritis research uk epidemiology unit,musculoskeletal research group,university of manchester,manchester academic health sciences centre,manchester,united kingdom,nihr manchester musculoskeletal biomedical research unit,central manchester nhs foundation trust,manchester academic health sciences centre,manchester, United Kingdom, arthritis research uk epidemiology unit,musculoskeletal research group,university of manchester,manchester academic health sciences centre,manchester,united kingdom,nihr manchester musculoskeletal biomedical research unit,central manchester nhs foundation trust,manchester academic health sciences centre,manchester, United Kingdom, rheumatology unit,department of medicine,karolinska institutet and karolinska university hospital solna,stockholm, Sweden, the feinstein institute for medical research,north shore-long island jewish health system,manhasset,ny, United States, arthritis research uk epidemiology unit,musculoskeletal research group,university of manchester,manchester academic health sciences centre,manchester,united kingdom,nihr manchester musculoskeletal biomedical research unit,central manchester nhs foundation trust,manchester academic health sciences centre,manchester, United Kingdom, medical and population genetics program,chemical biology program,broad institute,cambridge,ma, United States, chemical biology program,broad institute,cambridge,ma, United States, division of rheumatology,immunology,and allergy and division of genetics,brigham and women's hospital,harvard medical school,boston,ma,united states,medical and population genetics program,chemical biology program,broad institute,cambridge,ma, United States, chemical biology platform,broad institute,cambridge,ma, United States, division of rheumatology,immunology,and allergy and division of genetics,brigham and women's hospital,harvard medical school,boston,ma,united states,medical and population genetics program,chemical biology program,broad institute,cambridge,ma, United States
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