Autoimmune genetic risk variants as germline biomarkers of response to melanoma immune-checkpoint inhibition

被引:0
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作者
Vylyny Chat
Robert Ferguson
Danny Simpson
Esther Kazlow
Rebecca Lax
Una Moran
Anna Pavlick
Dennie Frederick
Genevieve Boland
Ryan Sullivan
Antoni Ribas
Keith Flaherty
Iman Osman
Jeffrey Weber
Tomas Kirchhoff
机构
[1] New York University School of Medicine,Laura and Issac Perlmutter Cancer Center
[2] New York University School of Medicine,Departments of Population Health and Environmental Medicine
[3] New York University School of Medicine,The Interdisciplinary Melanoma Cooperative Group
[4] New York University School of Medicine,Department of Medicine
[5] New York University,Ronald O. Perelman, Department of Dermatology
[6] Massachusetts General Hospital Cancer Center,Center for Melanoma
[7] Harvard Medical School,Division of Hematology
[8] University of California Los Angeles,Oncology, Department of Medicine
来源
关键词
Autoimmunity; Germline variants; Immune-checkpoint inhibition; Melanoma;
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摘要
Immune-checkpoint inhibition (ICI) treatments improve outcomes for metastatic melanoma; however, > 60% of treated patients do not respond to ICI. Current biomarkers do not reliably explain ICI resistance. Given the link between ICI and autoimmunity, we investigated if genetic susceptibility to autoimmunity modulates ICI efficacy. In 436 patients with metastatic melanoma receiving single line ICI or combination treatment, we tested 25 SNPs, associated with > 2 autoimmune diseases in recent genome-wide association studies, for modulation of ICI efficacy. We found that rs17388568—a risk variant for allergy, colitis and type 1 diabetes—was associated with increased anti-PD-1 response, with significance surpassing multiple testing adjustments (OR 0.26; 95% CI 0.12–0.53; p = 0.0002). This variant maps to a locus of established immune-related genes: IL2 and IL21. Our study provides first evidence that autoimmune genetic susceptibility may modulate ICI efficacy, suggesting that systematic testing of autoimmune risk loci could reveal personalized biomarkers of ICI response.
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页码:897 / 905
页数:8
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