Immune-related events in individuals with solid tumors on immunotherapy associate with Th17 and Th2 signatures

Chester Kao; Soren Charmsaz; Stephanie Alden; Madelena Brancati; Howard L. Li; Aanika Balaji; Kabeer Munjal; Kathryn L. Howe; Sarah Mitchell; James M. Leatherman; Ervin Griffin; Mari Nakazawa; Hua‐Ling Tsai; Ludmila Danilova; Christopher J. Thoburn; Jennifer Gizzi; Nicole Groß; Alexei Hernandez; Erin M. Coyne; Sarah M. Shin; Jayalaxmi Suresh Babu; George W. Apostol; Jennifer N. Durham; Brian J. Christmas; Maximilian F. Konig; Evan J. Lipson; Jarushka Naidoo; Laura C. Cappelli; Aliyah Pabani; Yasser Ged; Marina Baretti; Julie R. Brahmer; Jean Hoffman‐Censits; Tanguy Y. Seiwert; Rachel Garonce-Hediger; Aditi Guha; Sanjay Bansal; Laura Tang; Elizabeth M. Jaffee; G. Scott Chandler; Rajat Mohindra; Won Jin Ho; Mark Yarchoan

doi:10.1172/jci176567

Immune-related events in individuals with solid tumors on immunotherapy associate with Th17 and Th2 signatures

Chester Kao(Sidney Kimmel Comprehensive Cancer Center), Soren Charmsaz(Sidney Kimmel Comprehensive Cancer Center), Stephanie Alden(Johns Hopkins University), Madelena Brancati(Sidney Kimmel Comprehensive Cancer Center), Howard L. Li(Johns Hopkins University), Aanika Balaji(Johns Hopkins University), Kabeer Munjal(Sidney Kimmel Comprehensive Cancer Center), Kathryn L. Howe(Sidney Kimmel Comprehensive Cancer Center), Sarah Mitchell(Sidney Kimmel Comprehensive Cancer Center), James M. Leatherman(Sidney Kimmel Comprehensive Cancer Center), Ervin Griffin(Sidney Kimmel Comprehensive Cancer Center), Mari Nakazawa(Sidney Kimmel Comprehensive Cancer Center), Hua‐Ling Tsai(Johns Hopkins University), Ludmila Danilova(Bloomberg (United States)), Christopher J. Thoburn(Johns Hopkins University), Jennifer Gizzi(Johns Hopkins University), Nicole Groß(Sidney Kimmel Comprehensive Cancer Center), Alexei Hernandez(Sidney Kimmel Comprehensive Cancer Center), Erin M. Coyne(Sidney Kimmel Comprehensive Cancer Center), Sarah M. Shin(Sidney Kimmel Comprehensive Cancer Center), Jayalaxmi Suresh Babu(Sidney Kimmel Comprehensive Cancer Center), George W. Apostol(Sidney Kimmel Comprehensive Cancer Center), Jennifer N. Durham(Sidney Kimmel Comprehensive Cancer Center), Brian J. Christmas(Sidney Kimmel Comprehensive Cancer Center), Maximilian F. Konig(Johns Hopkins University), Evan J. Lipson(Johns Hopkins University), Jarushka Naidoo(Johns Hopkins University), Laura C. Cappelli(Johns Hopkins University), Aliyah Pabani(Johns Hopkins University), Yasser Ged(Johns Hopkins University), Marina Baretti(Johns Hopkins University), Julie R. Brahmer(Bloomberg (United States)), Jean Hoffman‐Censits(Johns Hopkins University), Tanguy Y. Seiwert(Johns Hopkins University), Rachel Garonce-Hediger(Roche (Switzerland)), Aditi Guha(General Tire (United States)), Sanjay Bansal(General Tire (United States)), Laura Tang(General Tire (United States)), Elizabeth M. Jaffee(Bloomberg (United States)), G. Scott Chandler(Roche (Switzerland)), Rajat Mohindra(Roche (Switzerland)), Won Jin Ho(Johns Hopkins University), Mark Yarchoan(Bloomberg (United States))

Journal of Clinical Investigation

August 29, 2024

10.1172/jci176567

Cited by 24Open Access

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Abstract

BACKGROUNDImmune-related adverse events (irAEs) and their associated morbidity/mortality are a key concern for patients receiving immune checkpoint inhibitors (ICIs). Prospective evaluation of the drivers of irAEs in a diverse pan-tumor cohort is needed to identify patients at greatest risk and to develop rational treatment and interception strategies.METHODSIn an observational study, we prospectively collected blood samples and performed regular clinical evaluations for irAEs in patients receiving ICI therapy as standard of care for solid tumors. We performed in-parallel analysis of cytokines by Luminex immunoassay and circulating immune cells by cytometry by time-of-flight (CyTOF) at baseline and on treatment to investigate mechanisms of irAEs.RESULTSWe enrolled 111 patients, of whom 40.5% developed a symptomatic irAE (grade ≥ 2). Development of a grade ≥ 2 irAE was positively associated with the use of combination ICI and a history of an autoimmune disorder. Early changes in T helper 17 (Th17) (IL-6, IL-17f), type 2 (IL-5, IL-13, IL-25), and type 1 (TNF-α) cytokine signatures and congruent on-treatment expansions of Th17 and Th2 effector memory (Th2EM) T cell populations in peripheral blood were positively associated with the development of grade ≥2 irAEs. IL-6 levels were also associated with inferior cancer-specific survival and overall survival.CONCLUSIONSIn a diverse, prospective pan-tumor cohort, Th17 and Th2 skewing during early ICI treatment was associated with the development of clinically relevant irAEs but not antitumor responses, providing possible targets for monitoring and therapeutic interventions.FUNDINGJohns Hopkins Bloomberg-Kimmel Institute for Cancer Immunotherapy, the NCI SPORE in Gastrointestinal Cancers (P50 CA062924), NCI grant (R50CA243627 to LD), the NIH Center Core Grant (P30 CA006973), Swim Across America (to MY), NIAMS (K23AR075872 to LC), and imCORE-Genentech grant 137515 (to Johns Hopkins Medicine on behalf of MY).

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