Validation of Immunotherapy Response Score as Predictive of Pan-solid Tumor Anti-PD-1/PD-L1 Benefit

Benjamin J Bulen; Nickolay A Khazanov; Daniel H Hovelson; Laura E Lamb; Marc Matrana; Mark E Burkard; Eddy Shih-Hsin Yang; William J Edenfield; Elizabeth Claire Dees; Adedayo A Onitilo; Gary L Buchschacher; Alan M Miller; Benjamin M Parsons; Timothy R Wassenaar; Jennifer M Suga; Robert D Siegel; William Irvin; Suresh Nair; Jennifer N Slim; Jamal Misleh; Jamil Khatri; Gregory A Masters; Sachdev Thomas; Malek M Safa; Daniel M Anderson; Jonathan Mowers; Anna C Dusenbery; Stephanie Drewery; Komal Plouffe; Travis Reeder; Hana Vakil; Lynnae Patrias; Amanda Falzetta; Ryan Hamilton; Kat Kwiatkowski; D Bryan Johnson; Daniel R Rhodes; Scott A Tomlins

doi:10.1158/2767-9764.CRC-23-0036

Validation of Immunotherapy Response Score as Predictive of Pan-solid Tumor Anti-PD-1/PD-L1 Benefit

Cancer Res Commun. 2023 Jul 25;3(7):1335-1349. doi: 10.1158/2767-9764.CRC-23-0036. eCollection 2023 Jul.

Authors

Benjamin J Bulen¹, Nickolay A Khazanov¹, Daniel H Hovelson¹, Laura E Lamb¹, Marc Matrana², Mark E Burkard³, Eddy Shih-Hsin Yang⁴, William J Edenfield⁵, Elizabeth Claire Dees⁶, Adedayo A Onitilo⁷, Gary L Buchschacher⁸, Alan M Miller⁹, Benjamin M Parsons¹⁰, Timothy R Wassenaar¹¹, Jennifer M Suga¹², Robert D Siegel¹³, William Irvin¹⁴, Suresh Nair¹⁵, Jennifer N Slim¹⁶, Jamal Misleh¹⁷, Jamil Khatri¹⁸, Gregory A Masters¹⁹, Sachdev Thomas²⁰, Malek M Safa²¹, Daniel M Anderson²², Jonathan Mowers¹, Anna C Dusenbery¹, Stephanie Drewery¹, Komal Plouffe¹, Travis Reeder¹, Hana Vakil¹, Lynnae Patrias¹, Amanda Falzetta¹, Ryan Hamilton¹, Kat Kwiatkowski¹, D Bryan Johnson¹, Daniel R Rhodes¹, Scott A Tomlins¹

Affiliations

¹ Strata Oncology, Ann Arbor, Michigan.
² Ochsner Cancer Institute, New Orleans, Louisiana.
³ University of Wisconsin Carbone Cancer Center, Madison, Wisconsin.
⁴ O'Neal Comprehensive Cancer Center, University of Alabama at Birmingham School of Medicine, Birmingham, Alabama.
⁵ Prisma Health Greenville Memorial Hospital, Greenville, Carolina.
⁶ UNC Lineberger Comprehensive Cancer Center, Chapel Hill, North Carolina.
⁷ Cancer Care and Research Center, Marshfield Clinic Research Institute, Marshfield, Wisconsin.
⁸ Kaiser Permanente Southern California, Los Angeles, California.
⁹ Translational Drug Development, Scottsdale, Arizona.
¹⁰ Gundersen Health System, La Crosse, Wisconsin.
¹¹ UW Health Cancer Center at ProHealth Care, Waukesha, Wisconsin.
¹² Kaiser Permanente Northern California, Vallejo, California.
¹³ Bon Secours St. Francis Cancer Center, Greenville, Carolina.
¹⁴ Bon Secours Cancer Institute, Midlothian, Virginia.
¹⁵ Lehigh Valley Topper Cancer Institute, Allentown, Pennsylvania.
¹⁶ MultiCare Regional Cancer Center - Tacoma, Washington.
¹⁷ The US Oncology Network, Newark, Delaware.
¹⁸ ChristianaCare Oncology Hematology, Newark, Delaware.
¹⁹ Medical Oncology Hematology Consultants, Helen F Graham Cancer Center and Research Institute, Newark, Delaware.
²⁰ Kaiser Permanente Northern California, Oakland, California.
²¹ Kettering Health, Kettering, Ohio.
²² Metro-Minnesota Community Oncology Research Consortium, St. Louis Park, Minnesota.

Abstract

Immunotherapy response score (IRS) integrates tumor mutation burden (TMB) and quantitative expression biomarkers to predict anti-PD-1/PD-L1 [PD-(L)1] monotherapy benefit. Here, we evaluated IRS in additional cohorts. Patients from an observational trial (NCT03061305) treated with anti-PD-(L)1 monotherapy were included and assigned to IRS-High (-H) versus -Low (-L) groups. Associations with real-world progression-free survival (rwPFS) and overall survival (OS) were determined by Cox proportional hazards (CPH) modeling. Those with available PD-L1 IHC treated with anti-PD-(L)1 with or without chemotherapy were separately assessed. Patients treated with PD-(L)1 and/or chemotherapy (five relevant tumor types) were assigned to three IRS groups [IRS-L divided into IRS-Ultra-Low (-UL) and Intermediate-Low (-IL), and similarly assessed]. In the 352 patient anti-PD-(L)1 monotherapy validation cohort (31 tumor types), IRS-H versus IRS-L patients had significantly longer rwPFS and OS. IRS significantly improved CPH associations with rwPFS and OS beyond microsatellite instability (MSI)/TMB alone. In a 189 patient (10 tumor types) PD-L1 IHC comparison cohort, IRS, but not PD-L1 IHC nor TMB, was significantly associated with anti-PD-L1 rwPFS. In a 1,103-patient cohort (from five relevant tumor types), rwPFS did not significantly differ in IRS-UL patients treated with chemotherapy versus chemotherapy plus anti-PD-(L)1, nor in IRS-H patients treated with anti-PD-(L)1 versus anti-PD-(L)1 + chemotherapy. IRS associations were consistent across subgroups, including both Europeans and non-Europeans. These results confirm the utility of IRS utility for predicting pan-solid tumor PD-(L)1 monotherapy benefit beyond available biomarkers and demonstrate utility for informing on anti-PD-(L)1 and/or chemotherapy treatment.

Significance: This study confirms the utility of the integrative IRS biomarker for predicting anti-PD-L1/PD-1 benefit. IRS significantly improved upon currently available biomarkers, including PD-L1 IHC, TMB, and MSI status. Additional utility for informing on chemotherapy, anti-PD-L1/PD-1, and anti-PD-L1/PD-1 plus chemotherapy treatments decisions is shown.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Biomarkers, Tumor / genetics
Humans
Immunotherapy / methods
Neoplasms* / drug therapy
Progression-Free Survival

Substances

Biomarkers, Tumor