Genomic, immunologic, and prognostic associations of TROP2 (TACSTD2) expression in solid tumors.

Publication Title

The oncologist

Authors

Dan Morgenstern-Kaplan
Samuel A Kareff
Asaad Trabolsi
Estelamari Rodriguez
Harris Krause
Jennifer R Ribeiro
Heng Tan
Emmanuel S Antonarakis
Emil Lou
Misako Nagasaka
Sandra Algaze
Heinz-Josef Lenz
Stephen V Liu
Balazs Halmos
Dave S B Hoon, Saint John's Cancer Institute, Providence Health System, Santa Monica, CA 90404, United States.Follow
Andreas Seeber
Patrick C Ma
Wafik S El-Deiry
Ari M Vanderwalde
Gilberto Lopes

Document Type

Article

Publication Date

7-10-2024

Keywords

TROP2; precision oncology; targeted therapy; tumor genetics.; california; santa monica; genomics; sjci

Abstract

BACKGROUND: TROP2 (TACSTD2) expression is associated with decreased overall survival (OS) in some solid tumors, and the TROP2-targeting antibody-drug conjugate (ADC) sacituzumab govitecan has been approved in breast and urothelial carcinomas. We aimed to explore the multi-omic landscape associated with TACSTD2 gene expression in various solid tumors to identify patients most likely to benefit from this approach.

METHODS: Breast (N = 11 246), colorectal (N = 15 425), hepatocellular (N = 433), pancreatic (N = 5488), and urothelial (N = 4125) tumors were stratified into quartiles by TACSTD2 gene expression, analyzed by next-generation DNA sequencing, whole transcriptome sequencing, and immunohistochemistry at Caris Life Sciences (Phoenix, AZ). Survival data were obtained from insurance claims, and Kaplan-Meier estimates were calculated for molecularly defined cohorts.

RESULTS: Several pathogenic mutations were associated with TACSTD2-high tumors, including TP53 in breast, colorectal (CRC), pancreatic, and hepatocellular cancers; KRAS in pancreatic and CRC cancers; ARID1A and FGFR3 in urothelial cancer; and CTNNB1 in hepatocellular cancer. TACSTD2-low breast tumors were enriched for copy number amplifications in CCND1 and FGF/R family member genes. TACSTD2 high was generally associated with more immune cell infiltration and greater T-cell inflammation scores. Patients with TACSTD2-high breast, CRC, and pancreatic cancers demonstrated a significantly shorter OS than TACSTD2-low tumors. This was restricted to CRC with microsatellite stable tumors and patients with pancreatic cancer with KRAS-mutant tumors. Patients with breast cancer with TACSTD2-high tumors also experienced significantly worse OS following immune checkpoint inhibitors.

CONCLUSIONS: TACSTD2 expression is associated with key driver alterations and a more active immune microenvironment, suggesting possible combinatorial strategies with TROP2-targeting ADCs plus immunotherapy in various solid tumors.

Clinical Institute

Cancer

Specialty/Research Institute

Oncology

DOI

10.1093/oncolo/oyae168