Prevalence and clinical implications of T-cell immunoglobulin mucin type-1 (TIM-1) in multiple tumor types.

Abstract

34 Background: TIM-1 (KIM-1, HAVcr-1) is a type 1 transmembrane glycoprotein. Expression is limited in healthy tissues but upregulated after kidney injury, in ovarian cancer and renal cell carcinoma (RCC). TIM-1 is associated with a more malignant RCC phenotype and immune response regulation. CDX-014, an antibody drug conjugate, contains a fully human IgG1 monoclonal antibody (mAb) conjugated to the potent cytotoxin MMAE. CDX-014 is in a Ph 1/2 trial for RCC (NCT02837991). The prevalence of TIM-1 in other cancers was investigated to explore the broader potential for CDX-014. Methods: Tumors and normal adjacent tissues (NAT) were provided (Mosaic Labs) via IRB-reviewed protocol MOS001 for in vitro analysis of remnant, anonymized human samples. The study included 188 tumors: 30 renal, 45 ovarian, 34 endometrial, 2 cervical, 2 vaginal, 15 bile duct, 15 CRC, 30 NSCLC and 15 thymoma plus 75 NAT. Mosaic performed a validated immunohistochemistry assay on FFPE tissues. A FITC-conjugated, anti-TIM-1 mAb was applied after slide deparaffinization and antigen retrieval. Anti-FITC (Novus Bio), Envision+ HRP and DAB (Dako) were used for visualization. A pathologist scored hematoxylin-counterstained slides for % positive cells and staining intensity. A cut-off of > 2% of cells staining at any intensity was deemed positive. Results: TIM-1 was universally prevalent in renal papillary (14/14) and clear cell carcinoma (CCC [13/13]) plus vaginal CCC (2/2). TIM-1 was also seen in ovarian CCC (12/15; 80%), endometrial CCC (9/21; 43%), adeno NSCLC (2/15; 13%), serous ovarian (1/10; 10%), adeno endometrial (1/13; 8%) and CRC (1/15; 7%). There was no staining in chromophobe RCC (3/3), cervical CCC, endometrioid or mucinous ovarian (10 each), bile duct carcinoma, squamous NSCLC or thymoma. There was minimal to no TIM-1 in NAT except for 7/10 kidney samples (possibly from unappreciated kidney injury). Conclusions: The data suggest that in addition to renal and ovarian cancer, TIM-1 targeted therapy such as CDX-014 warrants exploration in patients with endometrial CCC, vaginal CCC and adeno NCSLC. These results support the ongoing first in human Ph 1/2 study in RCC and potential broader clinical development of CDX-014 in other indications.