4.6 Article

VISTA+/CD8+status correlates with favorable prognosis in Epithelial ovarian cancer

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PLOS ONE
Volume 18, Issue 3, Pages -

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PUBLIC LIBRARY SCIENCE
DOI: 10.1371/journal.pone.0278849

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Immunotherapy targeting immune checkpoint regulators, such as VISTA, has shown promise as a new treatment option for certain cancers. This study investigated the role of VISTA in epithelial ovarian cancer (EOC) and its relationship with tumor-infiltrating lymphocytes (TILs) markers and prognosis. The expression of VISTA and TILs markers was evaluated in EOC tissue samples, and the association with clinicopathological variables and overall survival (OS) was analyzed. Results showed that VISTA expression was significantly associated with a high density of TILs, particularly CD8+ TILs, in immune cells (ICs). Furthermore, a subtype characterized by dual positive VISTA+/CD8+ was associated with prolonged OS in both tumor cells (TCs) and ICs. These findings suggest that VISTA could be a potential immunotherapeutic target in EOC.
Immunotherapy by blocking immune checkpoint regulators has emerged as a new targeted therapy for some cancers. Among them V-domain Ig suppressor of Tcell activation (VISTA) which is identified as a novel checkpoint regulator in ovarian cancer. This study aimed to investigate the VISTA role in Epithelial ovarian cancer (EOC), and its relationship with tumor-infiltrating lymphocytes (TILs) markers and its prognostic value. The expression of VISTA, CD3, CD8, CD4, FOXP3, and CD56 was assessed in 168 EOC tissue microarrays (TMA) by immunohistochemistry (IHC). In addition, associations between VISTA, TILs, clinicopathological variables, and overall survival (OS) were analyzed. VISTA expression in IGRov1 cells, as well as in PBMC of EOC patient, was evaluated by western blot. VISTA expression was detected in 64,28% of tissues, among which 42.3% were positive for tumor cells (TCs), and 47,9% were positive for immune cells (ICs). In univariate analysis, VISTA expression was significantly associated with a high density of TILs:CD3+ (p = 0,001), CD4+ (p = 0,002) and CD8+ (p <= 0,001), in ICs but not in TCs. In terms of OS, multivariate analysis showed a significant association between the high density of CD8+ TILs and VISTA positive staining in ICs (p = 0,044), but not in TCs (p = 0,108). Kaplan-Meier curves demonstrated no correlation between VISTA expression and prolonged OS in both ICs (p = 0,841) and TCs (p = 0,090). Classification of EOC tumor microenvironment based on VISTA and CD8+TILs expression, demonstrated four immune subtypes: VISTA+/CD8+, VISTA+/CD8-, VISTA-/CD8+ and VISTA-/CD8-. The dual positive VISTA+/CD8+ subtype was significantly associated with prolonged OS in both TCs and ICs (p = 0,012 and p <= 0,01, respectively), whereas patients with VISTA+/CD8- had the worst OS. Our results showed that VISTA is highly expressed in the IGRov1 cell line and LT-CD8 from a patient with EOC. Our results highlighted the association of VISTA expression and CD8+ TILs in EOC, with prolonged OS in patients with VISTA+/CD8+ and proposed VISTA as a potential immunotherapeutic target in EOC.

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