Non-classical HLA-class I expression in serous ovarian carcinoma: Correlation with the HLA-genotype, tumor infiltrating immune cells and prognosis

E Andersson, I Poschke, L Villabona, JW Carlson… - …, 2016 - Taylor & Francis
E Andersson, I Poschke, L Villabona, JW Carlson, A Lundqvist, R Kiessling, B Seliger…
Oncoimmunology, 2016Taylor & Francis
In our previous studies, we have shown that patients with serous ovarian carcinoma in
advanced surgical stage disease have a particularly poor prognosis if they carry the HLA-A*
02 genotype. This represent a stronger prognostic factor than loss or downregulation of the
MHC class I heavy chain (HC) on tumor cells. In this study, we investigated the expression of
the non-classical, immune tolerogenic HLA-G and-E on the tumor cells along with the
infiltration of immune cells in the tumor microenvironment. FFPE primary tumors from 72 …
In our previous studies, we have shown that patients with serous ovarian carcinoma in advanced surgical stage disease have a particularly poor prognosis if they carry the HLA-A*02 genotype. This represent a stronger prognostic factor than loss or downregulation of the MHC class I heavy chain (HC) on tumor cells. In this study, we investigated the expression of the non-classical, immune tolerogenic HLA -G and -E on the tumor cells along with the infiltration of immune cells in the tumor microenvironment. FFPE primary tumors from 72 patients with advanced stages of serous adenocarcinoma and metastatic cells present in ascites fluid from 8 additional patients were included in this study. Both expression of HLA-G and aberrant expression of HLA-E were correlated to a significant worse prognosis in patients with HLA-A*02, but not with different HLA genotypes. Focal cell expression of HLA-G correlated to a site-specific downregulation of classical MHC class I HC products and aberrant HLA-E expression, showing a poor survival. HLA-G was more frequently expressed in metastatic cells than in primary tumor lesions and the expression of HLA-G inversely correlated with the frequency of tumor infiltrating immune cells. All these parameters can contribute together to identify and discriminate subpopulations of patients with extremely poor prognosis and can give them the opportunity to receive, and benefit of individually tailored treatments.
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