• Media type: E-Article
  • Title: HLA-G and HLA-E Immune Checkpoints Are Widely Expressed in Ewing Sarcoma but Have Limited Functional Impact on the Effector Functions of Antigen-Specific CAR T Cells
  • Contributor: Altvater, Bianca; Kailayangiri, Sareetha; Pérez Lanuza, Lina F.; Urban, Katja; Greune, Lea; Flügge, Maike; Meltzer, Jutta; Farwick, Nicole; König, Simone; Görlich, Dennis; Hartmann, Wolfgang; Rossig, Claudia
  • Published: MDPI AG, 2021
  • Published in: Cancers, 13 (2021) 12, Seite 2857
  • Language: English
  • DOI: 10.3390/cancers13122857
  • ISSN: 2072-6694
  • Origination:
  • Footnote:
  • Description: Immune-inhibitory barriers in the tumor microenvironment of solid cancers counteract effective T cell therapies. Based on our finding that Ewing sarcomas (EwS) respond to chimeric antigen receptor (CAR) gene-modified effector cells through upregulation of human leukocyte antigen G (HLA-G), we hypothesized that nonclassical HLA molecules, HLA-G and HLA-E, contribute to immune escape of EwS. Here, we demonstrate that HLA-G isotype G1 expression on EwS cells does not directly impair cytolysis by GD2-specific CAR T cells (CART), whereas HLA-G1 on myeloid bystander cells reduces CART degranulation responses against EwS cells. HLA-E was induced in EwS cells by IFN-γ stimulation in vitro and by GD2-specific CART treatment in vivo and was detected on tumor cells or infiltrating myeloid cells in a majority of human EwS biopsies. Interaction of HLA-E-positive EwS cells with GD2-specific CART induced upregulation of HLA-E receptor NKG2A. However, HLA-E expressed by EwS tumor cells or by myeloid bystander cells both failed to reduce antitumor effector functions of CART. We conclude that non-classical HLA molecules are expressed in EwS under inflammatory conditions, but have limited functional impact on antigen-specific T cells, arguing against a relevant therapeutic benefit from combining CART therapy with HLA-G or HLA-E checkpoint blockade in this cancer.
  • Access State: Open Access