| Literature DB >> 30248181 |
Sarah Harris-Bookman1, Dimitrios Mathios1, Allison M Martin2, Yuanxuan Xia1, Eileen Kim1, Haiying Xu3, Zineb Belcaid1, Magdalena Polanczyk2, Theresa Barberi2, Debebe Theodros2, Jennifer Kim1, Janis M Taube3, Peter C Burger4, Mark Selby5, Corina Taitt5, Alan Korman5, Xiaobu Ye1, Charles G Drake6, Henry Brem1, Drew M Pardoll2,7, Michael Lim1.
Abstract
Like in many tumor types, immunotherapy is currently under investigation to assess its potential efficacy in glioblastoma patients. Trials are under way to assess the efficacy of new immune checkpoint inhibitors including anti-PD-1 or CTLA4. We here investigate the expression and efficacy of a novel immune-checkpoint inhibitor, called LAG-3. We show that LAG-3 is expressed in human glioblastoma samples and in a mouse glioblastoma model we show that knock out or LAG-3 inhibition with a blocking antibody is efficacious against glioblastoma and can be used in combination with other immune checkpoint inhibitors toward complete eradication of the model glioblastoma tumors. From a mechanistic standpoint we show that LAG-3 expression is an early marker of T cell exhaustion and therefore early treatment with LAG-3 blocking antibody is more efficacious than later treatment. These data provide insight and support the design of trials that incorporate LAG-3 in the treatment of glioblastoma.Entities:
Keywords: IFN-γ; T cell exhaustion; anti-LAG-3; anti-PD-1; glioblastoma
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Year: 2018 PMID: 30248181 PMCID: PMC7105259 DOI: 10.1002/ijc.31661
Source DB: PubMed Journal: Int J Cancer ISSN: 0020-7136 Impact factor: 7.396