| Literature DB >> 31700181 |
Diego Chowell1,2, Chirag Krishna3, Federica Pierini4, Vladimir Makarov1,2, Naiyer A Rizvi5, Fengshen Kuo2, Luc G T Morris2,6, Nadeem Riaz2,7, Tobias L Lenz8, Timothy A Chan9,10,11,12.
Abstract
Functional diversity of the highly polymorphic human leukocyte antigen class I (HLA-I) genes underlies successful immunologic control of both infectious disease and cancer. The divergent allele advantage hypothesis dictates that an HLA-I genotype with two alleles with sequences that are more divergent enables presentation of more diverse immunopeptidomes1-3. However, the effect of sequence divergence between HLA-I alleles-a quantifiable measure of HLA-I evolution-on the efficacy of immune checkpoint inhibitor (ICI) treatment for cancer remains unknown. In the present study the germline HLA-I evolutionary divergence (HED) of patients with cancer treated with ICIs was determined by quantifying the physiochemical sequence divergence between HLA-I alleles of each patient's genotype. HED was a strong determinant of survival after treatment with ICIs. Even among patients fully heterozygous at HLA-I, patients with an HED in the upper quartile respond better to ICIs than patients with a low HED. Furthermore, HED strongly impacts the diversity of tumor, viral and self-immunopeptidomes and intratumoral T cell receptor clonality. Similar to tumor mutation burden, HED is a fundamental metric of diversity at the major histocompatibility complex-peptide complex, which dictates ICI efficacy. The data link divergent HLA allele advantage to immunotherapy efficacy and unveil how ICI response relies on the evolved efficiency of HLA-mediated immunity.Entities:
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Year: 2019 PMID: 31700181 PMCID: PMC7938381 DOI: 10.1038/s41591-019-0639-4
Source DB: PubMed Journal: Nat Med ISSN: 1078-8956 Impact factor: 53.440