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Spatial heterogeneity of the T cell receptor repertoire reflects the mutational landscape in lung cancer.

Kroopa JoshiMarc Robert de MassyMazlina IsmailJames L ReadingImran UddinAnnemarie L WoolstonEmine HatipogluTheres OakesRachel RosenthalThomas PeacockTahel RonelMahdad NoursadeghiVirginia TuratiAndrew J S FurnessAndrew GeorgiouYien Ning Sophia WongAssma Ben AissaMariana Werner SunderlandMariam Jamal-HanjaniSelvaraju VeeriahNicolai J BirkbakGareth A WilsonCrispin T HileyEhsan GhoraniJosé Afonso Guerra-AssunçãoJavier HerreroTariq EnverSine Reker HadrupAllan HackshawKarl S PeggsNicholas McGranahanCharles Swantonnull nullSergio A QuezadaBenjamin M Chain
Published in: Nature medicine (2019)
Somatic mutations together with immunoediting drive extensive heterogeneity within non-small-cell lung cancer (NSCLC). Herein we examine heterogeneity of the T cell antigen receptor (TCR) repertoire. The number of TCR sequences selectively expanded in tumors varies within and between tumors and correlates with the number of nonsynonymous mutations. Expanded TCRs can be subdivided into TCRs found in all tumor regions (ubiquitous) and those present in a subset of regions (regional). The number of ubiquitous and regional TCRs correlates with the number of ubiquitous and regional nonsynonymous mutations, respectively. Expanded TCRs form part of clusters of TCRs of similar sequence, suggestive of a spatially constrained antigen-driven process. CD8+ tumor-infiltrating lymphocytes harboring ubiquitous TCRs display a dysfunctional tissue-resident phenotype. Ubiquitous TCRs are preferentially detected in the blood at the time of tumor resection as compared to routine follow-up. These findings highlight a noninvasive method to identify and track relevant tumor-reactive TCRs for use in adoptive T cell immunotherapy.
Keyphrases
  • single cell
  • small cell lung cancer
  • gene expression
  • patient safety
  • cell therapy
  • mesenchymal stem cells
  • bone marrow
  • binding protein
  • dendritic cells
  • tyrosine kinase