Frontiers in Immunology (Jan 2018)

Id Proteins Suppress E2A-Driven Invariant Natural Killer T Cell Development prior to TCR Selection

  • Sumedha Roy,
  • Amanda J. Moore,
  • Cassandra Love,
  • Anupama Reddy,
  • Deepthi Rajagopalan,
  • Sandeep S. Dave,
  • Leping Li,
  • Cornelis Murre,
  • Yuan Zhuang

DOI
https://doi.org/10.3389/fimmu.2018.00042
Journal volume & issue
Vol. 9

Abstract

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A family of transcription factors known as E proteins, and their antagonists, Id proteins, regulate T cell differentiation at critical developmental checkpoints. Id proteins promote the differentiation of conventional αβ T cells and suppress the expansion of innate-like αβ T cells known as invariant natural killer T (iNKT) cells. However, it remains to be determined whether Id proteins differentially regulate these distinct lineage choices in early stages of T cell development. In this manuscript, we report that in Id-deficient mice, uninhibited activity of the E protein family member E2A mediates activation of genes that support iNKT cell development and function. There is also biased rearrangement in Id-deficient DP cells that promotes selection into the iNKT lineage in these mice. The observed expansion of iNKT cells is not abrogated by blocking pre-TCR signaling, which is required for conventional αβ T cell development. Finally, E2A is found to be a key transcriptional regulator of both iNKT and γδNKT lineages, which appear to have shared lineage history. Therefore, our study reveals a previously unappreciated role of E2A in coordinating the development of the iNKT lineage at an early stage, prior to their TCR-mediated selection alongside conventional αβ T cells.

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