Regulation of mRNA translation is widespread and essential for cellular and organismal processes. However, its role in immunity remains poorly explored. Human T cells provide an excellent model to investigate this frontier in molecular immunology. They are readily available in sufficient quantities, can be stimulated in a physiologically relevant manner, and are genetically accessible. I propose to study translational control in T cells from healthy donors and patients with monogenic inborn errors affecting translation reinitiation. Specifically, I hypothesize that (I) translational regulation mediates specialized T cell functions, (II) T cell-specific 5’TOP mRNAs drive T cell function in an mTOR-dependent manner, and (III) MCTS1-dependent translation of ATF4 contributes to T cell function. My recent publication identifying X-linked recessive MCTS1 deficiency as a novel genetic cause of susceptibility to mycobacterial infections highlights the scientific significance and potential of these questions. To address these hypotheses, I outline a research program that leverages state-of-the-art molecular biology techniques to investigate translational control in T cells. The proposal is supported by extensive preliminary data, reducing the risk associated with these studies. This program will provide fundamental insights into regulated mRNA translation in T cells, pave the way for improved T cell function in cell therapies such as CAR T cells, and establish the foundation for my broader investigation into mRNA translation in human immunity.

DFG Programme Emmy Noether Independent Junior Research Groups

International Connection Belgium, China, Iran, Oman, USA

Cooperation Partners Professor Dr. Hassan Abolhassani; Professorin Dr. Ilaria Elia; Dr. Tariq Al Farsi; Professorin Dr. Lulu Tsao; Dr. Qinhua Zhou