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Clonal dynamics underlying the skewed CD4/CD8 ratio of mouse thymocytes revealed by TCR-independent barcoding.


ABSTRACT: T cell differentiation in the thymus generates CD4+ helper and cytotoxic CD8+ cells as the two principal T cell lineages. Curiously, at the end of this complex selection process, CD4+ cells invariably outnumber CD8+ cells. Here, we examine the dynamics of repertoire formation and the emergence of the skewed CD4/CD8 ratio using high-resolution endogenous CRISPR/Cas9 barcoding that indelibly marks immature T cells at the DN2/DN3 pre-TCR stage. In wild-type mice, greater clone size of CD4+ cells and an intrinsically greater probability of Tcr β clonotypes for pMHCII interactions are major contributors to the skewed CD4/CD8 ratio. Clonal perturbations of thymocyte differentiation following the precocious expression of a rearranged iNKT invariant TCR α chain are due to loss of Tcr β clonotypes from the CD4 lineage-committed pre-selection repertoire. The present barcoding scheme offers a novel means to examine the clonal dynamics of lymphocyte differentiation orthogonal to that using TCR clonotypes.

SUBMITTER: Iwanami N 

PROVIDER: S-EPMC9445074 | biostudies-literature | 2022 Sep

REPOSITORIES: biostudies-literature

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Clonal dynamics underlying the skewed CD4/CD8 ratio of mouse thymocytes revealed by TCR-independent barcoding.

Iwanami Norimasa N   Petersen Malte M   Diekhoff Dagmar D   Boehm Thomas T  

Communications biology 20220905 1


T cell differentiation in the thymus generates CD4<sup>+</sup> helper and cytotoxic CD8<sup>+</sup> cells as the two principal T cell lineages. Curiously, at the end of this complex selection process, CD4<sup>+</sup> cells invariably outnumber CD8<sup>+</sup> cells. Here, we examine the dynamics of repertoire formation and the emergence of the skewed CD4/CD8 ratio using high-resolution endogenous CRISPR/Cas9 barcoding that indelibly marks immature T cells at the DN2/DN3 pre-TCR stage. In wild-ty  ...[more]

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