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Role of the SET-like domain of Blimp-1 in plasma cell function and Immunoglobulin secretion

$235,500R21FY2018AINIH

University Of California At Davis, Davis CA

Investigators

Abstract

PROJECT SUMMARY Protective antibody responses depend upon secreted immunoglobulin. This is regulated in a stage-specific manner upon the differentiation of B cell blasts into plasma cells and depends on the upregulation of the Blimp-1 transcription factor. Blimp-1 orchestrates the plasma cell gene program that includes the regulation of genes important for secretion of large quantities of immunoglobulin, i.e. post-translational regulation. Blimp-1 is also necessary for post- transcriptional regulation of the immunoglobulin heavy chain primary transcript by somehow affecting the competing alternative splicing and alternative poly-adenylation reactions at play on this transcript. Using a structure-function approach, I had found a novel domain of Blimp-1, that exhibits a high degree of structural similarity to lysine-methyltransferase (SET) domains, to be essential for post-transcriptional regulation of the immunoglobulin primary transcript but not for post-translational regulation of immunoglobulin secretion. This proposal aims to elucidate the role of this domain in post-transcriptional regulation of the immunoglobulin transcript and perhaps other such regulated transcripts important for plasma cell biology. Furthermore, we will explore the possibility that methyltransferase activity of Blimp-1 plays a critical role in this process.

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