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BLMP-1 promotes developmental cell death in C. elegans by timely repression of ced-9 transcription.


ABSTRACT: Programmed cell death (PCD) is a common cell fate in metazoan development. PCD effectors are extensively studied, but how they are temporally regulated is less understood. Here, we report a mechanism controlling tail-spike cell death onset during Caenorhabditis elegans development. We show that the zinc-finger transcription factor BLMP-1, which controls larval development timing, also regulates embryonic tail-spike cell death initiation. BLMP-1 functions upstream of CED-9 and in parallel to DRE-1, another CED-9 and tail-spike cell death regulator. BLMP-1 expression is detected in the tail-spike cell shortly after the cell is born, and blmp-1 mutations promote ced-9-dependent tail-spike cell survival. BLMP-1 binds ced-9 gene regulatory sequences, and inhibits ced-9 transcription just before cell-death onset. BLMP-1 and DRE-1 function together to regulate developmental timing, and their mammalian homologs regulate B-lymphocyte fate. Our results, therefore, identify roles for developmental timing genes in cell-death initiation, and suggest conservation of these functions.

SUBMITTER: Jiang HS 

PROVIDER: S-EPMC8572009 | biostudies-literature | 2021 Oct

REPOSITORIES: biostudies-literature

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BLMP-1 promotes developmental cell death in C. elegans by timely repression of ced-9 transcription.

Jiang Hang-Shiang HS   Ghose Piya P   Han Hsiao-Fen HF   Wu Yun-Zhe YZ   Tsai Ya-Yin YY   Lin Huang-Chin HC   Tseng Wei-Chin WC   Wu Jui-Ching JC   Shaham Shai S   Wu Yi-Chun YC  

Development (Cambridge, England) 20211022 20


Programmed cell death (PCD) is a common cell fate in metazoan development. PCD effectors are extensively studied, but how they are temporally regulated is less understood. Here, we report a mechanism controlling tail-spike cell death onset during Caenorhabditis elegans development. We show that the zinc-finger transcription factor BLMP-1, which controls larval development timing, also regulates embryonic tail-spike cell death initiation. BLMP-1 functions upstream of CED-9 and in parallel to DRE-  ...[more]

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