4.4 Article

An extracellular matrix damage sensor signals through membrane-associated kinase DRL-1 to mediate cytoprotective responses in Caenorhabditis elegans

期刊

GENETICS
卷 220, 期 3, 页码 -

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GENETICS SOCIETY AMERICA
DOI: 10.1093/genetics/iyab217

关键词

stress response; extracellular matrix; cuticle; receptor; signaling; collagen

资金

  1. National Science Foundation [IOS-1120130, IOS-1452948]
  2. William Townsend Porter Fellowship - American Physiological Society

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The study identified collagen bands outside the annular furrows as key components of a damage sensor in the cuticle of Caenorhabditis elegans. It found that the protein kinase DRL-1 plays a crucial role in regulating cytoprotective gene expression and stress resistance in mutant worms lacking extracellular proteins.
We and others previously identified circumferential bands of collagen named annular furrows as key components of a damage sensor in the cuticle of Caenorhabditis elegans that regulates cytoprotective genes. Mutation or loss of noncollagen secreted proteins OSM-7, OSM-8, and OSM-11 activate the same cytoprotective responses without obvious changes to the cuticle indicating that other extracellular proteins are involved. Here, we used RNAi screening to identify protein kinase DRL-1 as a key modulator of cytoprotective gene expression and stress resistance in furrow and extracellular OSM protein mutants. DRL-1 functions downstream from furrow disruption and is expressed in cells that induce cytoprotective genes. DRL-1 is not required for the expression of cytoprotective genes under basal or oxidative stress conditions consistent with specificity to extracellular signals. DRL-1 was previously shown to regulate longevity via a Dietary Restriction-Like state, but it functions downstream from furrow disruption by a distinct mechanism. The kinase domain of DRL-1 is related to mammalian MEKK3, and MEKK3 is recruited to a plasma membrane osmosensor complex by a scaffold protein. In C. elegans, DRL-1 contains an atypical hydrophobic C-terminus with predicted transmembrane domains and is constitutively expressed at or near the plasma membrane where it could function to receive extracellular damage signals for cells that mount cytoprotective responses.

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