| Literature DB >> 19531354 |
J Thomas Hannich1, Eugeni V Entchev, Fanny Mende, Hristio Boytchev, René Martin, Vyacheslav Zagoriy, Gabriele Theumer, Isabelle Riezman, Howard Riezman, Hans-Joachim Knölker, Teymuras V Kurzchalia.
Abstract
In response to pheromone(s), Caenorhabditis elegans interrupts its reproductive life cycle and enters diapause as a stress-resistant dauer larva. This decision is governed by a complex system of neuronal and hormonal regulation. All the signals converge onto the nuclear hormone receptor DAF-12. A sterol-derived hormone, dafachronic acid (DA), supports reproductive development by binding to DAF-12 and inhibiting its dauer-promoting activity. Here, we identify a methyltransferase, STRM-1, that modulates DA levels and thus dauer formation. By modifying the substrates that are used for the synthesis of DA, STRM-1 can reduce the amount of hormone produced. Loss of STRM-1 function leads to elevated levels of DA and inefficient dauer formation. Sterol methylation was not previously recognized as a mechanism for regulating hormone activity. Moreover, the C-4 sterol nucleus methylation catalyzed by STRM-1 is unique to nematodes and thus could be a target for therapeutic strategies against parasitic nematode infections.Entities:
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Year: 2009 PMID: 19531354 DOI: 10.1016/j.devcel.2009.04.012
Source DB: PubMed Journal: Dev Cell ISSN: 1534-5807 Impact factor: 12.270