| Literature DB >> 12110170 |
Ross Francis1, Garth McGrath, Jianhuan Zhang, David A Ruddy, Mary Sym, Javier Apfeld, Monique Nicoll, Mark Maxwell, Bing Hai, Michael C Ellis, Annette L Parks, Wei Xu, Jinhe Li, Mark Gurney, Richard L Myers, Carol S Himes, Ronald Hiebsch, Cara Ruble, Jeffrey S Nye, Daniel Curtis.
Abstract
Presenilins are components of the gamma-secretase protein complex that mediates intramembranous cleavage of betaAPP and Notch proteins. A C. elegans genetic screen revealed two genes, aph-1 and pen-2, encoding multipass transmembrane proteins, that interact strongly with sel-12/presenilin and aph-2/nicastrin. Human aph-1 and pen-2 partially rescue the C. elegans mutant phenotypes, demonstrating conserved functions. The human genes must be provided together to rescue the mutant phenotypes, and the inclusion of presenilin-1 improves rescue, suggesting that they interact closely with each other and with presenilin. RNAi-mediated inactivation of aph-1, pen-2, or nicastrin in cultured Drosophila cells reduces gamma-secretase cleavage of betaAPP and Notch substrates and reduces the levels of processed presenilin. aph-1 and pen-2, like nicastrin, are required for the activity and accumulation of gamma-secretase.Entities:
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Year: 2002 PMID: 12110170 DOI: 10.1016/s1534-5807(02)00189-2
Source DB: PubMed Journal: Dev Cell ISSN: 1534-5807 Impact factor: 12.270