| Literature DB >> 23539603 |
Andrew Quigley1, Yin Yao Dong, Ashley C W Pike, Liang Dong, Leela Shrestha, Georgina Berridge, Phillip J Stansfeld, Mark S P Sansom, Aled M Edwards, Chas Bountra, Frank von Delft, Alex N Bullock, Nicola A Burgess-Brown, Elisabeth P Carpenter.
Abstract
Mutations in the nuclear membrane zinc metalloprotease ZMPSTE24 lead to diseases of lamin processing (laminopathies), such as the premature aging disease progeria and metabolic disorders. ZMPSTE24 processes prelamin A, a component of the nuclear lamina intermediate filaments, by cleaving it at two sites. Failure of this processing results in accumulation of farnesylated, membrane-associated prelamin A. The 3.4 angstrom crystal structure of human ZMPSTE24 has a seven transmembrane α-helical barrel structure, surrounding a large, water-filled, intramembrane chamber, capped by a zinc metalloprotease domain with the catalytic site facing into the chamber. The 3.8 angstrom structure of a complex with a CSIM tetrapeptide showed that the mode of binding of the substrate resembles that of an insect metalloprotease inhibitor in thermolysin. Laminopathy-associated mutations predicted to reduce ZMPSTE24 activity map to the zinc metalloprotease peptide-binding site and to the bottom of the chamber.Entities:
Mesh:
Substances:
Year: 2013 PMID: 23539603 DOI: 10.1126/science.1231513
Source DB: PubMed Journal: Science ISSN: 0036-8075 Impact factor: 63.714