Author: Goblirsch, Brandon R.; Pryor, Edward E.; Wiener, Michael C.
Title: The tripartite architecture of the eukaryotic integral membrane protein zinc metalloprotease Ste24 Cord-id: qp568e3z Document date: 2019_11_5
ID: qp568e3z
Snippet: Ste24 enzymes, a family of eukaryotic integral membrane proteins, are zinc metalloproteases (ZMPs) originally characterized as “CAAX proteases†targeting prenylated substrates, including aâ€factor mating pheromone in yeast and prelamin A in humans. Recently, Ste24 was shown to also cleave nonprenylated substrates. Reduced activity of the human ortholog, HsSte24, is linked to multiple disease states (laminopathies), including progerias and lipid disorders. Ste24 possesses a unique “αâ€ba
Document: Ste24 enzymes, a family of eukaryotic integral membrane proteins, are zinc metalloproteases (ZMPs) originally characterized as “CAAX proteases†targeting prenylated substrates, including aâ€factor mating pheromone in yeast and prelamin A in humans. Recently, Ste24 was shown to also cleave nonprenylated substrates. Reduced activity of the human ortholog, HsSte24, is linked to multiple disease states (laminopathies), including progerias and lipid disorders. Ste24 possesses a unique “αâ€barrel†structure consisting of seven transmembrane (TM) αâ€helices encircling a large intramembranous cavity (~14 000 Ã…(3)). The catalytic zinc, coordinated via a HExxH…E/H motif characteristic of gluzincin ZMPs, is positioned at one of the cavity's bases. The interrelationship between Ste24 as a gluzincin, a longâ€studied class of soluble ZMPs, and as a novel cavityâ€containing integral membrane protein protease has been minimally explored to date. Informed by homology to wellâ€characterized soluble, gluzincin ZMPs, we develop a model of Ste24 that provides a conceptual framework for this enzyme family, suitable for development and interpretation of structure/function studies. The model consists of an interfacial, zincâ€containing “ZMP Core†module surrounded by a “ZMP Accessory†module, both capped by a TM helical “αâ€barrel†module of as yet unknown function. Multiple sequence alignment of 58 Ste24 orthologs revealed 38 absolutely conserved residues, apportioned unequally among the ZMP Core (18), ZMP Accessory (13), and αâ€barrel (7) modules. This Tripartite Architecture representation of Ste24 provides a unified image of this enzyme family.
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