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  • Intramembrane proteases cleave membrane proteins in their transmembrane helices to regulate a wide range of biological processes. They catalyse hydrolytic reactions within the hydrophobic environment of lipid membranes where water is normally excluded. How? Do the different classes of intramembrane proteases share any mechanistic principles? In this review these questions will be discussed in view of the crystal structures of prokaryotic members of the three known catalytic types of intramembrane proteases published over the past 7years. Rhomboids, the intramembrane serine proteases that are the best understood family, will be the initial area of focus, and the principles that have arisen from a number of structural and biochemical studies will be considered. The site-2 metalloprotease and GXGD-type aspartyl protease structures will then be discussed, with parallels drawn and differences highlighted between these enzymes and the rhomboids. Despite the significant advances achieved so far, to obtain a detailed understanding of the mechanism of any intramembrane protease, high-resolution structural information on the substrateenzyme complex is required. This remains a major challenge for the field.
  • Intramembrane proteases cleave membrane proteins in their transmembrane helices to regulate a wide range of biological processes. They catalyse hydrolytic reactions within the hydrophobic environment of lipid membranes where water is normally excluded. How? Do the different classes of intramembrane proteases share any mechanistic principles? In this review these questions will be discussed in view of the crystal structures of prokaryotic members of the three known catalytic types of intramembrane proteases published over the past 7years. Rhomboids, the intramembrane serine proteases that are the best understood family, will be the initial area of focus, and the principles that have arisen from a number of structural and biochemical studies will be considered. The site-2 metalloprotease and GXGD-type aspartyl protease structures will then be discussed, with parallels drawn and differences highlighted between these enzymes and the rhomboids. Despite the significant advances achieved so far, to obtain a detailed understanding of the mechanism of any intramembrane protease, high-resolution structural information on the substrateenzyme complex is required. This remains a major challenge for the field. (en)
Title
  • Structural and mechanistic principles of intramembrane proteolysis lessons from rhomboids
  • Structural and mechanistic principles of intramembrane proteolysis lessons from rhomboids (en)
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  • Structural and mechanistic principles of intramembrane proteolysis lessons from rhomboids
  • Structural and mechanistic principles of intramembrane proteolysis lessons from rhomboids (en)
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  • RIV/61388963:_____/13:00392839!RIV14-MSM-61388963
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  • I, P(GAP305/11/1886), P(LK11206)
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  • 7
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  • 108331
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  • RIV/61388963:_____/13:00392839
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  • crystal structure; enzymatic mechanism; intramembrane protease; presenilin; rhomboid (en)
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  • GB - Spojené království Velké Británie a Severního Irska
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  • [C2C5B3D7C907]
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  • FEBS Journal
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  • 280
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  • Stříšovský, Kvido
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  • 000316913500001
issn
  • 1742-464X
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http://bibframe.org/vocab/doi
  • 10.1111/febs.12199
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