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Orphan kinases turn eccentric (CROSBI ID 308742)

Prilog u časopisu | izvorni znanstveni rad | međunarodna recenzija

Mikolcevic, Petra ; Rainer, Johannes ; Geley, Stephan Orphan kinases turn eccentric // Cell cycle, 11 (2012), 20; 3758-3768. doi: 10.4161/cc.21592

Podaci o odgovornosti

Mikolcevic, Petra ; Rainer, Johannes ; Geley, Stephan

engleski

Orphan kinases turn eccentric

PCTAIRE kinases (PCTK) are a highly conserved, but poorly characterized, subgroup of cyclin-dependent kinases (CDK). They are characterized by a conserved catalytic domain flanked by N- and C- terminal extensions that are involved in cyclin binding. Vertebrate genomes contain three highly similar PCTAIRE kinases (PCTK1, 2, 3, a.k.a., CDK16, 17, 18), which are most abundant in post- mitotic cells in brain and testis. Consistent with this restricted expression pattern, PCTK1 (CDK16) has recently been shown to be essential for spermatogenesis. PCTAIREs are activated by cyclin Y (CCNY), a highly conserved single cyclin fold protein. By binding to N-myristoylated CCNY, CDK16 is targeted to the plasma membrane. Unlike conventional cyclin-CDK interactions, binding of CCNY to CDK16 not only requires the catalytic domain, but also domains within the N-terminal extension. Interestingly, phosphorylation within this domain blocks CCNY binding, providing a novel means of cyclin-CDK regulation. By using these functional characteristics, we analyzed “PCTAIRE” sequence containing protein kinase genes in genomes of various organisms and found that CCNY and CCNY-dependent kinases are restricted to eumetazoa and possibly evolved along with development of a central nervous system. Here, we focus on the structure and regulation of PCTAIREs and discuss their established functions.

cyclin, CDK, PCTAIRE, PCTK, evolution, development, spermatogenesis, CDK16

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Podaci o izdanju

11 (20)

2012.

3758-3768

objavljeno

1538-4101

1551-4005

10.4161/cc.21592

Povezanost rada

Biologija, Interdisciplinarne prirodne znanosti

Poveznice
Indeksiranost