Bimodal Binding of STIL to Plk4 Controls Proper Centriole Copy Number | Zendy

Midori Ohta | Zendy; Koki Watanabe | Zendy; Tomoko Ashikawa | Zendy; Yuka Nozaki | Zendy; Satoko Yoshiba | Zendy; Akatsuki Kimura | Zendy; Daiju Kitagawa | Zendy

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Bimodal Binding of STIL to Plk4 Controls Proper Centriole Copy Number

Author(s) -

Midori Ohta,

Koki Watanabe,

Tomoko Ashikawa,

Yuka Nozaki,

Satoko Yoshiba,

Akatsuki Kimura,

Daiju Kitagawa

Publication year - 2018

Publication title -

cell reports

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 6.264

H-Index - 154

eISSN - 2639-1856

pISSN - 2211-1247

DOI - 10.1016/j.celrep.2018.05.030

Subject(s) - centriole , microbiology and biotechnology , autophosphorylation , biology , regulator , genetics , microtubule , gene , kinase , protein kinase a

The number of centrioles is tightly controlled to ensure bipolar spindle assembly, which is a prerequisite to maintain genome integrity. However, our understanding of the fundamental principle that governs the formation of a single procentriole per parental centriole is incomplete. Here, we show that the local restriction of Plk4, a master regulator of the procentriole formation, is achieved by a bimodal interaction of STIL with Plk4. We demonstrate that the conserved short coiled-coil region of STIL binds to and protects Plk4 from protein degradation at the site of procentriole formation. On the other hand, the conserved C-terminal region of STIL named truncated in microcephaly (TIM) domain promotes autophosphorylation and degradation of adjacent Plk4 by the direct interaction. Thus, we propose that positive and negative regulation based on the bimodal binding of Plk4 and STIL ensures the formation of a single procentriole per parental centriole.

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