Arpc1b, a centrosomal protein, is both an activator and substrate of Aurora A

Poonam R. Molli; Da-Qiang Li; Rozita Bagheri-Yarmand; Suresh B. Pakala; Hiroshi Katayama; Subrata Sen; Jyoti Iyer; Jonathan Chernoff; Ming-Ying Tsai; Sujit S. Nair; Rakesh Kumar

doi:10.1083/jcb.200908050

Arpc1b, a centrosomal protein, is both an activator and substrate of Aurora A

Poonam R. Molli
, Da-Qiang Li
, Rozita Bagheri-Yarmand
, Suresh B. Pakala
, Hiroshi Katayama
, Subrata Sen
, Jyoti Iyer
, Jonathan Chernoff
, Ming-Ying Tsai
, Sujit S. Nair
, Rakesh Kumar

Biology

Research output: Contribution to journal › Article › peer-review

58 Scopus citations

Abstract

Here we provide evidence in support of an inherent role for Arpc1b, a component of the Arp2/3 complex, in regulation of mitosis and demonstrate that its depletion inhibits Aurora A activation at the centrosome and impairs the ability of mammalian cells to enter mitosis. We discovered that Arpc1b colocalizes with γ-tubulin at centrosomes and stimulates Aurora A activity. Aurora A phosphorylates Arpc1b on threonine 21, and expression of Arpc1b but not a nonphosphorylatable Arpc1b mutant in mammalian cells leads to Aurora A kinase activation and abnormal centrosome amplification in a Pak1-independent manner. Together, these findings reveal a new function for Arpc1b in centrosomal homeostasis. Arpc1b is both a physiological activator and substrate of Aurora A kinase and these interactions help to maintain mitotic integrity in mammalian cells. © 2010 Molli et al.

Original language	English
Pages (from-to)	101-114
Number of pages	14
Journal	Journal of Cell Biology
Volume	190
Issue number	1
DOIs	https://doi.org/10.1083/jcb.200908050
State	Published - Jul 12 2010

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title = "Arpc1b, a centrosomal protein, is both an activator and substrate of Aurora A",

abstract = "Here we provide evidence in support of an inherent role for Arpc1b, a component of the Arp2/3 complex, in regulation of mitosis and demonstrate that its depletion inhibits Aurora A activation at the centrosome and impairs the ability of mammalian cells to enter mitosis. We discovered that Arpc1b colocalizes with γ-tubulin at centrosomes and stimulates Aurora A activity. Aurora A phosphorylates Arpc1b on threonine 21, and expression of Arpc1b but not a nonphosphorylatable Arpc1b mutant in mammalian cells leads to Aurora A kinase activation and abnormal centrosome amplification in a Pak1-independent manner. Together, these findings reveal a new function for Arpc1b in centrosomal homeostasis. Arpc1b is both a physiological activator and substrate of Aurora A kinase and these interactions help to maintain mitotic integrity in mammalian cells. {\textcopyright} 2010 Molli et al.",

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AU - Molli, Poonam R.

AU - Li, Da-Qiang

AU - Bagheri-Yarmand, Rozita

AU - Pakala, Suresh B.

AU - Katayama, Hiroshi

AU - Sen, Subrata

AU - Iyer, Jyoti

AU - Chernoff, Jonathan

AU - Tsai, Ming-Ying

AU - Nair, Sujit S.

AU - Kumar, Rakesh

PY - 2010/7/12

Y1 - 2010/7/12

N2 - Here we provide evidence in support of an inherent role for Arpc1b, a component of the Arp2/3 complex, in regulation of mitosis and demonstrate that its depletion inhibits Aurora A activation at the centrosome and impairs the ability of mammalian cells to enter mitosis. We discovered that Arpc1b colocalizes with γ-tubulin at centrosomes and stimulates Aurora A activity. Aurora A phosphorylates Arpc1b on threonine 21, and expression of Arpc1b but not a nonphosphorylatable Arpc1b mutant in mammalian cells leads to Aurora A kinase activation and abnormal centrosome amplification in a Pak1-independent manner. Together, these findings reveal a new function for Arpc1b in centrosomal homeostasis. Arpc1b is both a physiological activator and substrate of Aurora A kinase and these interactions help to maintain mitotic integrity in mammalian cells. © 2010 Molli et al.

AB - Here we provide evidence in support of an inherent role for Arpc1b, a component of the Arp2/3 complex, in regulation of mitosis and demonstrate that its depletion inhibits Aurora A activation at the centrosome and impairs the ability of mammalian cells to enter mitosis. We discovered that Arpc1b colocalizes with γ-tubulin at centrosomes and stimulates Aurora A activity. Aurora A phosphorylates Arpc1b on threonine 21, and expression of Arpc1b but not a nonphosphorylatable Arpc1b mutant in mammalian cells leads to Aurora A kinase activation and abnormal centrosome amplification in a Pak1-independent manner. Together, these findings reveal a new function for Arpc1b in centrosomal homeostasis. Arpc1b is both a physiological activator and substrate of Aurora A kinase and these interactions help to maintain mitotic integrity in mammalian cells. © 2010 Molli et al.

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Arpc1b, a centrosomal protein, is both an activator and substrate of Aurora A

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