Literature DB >> 18635967

Differential regulation of centrosome integrity by DNA damage response proteins.

Rekha Rai1, Ashwini Phadnis, Sharda Haralkar, Rajendra A Badwe, Hui Dai, Kaiyi Li, Shiaw-Yih Lin.   

Abstract

MDC1 and BRIT1 have been shown to function as key regulators in response to DNA damage. However, their roles in centrosomal regulation haven't been elucidated. In this study, we demonstrated the novel functions of these two molecules in regulating centrosome duplication and mitosis. We found that MDC1 and BRIT1 were integral components of the centrosome that colocalize with gamma-tubulin. Depletion of either protein led to centrosome amplification. However, the mechanisms that allow them to maintain centrosome integrity are different. MDC1-depleted cells exhibited centrosome overduplication, leading to multipolar mitosis, chromosome missegregation, and aneuploidy, whereas BRIT1 depletion led to misaligned spindles and/or lagging chromosomes with defective spindle checkpoint activation that resulted in defective cytokinesis and polyploidy. We further illustrated that both MDC1 and BRIT1 were negative regulators of Aurora A and Plk1, two centrosomal kinases involved in centrosome maturation and spindle assembly. Moreover, the levels of MDC1 and BRIT1 inversely correlated with centrosome amplification, defective mitosis and cancer metastasis in human breast cancer. Together, MDC1 and BRIT1 may function as tumor-suppressor genes, at least in part by orchestrating proper centrosome duplication and mitotic spindle assembly.

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Year:  2008        PMID: 18635967      PMCID: PMC2557875          DOI: 10.4161/cc.7.14.6303

Source DB:  PubMed          Journal:  Cell Cycle        ISSN: 1551-4005            Impact factor:   4.534


  51 in total

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  31 in total

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4.  Centrosomes at M phase act as a scaffold for the accumulation of intracellular ubiquitinated proteins.

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7.  Overexpression of MCPH1 inhibits uncontrolled cell growth by promoting cell apoptosis and arresting the cell cycle in S and G2/M phase in lung cancer cells.

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8.  BRCA1 and FancJ cooperatively promote interstrand crosslinker induced centrosome amplification through the activation of polo-like kinase 1.

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Review 9.  The linkage of chromatin remodeling to genome maintenance: contribution from a human disease gene BRIT1/MCPH1.

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Review 10.  Primary microcephaly: do all roads lead to Rome?

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