Literature DB >> 19055485

Spindle assembly defects leading to the formation of a monopolar mitotic apparatus.

Vanessa Tillement1, Marie-Hélène Remy, Brigitte Raynaud-Messina, Laurent Mazzolini, Laurence Haren, Andreas Merdes.   

Abstract

Mitotic spindle formation in animal cells involves microtubule nucleation from two centrosomes that are positioned at opposite sides of the nucleus. Microtubules are captured by the kinetochores and stabilized. In addition, microtubules can be nucleated independently of the centrosome and stabilized by a gradient of Ran-GTP, surrounding the mitotic chromatin. Complex regulation ensures the formation of a bipolar apparatus, involving motor proteins and controlled polymerization and depolymerization of microtubule ends. The bipolar apparatus is, in turn, responsible for faithful chromosome segregation. During recent years, a variety of experiments has indicated that defects in specific motor proteins, centrosome proteins, kinases and other proteins can induce the assembly of aberrant spindles with a monopolar morphology or with poorly separated poles. Induction of monopolar spindles may be a useful strategy for cancer therapy, since ensuing aberrant mitotic exit will usually lead to cell death. In this review, we will discuss the various underlying molecular mechanisms that may be responsible for monopolar spindle formation.

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Year:  2009        PMID: 19055485     DOI: 10.1042/BC20070162

Source DB:  PubMed          Journal:  Biol Cell        ISSN: 0248-4900            Impact factor:   4.458


  16 in total

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2.  Dishevelled is a NEK2 kinase substrate controlling dynamics of centrosomal linker proteins.

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3.  Plk1 regulates both ASAP localization and its role in spindle pole integrity.

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Review 7.  A guide to classifying mitotic stages and mitotic defects in fixed cells.

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9.  Centrosomal localization of RhoGDIβ and its relevance to mitotic processes in cancer cells.

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