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Glynn M, et al.  (2010) Centromeres: assembling and propagating epigenetic function. Subcell Biochem 50():223-49

Abstract: The faithful replication of DNA and the accurate segregation of genomic material from one generation to the next is critical in the maintenance of genomic stability. This chapter will describe the structure and assembly of an epigenetically inherited locus, the centromere, and its role in the processes by which sister chromatids are evenly segregated to daughter cells. During the G2 phase of the cell cycle kinetochores are assembled upon the chromatids. During mitosis, kinetochores attach chromosome(s) to the mitotic spindle. The kinetochore structure serves as the interface between the mitotic spindle and the chromatids and it is at the kinetochore where the forces that drive chromatid separation are generated. Unattached chromosomes fail to satisfy the spindle assembly checkpoint (SAC), resulting in cell cycle arrest. The centromere is the locus upon which the kinetochore assembles, and centromeres themselves are determined by their unique protein composition. Apart from budding yeast, centromeres are not specified simply by DNA sequence, but rather through chromatin composition and architecture and are thus epigenetically determined. Centromeres are built on a specific nucleosome not found elsewhere in the genome, in which histone H3 is replaced with a homologue - CENP-A or CenH3. This domain is flanked by heterochromatin and is folded to provide a 3-dimensional cylinder-like structure at metaphase that establishes the kinetochore on the surface of the mitotic chromosomes. A large family of CENtromere Proteins (CENPs) associates with centromeric chromatin throughout the cell cycle and are required for kinetochore function. Unlike the bulk of histones, CENP-A is not assembled concurrently with DNA synthesis in S-phase but rather assembles into the centromere in the subsequent G1 phase. The assembly of CENP-A chromatin following DNA replication and the re-establishment of this network of constitutive proteins have emerged as critical mechanisms for understanding how the centromere is replicated during the cell cycle.

Status: Published Type: Journal Article PubMed ID: 20012585

Topics addressed in this paper

Number of different genes curated to this paper: 34

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Topics Genes linked to topics (#1 - 10 )
CBF2 CDC20 CEN1 CEN10 CEN11 CEN12 CEN13 CEN14 CEN15 CEN16
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Topics Genes linked to topics (#11 - 20 )
CEN2 CEN3 CEN4 CEN5 CEN6 CEN7 CEN8 CEN9 CSE4 CSM3
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Topics Genes linked to topics (#21 - 30 )
HHF1 HHF2 HHT1 HHT2 HIR1 HTA1 HTA2 HTB1 HTB2 IPL1
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Topics Genes linked to topics (#31 - 34 )
MAD1 MAD2 MAD3 MPS1
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