Histone Hyperacetylation in Mitosis Prevents Sister Chromatid Separation and Produces Chromosome Segregation Defects

Abstract: Posttranslational modifications of core histones contribute to driving changes in chromatin conformation and compaction. Herein, we investigated the role of histone deacetylation on the mitotic process by inhibiting histone deacetylases shortly before mitosis in human primary fibroblasts. Cells entering mitosis with hyperacetylated histones displayed altered chromatin conformation associated with decreased reactivity to the anti-Ser 10 phospho H3 antibody, increased recruitment of protein phosphatase 1-δ on mi… Show more

“…62 In contrast, normal primary human cells tolerated HDIs quite well, despite minor chromosome segregation defects and a delay to progression through mitosis, as described by others previously. [63][64][65][66][67] We also found that in normal primary human cells not expressing HP1bDN, treatment with HDIs caused a rapid relocalization of endogenous HP1 proteins to pericentromeric regions, adjacent to chromosome kinetochores. 62 This relocalization was blocked in the cells expressing HP1bDN.…”

Heterochromatin and its Relationship to Cell Senescence and Cancer Therapy

“…62 In contrast, normal primary human cells tolerated HDIs quite well, despite minor chromosome segregation defects and a delay to progression through mitosis, as described by others previously. [63][64][65][66][67] We also found that in normal primary human cells not expressing HP1bDN, treatment with HDIs caused a rapid relocalization of endogenous HP1 proteins to pericentromeric regions, adjacent to chromosome kinetochores. 62 This relocalization was blocked in the cells expressing HP1bDN.…”

Heterochromatin and its Relationship to Cell Senescence and Cancer Therapy

“…Newly replicated chromatin contains acetylated histones. In culture with TSA, histones in newly synthesized chromatin remain acetylated, and this disrupts the structure and function of the centromere and the pericentric heterochromatin, with loss of binding to heterochromatin binding proteins (Taddei et al, 2001;Cimini et al, 2003). Histone acetylation interferes with histone phosphorylation and disrupts the function of mitotic spindle checkpoint proteins, such as BubR1, hBUB1, CENP-F and CENP-E (Dowling et al, 2005;Robbins et al, 2005).…”

“…Histone acetylation interferes with histone phosphorylation and disrupts the function of mitotic spindle checkpoint proteins, such as BubR1, hBUB1, CENP-F and CENP-E (Dowling et al, 2005;Robbins et al, 2005). As a result, the cells show a transient arrest at prometaphase, followed with aberrant mitosis such as missegregation and loss of chromosomes, resulting in cell death by either apoptosis or, mitotic cell death/ catastrophe (Qiu et al, 2000;Cimini et al, 2003;Xu et al, 2005). HDACi-induced a-tubulin acetylation does not affect mitosis, although a-tubulin is a component of mitotic spindle that mediates mitosis.…”

Histone deacetylase inhibitors: molecular mechanisms of action

“…Short-term treatment with high doses of TSA induces heterogeneity in chromosome condensation in all mitotic stages, associated with a delay in prophase progression and the occurrence of lagging chromosomes and chromatid bridges in anaphase [86]. In a Xenopus oocyte maturation system commonly used to mimic mitosis, TSA treatment impedes chromosome condensation without preventing meiosis progression [87].…”

Histone deacetylase inhibitors and genomic instability