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Delayed Cell Cycle Progression in STHdh(Q111)/Hdh(Q111) Cells, a Cell Model for Huntington's Disease Mediated by microRNA-19a, microRNA-146a and microRNA-432.

Microrna. 2015; 
DasEashita,JanaNihar Ranjan,BhattacharyyaNitai
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PCR Cloning and Subcloning … Cloning of Precursor microRNA-19a (pre-mirna) The cloning of precursor mir-146a (pre-mir-146a), pre- mir-124 and pre-mir-432 sequences in pRNA-U61.Hygro (Genscript, USA) vector was done as described earlier [28, 31]. Similar procedures were used to clone pre-mir-19a … Get A Quote

摘要

Several indirect evidences are available to indicate that abnormalities in cell cycle may contribute to pathogenesis of Huntington's disease (HD). Here, we show that the cell cycle progression in STsdh(Q111)/Hdh(Q111)cells, a cell model of HD, is delayed in S and G2-M phases compared to control STHdhQ7/HdhQ7cells. Expression of 17 genes, like PCNA and CHEK1, was increased in STHdh(Q111)/Hdh(Q111)cells. Increased expressions of PCNA, CHEK1 and CCNA2, and an enhanced phosphorylation of Rb1 were observed in primary cortical neurons expressing mutant N-terminal huntingtin (HTT), R6/2 mice and STHdh(Q111)/Hdh(Q111) cells. This increase in the expressions of PCNA, CHEK1 and CCNA2 was found to be the... More

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