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HMGB2 expression is associated with transition from a quiescent to an activated state of adult neural stem cells

机译:HMGB2表达与从静态到成年神经干细胞的激活状态的转变相关联

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Background : Although quiescent neural stem cells (NSCs) in the adult hippocampus proliferate in response to neurogenic stimuli and subsequently give rise to new neurons continuously throughout life, misregulation of NSCs in pathological conditions, including aging, leads to the impairment of learning and memory. High mobility group B family 1 (HMGB1) and HMGB2, HMG family proteins that function as transcriptional activators through the modulation of chromatin structure, have been assumed to play some role in the regulation of adult NSCs; however, their precise functions and even expression patterns in the adult hippocampus remain elusive. Results : Here we show that expression of HMGB2 but not HMGB1 is restricted to the subset of NSCs and their progenitors. Furthermore, running, a well‐known positive neurogenic stimulus, increased the proliferation of HMGB2‐expressing cells, whereas aging was accompanied by a marked decrease in these cells. Intriguingly, HMGB2‐expressing quiescent NSCs, which were shifted toward the proliferative state, were decreased as aging progressed. Conclusions : HMGB2 expression is strongly associated with transition from the quiescent to the proliferative state of NSCs, supporting the possibility that HMGB2 is involved in the regulation of adult neurogenesis and can be used as a novel marker to identify NSCs primed for activation in the adult hippocampus. Developmental Dynamics 247:229–238, 2018 . ? 2017 Wiley Periodicals, Inc.
机译:背景:虽然成年海马的静态神经干细胞(NSCs)响应神经源性刺激而增殖,但随后在整个生命中连续产生新的神经元,虽然在整个生命中连续地产生新神经元,但在病理条件下的误解,包括老化,导致学习和记忆的损害导致学习和记忆的损害。在通过调节染色质结构的情况下,HMG系列蛋白质的高迁移率组B系列1(HMGB1)和HMGB2,HMG系列蛋白在成人NSC的调节中发挥了一些作用;然而,他们的精确功能甚至成年海马的表达模式仍然难以捉摸。结果:在这里,我们表明HMGB2的表达但不是HMGB1仅限于NSCs及其祖细胞的子集。此外,运行众所周知的阳性神经刺激刺激,增加了HMGB2表达细胞的增殖,而老化伴随着这些细胞的显着降低。随着老化进展,朝向增殖状态变化的可感染性HMGB2表达静态NSC。结论:HMGB2表达与从静态到NSC的增殖状态的转变强烈相关,支持HMGB2参与成年神经发生的调节,可用作新的标记,以鉴定成年海马激活的NSCs 。发展动力学247:229-238,2018。还2017年Wiley期刊,Inc。

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