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ADAM23 敲低通过上调 P27KIP1 表达促进 P19 胚胎癌细胞的神经元分化。

ADAM23 knockdown promotes neuronal differentiation of P19 embryonal carcinoma cells by up-regulating P27KIP1 expression.

机构信息

School of Life Sciences, Fudan University, Shanghai, People's Republic of China.

出版信息

Cell Biol Int. 2012;36(12):1275-9. doi: 10.1042/CBI20120154.

Abstract

ADAM23 (a disintegrin and metalloprotease 23), a member of brain MDC (macrophage-derived chemokine) family, is important for the development of CNS (central nervous system). P19 mouse embryonal carcinoma cells can differentiate into neurons when cultured in aggregates and induced with RA (retinoic acid). We have found that under conditions without RA induction, knocking down ADAM23 with RNAi (RNA interference) promoted neuronal differentiation, and similarly recombinant GST (glutathione transferase)-ADAM23-DIS protein inhibited neuronal differentiation of P19/ADAM23KD (P19/ADAM23-knockdown) cells. In P19/ADAM23KD, there were more cells arrested in G1 phase than normal P19 cells, due to the up-regulation of P57KIP2 and P27KIP1 expression. P27KIP1 was up-regulated during the differentiation process of both P19/ADAM23KD cells without RA induction, and P19 cells with RA induction. Transient overexpression of P27KIP1 in P19 cells also promoted neuronal differentiation of P19 cells. The findings indicate that ADAM23 suppresses neuronal differentiation through its disintegrin domain, and Adam23 KD up-regulates P27KIP1 in P19/ADAM23KD cells, one reason that P19/ADAM23KD cells can differentiate into neurons without RA induction.

摘要

ADAM23(解整合素和金属蛋白酶 23)是脑 MDC(巨噬细胞来源的趋化因子)家族的成员,对于中枢神经系统(CNS)的发育很重要。当 P19 鼠胚胎癌细胞在聚集状态下培养并在 RA(视黄酸)诱导下可以分化为神经元。我们发现,在没有 RA 诱导的情况下,用 RNAi(RNA 干扰)敲低 ADAM23 促进了神经元分化,类似地,重组 GST(谷胱甘肽转移酶)-ADAM23-DIS 蛋白抑制了 P19/ADAM23KD(P19/ADAM23 敲低)细胞的神经元分化。在 P19/ADAM23KD 中,由于 P57KIP2 和 P27KIP1 表达上调,G1 期阻滞的细胞比正常 P19 细胞更多。在没有 RA 诱导的情况下,P19/ADAM23KD 细胞和有 RA 诱导的 P19 细胞的分化过程中,P27KIP1 都被上调。瞬时过表达 P27KIP1 也促进了 P19 细胞的神经元分化。这些发现表明,ADAM23 通过其解整合素结构域抑制神经元分化,而 ADAM23KD 在 P19/ADAM23KD 细胞中上调 P27KIP1,这是 P19/ADAM23KD 细胞在没有 RA 诱导的情况下分化为神经元的原因之一。

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