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NG108-15细胞分化过程中蛋白激酶C的调控

Regulation of protein kinase C in NG108-15 cell differentiation.

作者信息

Battaini F, Garbillo G, Bergamaschi S, Parenti M, Wetsel W C, Govoni S, Trabucchi M

机构信息

Department of Experimental Medicine and Biochemical Sciences, University of Roma Tor Vergata, Italy.

出版信息

Biochem Biophys Res Commun. 1994 May 30;201(1):135-42. doi: 10.1006/bbrc.1994.1679.

Abstract

The involvement of PKC in NG108-15 cell differentiation was investigated. Differentiation with dBcAMP was associated with a decrease in total cellular phorbol ester binding. The histone-directed PKC activity was decreased in the soluble fraction. Northern and Western blotting revealed the presence of only PKC alpha but not PKC beta and PKC gamma among the calcium-dependent isoforms. Differentiation induced a decrease of cytosolic PKC alpha immunoreactivity, with no changes of mRNA content or appearance of PKC beta and PKC gamma isoforms. The low levels of PKC alpha in the soluble fraction suggest that the mRNA for this species is less efficiently translated in differentiated NG108-15 cells. The data suggest that down-regulation of PKC alpha protein and kinase activity are associated with induction of neuronal morphology in NG108-15 cells.

摘要

研究了蛋白激酶C(PKC)在NG108 - 15细胞分化中的作用。用二丁酰环磷腺苷(dBcAMP)诱导分化与细胞总的佛波酯结合能力下降有关。在可溶性部分中,组蛋白定向的PKC活性降低。Northern印迹和Western印迹显示,在钙依赖性同工型中仅存在PKCα,而不存在PKCβ和PKCγ。分化导致胞质PKCα免疫反应性降低,PKCβ和PKCγ同工型的mRNA含量或表达没有变化。可溶性部分中PKCα水平较低表明,该同工型的mRNA在分化的NG108 - 15细胞中翻译效率较低。数据表明,PKCα蛋白和激酶活性的下调与NG108 - 15细胞中神经元形态的诱导有关。

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