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海马体中蛋白激酶C和F1/GAP - 43基因的表达与持续3天的突触增强呈负相关。

Protein kinase C and F1/GAP-43 gene expression in hippocampus inversely related to synaptic enhancement lasting 3 days.

作者信息

Meberg P J, Barnes C A, McNaughton B L, Routtenberg A

机构信息

Department of Psychology, Northwestern University, Evanston, IL 60208.

出版信息

Proc Natl Acad Sci U S A. 1993 Dec 15;90(24):12050-4. doi: 10.1073/pnas.90.24.12050.

Abstract

The mRNA levels of protein F1 (also known as GAP-43), and protein kinase C (PKC) subtypes were measured 3 days after the induction of long-term enhancement (also known as long-term potentiation) in the hippocampus of chronically prepared conscious rats by quantitative in situ hybridization. Altered mRNA levels correlated significantly with alternations in synaptic efficacy; such correlations have not been reported previously. Rats with greater synaptic enhancement had lower gene expression in the CA3 subfield of F1/GAP-43 and both beta-PKC and gamma-PKC, but not alpha-PKC. For microtubule-associated protein 2 (MAP-2), neurogranin, and the glutamate receptor subtype B-flip, no correlation was observed in any cell field between synaptic enhancement and hybridization to the mRNA. To our surprise, alterations in mRNA levels of F1/GAP-43 and gamma-PKC were highly correlated (r = +0.928, P < 0.001), suggesting coordinate regulation. Since F1/GAP-43 is associated with neurite growth, its lowered expression at 3 days would reduce potential growth, leading to synaptic stabilization. We propose that long-term synaptic change is mediated by gene expression of the very same proteins initially modified posttranslationally.

摘要

通过定量原位杂交技术,在长期制备的清醒大鼠海马体中诱导长期增强(也称为长时程增强)3天后,检测蛋白F1(也称为GAP - 43)和蛋白激酶C(PKC)亚型的mRNA水平。mRNA水平的改变与突触效能的变化显著相关;此前尚未有此类相关性的报道。突触增强程度较高的大鼠,在F1/GAP - 43的CA3亚区以及β - PKC和γ - PKC的基因表达较低,但α - PKC无此现象。对于微管相关蛋白2(MAP - 2)、神经颗粒蛋白和谷氨酸受体亚型B - flip,在任何细胞区域中均未观察到突触增强与mRNA杂交之间的相关性。令我们惊讶的是,F1/GAP - 43和γ - PKC的mRNA水平变化高度相关(r = +0.928,P < 0.001),表明存在协同调节。由于F1/GAP - 43与神经突生长相关,其在3天时表达降低会减少潜在的生长,导致突触稳定。我们提出,长期的突触变化是由最初在翻译后修饰的相同蛋白质的基因表达介导的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1468/48123/9eb01ea0c75f/pnas01531-0623-a.jpg

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