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老年大鼠同侧和对侧皮质对中风的基因组反应。

The genomic response of the ipsilateral and contralateral cortex to stroke in aged rats.

作者信息

Buga A-M, Sascau M, Pisoschi C, Herndon J G, Kessler C, Popa-Wagner A

机构信息

Molecular Neurobiology Laboratory, Clinic of Neurology, University of Greifswald, Germany.

出版信息

J Cell Mol Med. 2008 Dec;12(6B):2731-53. doi: 10.1111/j.1582-4934.2008.00252.x. Epub 2008 Feb 4.

Abstract

Aged rats recover poorly after unilateral stroke, whereas young rats recover readily possibly with the help from the contralateral, healthy hemisphere. In this study we asked whether anomalous, age-related changes in the transcriptional activity in the brains of aged rats could be one underlying factor contributing to reduced functional recovery. We analysed gene expression in the periinfarct and contralateral areas of 3-month- and 18-month-old Sprague Dawley rats. Our experimental end-points were cDNA arrays containing genes related to hypoxia signalling, DNA damage and apoptosis, cellular response to injury, axonal damage and re-growth, cell lineage differentiation, dendritogenesis and neurogenesis. The major transcriptional events observed were: (i) Early up-regulation of DNA damage and down-regulation of anti-apoptosis-related genes in the periinfarct region of aged rats after stroke; (ii) Impaired neurogenesis in the periinfarct area, especially in aged rats; (iii) Impaired neurogenesis in the contralateral (unlesioned) hemisphere of both young and aged rats at all times after stroke and (iv) Marked up-regulation, in aged rats, of genes associated with inflammation and scar formation. These results were confirmed with quantitative real-time PCR. We conclude that reduced transcriptional activity in the healthy, contralateral hemisphere of aged rats in conjunction with an early up-regulation of DNA damage-related genes and pro-apoptotic genes and down-regulation of axono- and neurogenesis in the periinfarct area are likely to account for poor neurorehabilitation after stroke in old rats.

摘要

老年大鼠单侧中风后恢复较差,而年轻大鼠可能在对侧健康半球的帮助下很容易恢复。在本研究中,我们探讨了老年大鼠大脑中转录活性与年龄相关的异常变化是否可能是导致功能恢复降低的一个潜在因素。我们分析了3个月和18个月大的Sprague Dawley大鼠梗死灶周围和对侧区域的基因表达。我们的实验终点是包含与缺氧信号传导、DNA损伤和凋亡、细胞对损伤的反应、轴突损伤和再生、细胞谱系分化、树突形成和神经发生相关基因的cDNA阵列。观察到的主要转录事件有:(i)中风后老年大鼠梗死灶周围区域DNA损伤早期上调,抗凋亡相关基因下调;(ii)梗死灶周围区域神经发生受损,尤其是老年大鼠;(iii)中风后任何时候,年轻和老年大鼠对侧(未受损)半球的神经发生均受损;(iv)老年大鼠中与炎症和瘢痕形成相关的基因显著上调。这些结果通过定量实时PCR得到证实。我们得出结论,老年大鼠健康对侧半球转录活性降低,同时梗死灶周围区域DNA损伤相关基因和促凋亡基因早期上调,轴突和神经发生下调,可能是老年大鼠中风后神经康复不良的原因。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c488/3828887/86cb9ab5c00c/jcmm0012-2731-f1.jpg

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