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含有视交叉上核的胎儿组织可恢复老龄大鼠的多种昼夜节律。

Fetal tissue containing the suprachiasmatic nucleus restores multiple circadian rhythms in old rats.

作者信息

Li H, Satinoff E

机构信息

Department of Psychology, University of Illinois at Urbana-Champaign, Champaign, Illinois 61820, USA.

出版信息

Am J Physiol. 1998 Dec;275(6):R1735-44. doi: 10.1152/ajpregu.1998.275.6.R1735.

Abstract

The suprachiasmatic nucleus (SCN) is the major circadian pacemaker in mammals. When fetal tissue containing the SCN is transplanted into young rats whose circadian rhythms have been abolished by SCN lesions, the rhythms gradually reappear. Circadian rhythms in many rats deteriorate or disappear with age. The rationale of the present study was that old rats with poor circadian rhythms resemble young rats with SCN lesions. If there is a similar mechanism underlying this resemblance, then fetal tissue containing the SCN should restore rhythms in old rats. Therefore, we implanted such tissue into the third ventricle of intact aged rats with poor circadian rhythms. Body temperature, locomotor activity, and/or drinking were measured simultaneously within subjects. Grafts and hosts were stained immunocytochemically for vasoactive intestinal polypeptide (VIP), arginine vasopressin (AVP), and neuropeptide Y (NPY). Of 23 SCN grafts, 14 were viable (cells observable with Nissl or peptide staining). In 7 of the 14 aged hosts, up to three circadian rhythms were improved or restored. VIP cells were always observable, which was not the case for AVP cells or NPY fibers. In the other seven hosts, no circadian rhythm was improved. Compared with the successful grafts, these unsuccessful grafts had similar amounts of AVP and NPY staining but significantly less VIP cell and/or fiber staining. Fetal cerebellar grafts, which do not contain any of the three peptides, did not improve or restore any rhythms. Thus the degeneration of circadian rhythms in aged rats may be due, at least in part, to deterioration of the aged SCN and in particular, to a loss of function of VIP-containing neurons.

摘要

视交叉上核(SCN)是哺乳动物主要的昼夜节律起搏器。当将含有SCN的胎儿组织移植到因SCN损伤而昼夜节律被消除的幼鼠体内时,节律会逐渐重新出现。许多大鼠的昼夜节律会随着年龄增长而恶化或消失。本研究的理论依据是,昼夜节律差的老年大鼠类似于患有SCN损伤的幼鼠。如果这种相似性背后存在类似机制,那么含有SCN的胎儿组织应该能恢复老年大鼠的节律。因此,我们将此类组织植入了昼夜节律差的完整老年大鼠的第三脑室。在实验对象体内同时测量体温、运动活动和/或饮水情况。对移植物和宿主进行免疫细胞化学染色,以检测血管活性肠肽(VIP)、精氨酸加压素(AVP)和神经肽Y(NPY)。在23个SCN移植物中,14个存活(通过尼氏染色或肽染色可观察到细胞)。在14只老年宿主中的7只中,多达三种昼夜节律得到改善或恢复。VIP细胞始终可观察到,而AVP细胞或NPY纤维则不然。在另外7只宿主中,昼夜节律没有得到改善。与成功的移植物相比,这些未成功的移植物中AVP和NPY染色量相似,但VIP细胞和/或纤维染色明显较少。不含这三种肽中任何一种的胎儿小脑移植物,没有改善或恢复任何节律。因此,老年大鼠昼夜节律的退化可能至少部分是由于老年SCN的恶化,特别是由于含VIP神经元的功能丧失。

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