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大鼠纹状体内注射喹啉酸后纹状体投射神经元和中间神经元的相对存活率。

Relative survival of striatal projection neurons and interneurons after intrastriatal injection of quinolinic acid in rats.

作者信息

Figueredo-Cardenas G, Anderson K D, Chen Q, Veenman C L, Reiner A

机构信息

Department of Anatomy and Neurobiology, University of Tennessee at Memphis 38163.

出版信息

Exp Neurol. 1994 Sep;129(1):37-56. doi: 10.1006/exnr.1994.1145.

Abstract

An excitotoxic process mediated by the NMDA type glutamate receptor may be involved in striatal neuron death in Huntington's disease (HD). To explore this possibility, we have injected an NMDA-receptor-specific excitotoxin, quinolinic acid (QA), into the striatum in adult rats and 2-4 months postlesion explored the relative patterns of survival for the various different types of striatal projection neurons and interneurons and for the striatal efferent fibers in the different striatal projection areas. The perikarya of specific types of striatal neurons were identified by neurotransmitter immunohistochemical labeling or by retrograde labeling from striatal target areas, while the striatal efferent fiber plexuses were identified by neurotransmitter immunohistochemical labeling. The pattern of survival for the perikarya of each neuron type as a function of distance from the center of the injection site was determined, and the relative survival of each type was compared. For the fibers in target areas, computer-assisted image analysis was used to determine the degree of fiber loss for each projection target. In the study of perikaryal vulnerability, we found that the somatostatin-neuropeptide Y (SS/NPY) interneurons were the most vulnerable to QA and the cholinergic neurons were invulnerable to QA. The perikarya of all projection neuron types (striatopallidal, striatonigral, and striato-entopeduncular) were less vulnerable than the SS/NPY interneurons and more vulnerable than the cholinergic interneurons. Among projection neuron perikarya, there was evidence of differential vulnerability, with striatonigral neurons appearing to be the most vulnerable. Examination of immunolabeled striatal fibers in the striatal target areas indicated that striato-entopeduncular fibers better survived intrastriatal QA than did striatopallidal or striatonigral fibers. The apparent order of vulnerability observed in this study among projection neurons and/or their efferent fiber plexuses and the invulnerability observed in this study of cholinergic interneurons is similar to that observed in HD. The vulnerability of the SS/NPY interneurons to QA is, however, in stark contrast to their invulnerability in HD. The results thus suggest that although the excitotoxin hypothesis of striatal neuron death in HD has merit, QA injections into adult rat striatum do not strictly mimic the outcome in HD. This suggests that either adult rats are not a completely suitable subject for mimicking HD or the HD excitotoxic process does not involve a freely circulating excitotoxin such as QA.

摘要

由N-甲基-D-天冬氨酸(NMDA)型谷氨酸受体介导的兴奋毒性过程可能参与了亨廷顿舞蹈病(HD)中纹状体神经元的死亡。为探究这种可能性,我们将一种NMDA受体特异性兴奋毒素喹啉酸(QA)注射到成年大鼠的纹状体中,并在损伤后2至4个月,探究不同类型的纹状体投射神经元、中间神经元以及不同纹状体投射区域中纹状体传出纤维的相对存活模式。通过神经递质免疫组织化学标记或从纹状体靶区域逆行标记来识别特定类型纹状体神经元的胞体,而通过神经递质免疫组织化学标记来识别纹状体传出纤维丛。确定每种神经元类型胞体的存活模式与距注射部位中心距离的函数关系,并比较每种类型的相对存活率。对于靶区域中的纤维,使用计算机辅助图像分析来确定每个投射靶点的纤维损失程度。在对胞体易损性的研究中,我们发现生长抑素-神经肽Y(SS/NPY)中间神经元对QA最敏感,而胆碱能神经元对QA不敏感。所有投射神经元类型(纹状体苍白球、纹状体黑质和纹状体终纹床核)的胞体比SS/NPY中间神经元更不易受损,比胆碱能中间神经元更易受损。在投射神经元胞体中,存在易损性差异的证据,其中纹状体黑质神经元似乎最易受损。对纹状体靶区域中免疫标记的纹状体纤维的检查表明,纹状体终纹床核纤维比纹状体苍白球或纹状体黑质纤维在纹状体内注射QA后存活得更好。本研究中观察到的投射神经元和/或其传出纤维丛之间明显的易损性顺序以及胆碱能中间神经元在本研究中观察到的不易损性与HD中观察到的相似。然而,SS/NPY中间神经元对QA的易损性与它们在HD中的不易损性形成鲜明对比。因此,结果表明,尽管HD中纹状体神经元死亡的兴奋毒素假说是有价值的,但向成年大鼠纹状体注射QA并不能严格模拟HD中的结果。这表明,要么成年大鼠不是模拟HD的完全合适的对象,要么HD兴奋毒性过程不涉及像QA这样自由循环的兴奋毒素。

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