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突触后致密物抗原:抗突触后致密物抗血清的制备与特性鉴定

Postsynaptic density antigens: preparation and characterization of an antiserum against postsynaptic densities.

作者信息

Sampedro M N, Bussineau C M, Cotman C W

出版信息

J Cell Biol. 1981 Sep;90(3):675-86. doi: 10.1083/jcb.90.3.675.

Abstract

Long-term immunization of rabbits with postsynaptic densities (PSD) from bovine brain produced an antiserum specific for PSD as judged by binding to subcellular fractions and immunohistochemical location at the light and electron microscope levels. (a) The major antigens of bovine PSD preparations were three polypeptides of molecular weight 95,000 (PSD-95), 82,000 (PSD-82), and 72,000 (PSD-72), respectively. Antigen PSD-95, also present in mouse and rat PSDs was virtually absent from cytoplasm, myelin, mitochondria, and microsomes from rodent or bovine brain. Antigens PSD-82 and PSD-72 were present in all subcellular fractions from bovine brain, especially in mitochondria, but were almost absent from rodent brain. The antiserum also contained low-affinity antibodies against tubulin. (b)Immunohistochemical studies were performed in mouse and rat brain, where antigen PSD-95 accounted for 90 percent of the antiserum binding after adsorption with purified brain tubulin. At the light microscope level, antibody binding was observed only in those regions of the brain where synapses are known to be present. No reaction was observed in myelinated tracts, in the neuronal cytoplasm, or in nonneuronal cells. Strong reactivity was observed in the molecular layer of the dentate gyrus, stratum oriens and stratum radiatum of the hippocampus, and the molecular layer of the cerebellum. Experimental lesions, such as ablation of the rat entorhinal cortex or intraventricular injection of kainic acid, which led to a major loss of PSD in well- defined areas of the hippocampal formation, caused a correlative decrease in immunoreactivity in these areas. Abnormal patterns of immunohistochemical staining correlated with abnormal synaptic patterns in the cerebella of reeler and staggerer mouse mutants. (c) At the electron microscopic level, immunoreactivity was detectable only in PSD. The antibody did not bind to myelin, mitochondria or plasma membranes. (d) The results indicate that antigen PSD-95 is located predominantly or exclusively in PSD and can be used as a marker during subcellular fractionation. Other potential uses include the study of synaptogenesis, and the detection of changes in synapse number after experimental perturbations of the nervous system.

摘要

用牛脑突触后致密物(PSD)对兔子进行长期免疫,通过与亚细胞组分结合以及在光学显微镜和电子显微镜水平的免疫组织化学定位判断,产生了一种对PSD特异的抗血清。(a)牛PSD制剂的主要抗原分别是分子量为95,000(PSD - 95)、82,000(PSD - 82)和72,000(PSD - 72)的三种多肽。抗原PSD - 95也存在于小鼠和大鼠的PSD中,在啮齿动物或牛脑的细胞质、髓磷脂、线粒体和微粒体中几乎不存在。抗原PSD - 82和PSD - 72存在于牛脑的所有亚细胞组分中,尤其是线粒体中,但在啮齿动物脑中几乎不存在。该抗血清还含有针对微管蛋白的低亲和力抗体。(b)在小鼠和大鼠脑中进行了免疫组织化学研究,在用纯化的脑微管蛋白吸附后,抗原PSD - 95占抗血清结合的90%。在光学显微镜水平,仅在已知存在突触的脑区观察到抗体结合。在有髓神经纤维束、神经元细胞质或非神经元细胞中未观察到反应。在齿状回的分子层、海马的原层和辐射层以及小脑的分子层中观察到强反应性。实验性损伤,如大鼠内嗅皮层切除或脑室内注射 kainic 酸,导致海马结构特定区域的PSD大量丢失,这些区域的免疫反应性相应降低。免疫组织化学染色的异常模式与 reeler 和 staggerer 小鼠突变体小脑的异常突触模式相关。(c)在电子显微镜水平,仅在PSD中可检测到免疫反应性。该抗体不与髓磷脂、线粒体或质膜结合。(d)结果表明,抗原PSD - 95主要或仅位于PSD中,可在亚细胞分级分离过程中用作标志物。其他潜在用途包括突触发生的研究以及在神经系统实验性扰动后突触数量变化的检测。

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