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外显子10和11在正常tau蛋白以及与成对螺旋丝相关的tau蛋白中的差异表达。

Differential expression of exons 10 and 11 in normal tau and tau associated with paired helical filaments.

作者信息

Ksiezak-Reding H, Shafit-Zagardo B, Yen S H

机构信息

Dept. of Pathology, Albert Einstein College of Medicine, Bronx, NY 10461, USA.

出版信息

J Neurosci Res. 1995 Aug 1;41(5):583-93. doi: 10.1002/jnr.490410504.

Abstract

Antibodies were raised to two synthetic peptides with amino acid sequences encoded by a variable region of exons 10 and 11 of the tau gene. The affinity-purified antibodies, designated E-10 and E-11, were used to determine whether PHF-tau and normal tau differ in variants containing three or four repeats in the microtubule-binding domain, respectively. Normal adult human brain was shown by gel electrophoresis to contain six isoforms of tau. All of the isoforms reacted with E-11, whereas only four of them with slower electrophoretic mobility were recognized by E-10. Fetal brain tau was readily recognized by E-11 but reacted poorly with E-10. In PHF preparations, E-11 bound to all three polypeptides of PHF-tau of 68 kD, 64 kD, and 60 kD and reacted intensely with a material smearing from the top of the gel to about the 50-kD region. In contrast, E-10 only weakly recognized the two higher molecular weight PHF-tau polypeptides of 68 kD and 64 kD, as well as smeared material, and the binding was not affected by phosphatase treatment. Using recombinant tau with four repeats as a reference, the immunoreactivity of E-10 with PHF-tau was estimated to be approximately 5% of that of E-11. By comparison, the immunoreactivity of E-10 with four isoforms of normal tau was comparable to that of E-11. These results indicate that the ratio of three vs. four repeat variants in PHF-tau is higher than in normal tau and suggest that Alzheimer disease may be associated with the disproportional expression of fetal (or juvenile) forms of tau. Alternatively, the weak reactivity of PHF-tau with E-10 antibody could be due to post-translational modifications other than phosphorylation.

摘要

针对由tau基因第10和11外显子可变区编码的两个合成肽段制备了抗体。将亲和纯化的抗体命名为E - 10和E - 11,用于确定PHF - tau和正常tau在微管结合结构域中分别含有三个或四个重复序列的变体中是否存在差异。凝胶电泳显示正常成人大脑含有六种tau异构体。所有异构体均与E - 11反应,而只有四种电泳迁移率较慢的异构体可被E - 10识别。胎儿脑tau很容易被E - 11识别,但与E - 10反应较弱。在PHF制剂中,E - 11与68 kD、64 kD和60 kD的所有三种PHF - tau多肽结合,并与从凝胶顶部延伸至约50 - kD区域的拖尾物质强烈反应。相比之下,E - 10仅微弱识别68 kD和64 kD的两种较高分子量的PHF - tau多肽以及拖尾物质,并且这种结合不受磷酸酶处理的影响。以具有四个重复序列的重组tau作为参照,估计E - 10与PHF - tau的免疫反应性约为E - 11的5%。相比之下,E - 10与四种正常tau异构体的免疫反应性与E - 11相当。这些结果表明,PHF - tau中三个重复序列与四个重复序列变体的比例高于正常tau,并提示阿尔茨海默病可能与胎儿(或幼年)形式的tau的不成比例表达有关。或者,PHF - tau与E - 10抗体的弱反应性可能是由于除磷酸化以外的翻译后修饰所致。

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