Tubulin orientation in microtubules probed with domain-specific antibodies.

Acta histochemica. Supplementband Pub Date : 1991-01-01
P Dráber, E Dráberová, I Linhartová, V Viklický
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Abstract

A panel of monoclonal antibodies specific to alpha- or beta-tubulin subunits was used to study the location of tubulin molecules in microtubules. Limited proteolysis of tubulin with trypsin and chymotrypsin followed by immunoblotting demonstrated that the antibodies discriminated between structural domains of tubulin subunits. Antibodies against N-terminal domains were tested for their ability to interfere with the formation of microtubules in vitro. Although the antibodies exhibited similar association constants when tested on immobilized tubulin, they differed in their inhibitory effect on microtubule assembly. The sedimentation assay using microtubules prepared from purified tubulin showed an almost undetectable binding of the antibodies with the strongest inhibitory power to the microtubules. Immunofluorescence staining of unfixed detergent-extracted cells revealed that antibodies to determinants on C-terminal domains labelled microtubules, but these were not decorated with antibodies against N-terminal domains. The same results were obtained after a microinjection of antibodies into living cells. The data indicate that while parts of C-terminal domains of both subunits are exposed on the exterior of microtubules, considerable regions of the N-terminal domains are not. The surface regions of N-terminal domains appear to be involved in the formation of microtubules.

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用结构域特异性抗体探测微管中的微管蛋白取向。
一组针对α -或β -微管蛋白亚基的单克隆抗体被用来研究微管中微管蛋白分子的位置。用胰蛋白酶和凝乳胰蛋白酶对微管蛋白进行有限的蛋白水解,随后进行免疫印迹检测,证明抗体能够区分微管蛋白亚基的结构域。针对n端结构域的抗体在体外测试了其干扰微管形成的能力。虽然抗体在固定微管蛋白上表现出相似的结合常数,但它们对微管组装的抑制作用不同。用纯化微管蛋白制备的微管进行沉降试验,发现对微管具有最强抑制能力的抗体几乎检测不到结合。未固定的洗涤剂提取细胞的免疫荧光染色显示,c端结构域上的决定因子抗体标记了微管,但这些微管没有修饰针对n端结构域的抗体。将抗体微量注射到活细胞中也得到了同样的结果。数据表明,虽然这两个亚基的c端结构域的一部分暴露在微管的外部,但n端结构域的相当大区域却没有。n端结构域的表面区域似乎参与了微管的形成。
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Immunocytochemical characterization of cytomegalovirus (CMV) infected giant cells in perinatal acquired human immunodeficiency virus (HIV) infection. Transglutaminase activity in human brain tumors. Is it still adequate to study the nervous system using methods of catalytic enzyme histochemistry? [Histochemical representation of acetylcholinesterase in Alzheimer's disease]. [Changes of microenvironment and tumor cell heterogeneity--consequences for bioptic diagnosis].
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