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Structural differences between brain beta 1- and beta 2-tubulins: implications for microtubule assembly and colchicine binding.

机译:脑β1-微管蛋白和β2-微管蛋白之间的结构差异:对微管组装和秋水仙碱结合的影响。

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摘要

Brain beta 1- and beta 2-tubulins are the major and minor beta-tubulin components of chordate brain tissue, respectively. Two cysteines of beta 1, but not beta 2, can be specifically cross-linked with the bifunctional sulfhydryl reagent N,N'-ethylenebis(iodoacetamide) (EBI). They are in positions 239 and 354. Although separated by 115 amino acid residues along the beta 1-chain, the two sulfur atoms are maximally 9 A apart in the beta 1 tertiary structure. The failure of beta 2 to form a similar cross-bridge is due to the absence of a cysteine in position 239. At least 10 other sequence differences are also present between beta 1 and beta 2. Positions 239 and 354 of beta 1 probably occupy a key part of the tubulin molecule. The microtubule assembly inhibitors colchicine and podophyllotoxin appear to bind on or near this site and EBI is a potent inhibitor of microtubule assembly. Furthermore, the beta 1-cysteine in position 239 appears to be the most reactive in brain tubulin under the given conditions. The marked difference between beta 1 and beta 2 in this critical region suggests that they may have different functions in brain tissue.
机译:脑β1-微管蛋白和β2-微管蛋白分别是胆酸盐脑组织的主要和次要β-微管蛋白成分。可以用双功能巯基试剂N,N'-亚乙基双(碘乙酰胺)(EBI)特异性地交联两个1型的半胱氨酸而不是2型的半胱氨酸。它们位于239和354位。尽管沿β1链被115个氨基酸残基隔开,但两个硫原子在β1三级结构中的最大距离为9A。 β2未能形成相似的跨桥是由于239位没有半胱氨酸。β1和β2之间也存在至少10个其他序列差异。β1的239位和354位可能占据微管蛋白分子的关键部分。微管组装抑制剂秋水仙碱和鬼臼毒素似乎在该部位或附近结合,EBI是微管组装的有效抑制剂。此外,在给定条件下,位置239处的β1-半胱氨酸在脑微管蛋白中的反应性最高。 beta 1和beta 2在此关键区域的明显区别表明它们在脑组织中可能具有不同的功能。

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