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Activity of the Mitogenic Pasteurella multocida Toxin Requires an Essential C-Terminal Residue

机译:有丝分裂的多杀性巴氏杆菌毒素的活性需要基本的C端残基。

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摘要

Pasteurella multocida toxin (PMT) is a potent mitogen that also affects bone resorption. PMT acts intracellularly and is therefore postulated to have several domains involved in different aspects of its function. The toxin contains eight cysteine residues. Mutants with individual substitutions for each of these residues were constructed, and the effects of these on the biological activity of the toxin were determined by cultured-cell assays. Only the most C-terminal of the eight cysteines (C1165) was essential for full activity, although mutation of the cysteine residue at position 1159 caused a slight but reproducible loss of potency. In animal challenge experiments, mutant toxin (C1165S) was not toxic to piglets, even at doses exceeding a lethal dose of active PMT 1,000-fold. The mutant and wild-type toxins displayed identical purification characteristics, similar susceptibility to proteolytic digestion, and circular dichroism profiles, which indicated that no gross structural changes had taken place. The function of the essential C1165 residue is not yet known, although its most likely role is an enzymatic one at or near the catalytic center of the toxin.
机译:多杀性巴斯德氏菌毒素(PMT)是一种有效的促分裂原,也影响骨骼的吸收。 PMT在细胞内起作用,因此被假定具有与其功能的不同方面有关的几个域。该毒素包含八个半胱氨酸残基。构建了对这些残基中的每个残基进行单独取代的突变体,并通过培养细胞测定法确定了它们对毒素生物学活性的影响。尽管八个半胱氨酸(C1165)的最C末端对完整活性至关重要,但是1159位半胱氨酸残基的突变会导致效力的轻微但可再现的降低。在动物攻击实验中,即使毒素的致死剂量超过活性PMT的致死剂量1,000倍,突变毒素(C1165S)对仔猪也没有毒性。突变体和野生型毒素显示出相同的纯化特性,相似的蛋白水解消化敏感性和圆二色性,表明没有发生重大的结构变化。必需的C1165残基的功能尚不清楚,尽管它最可能的作用是在毒素催化中心或附近的酶促作用。

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