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使用游离硫醇半胱胺对突变型人类蛋白质进行体内改造。

In vivo alteration of a mutant human protein using the free thiol cysteamine.

作者信息

Gahl W A, Gregg R E, Hoeg J M, Fisher E

出版信息

Am J Med Genet. 1985 Feb;20(2):409-17. doi: 10.1002/ajmg.1320200226.

Abstract

Inborn errors of metabolism in which there is a mutant protein due to a cysteine for arginine substitution may be amenable to treatment with the free thiol cysteamine. Evidence for this derives from patients with type III hyperlipoproteinemia, who are homozygous for apolipoprotein E2, which differs in charge and in vitro function based on a single such amino acid substitution. The plasma of a type III hyperlipoproteinemic patient, when made at least 50 microM with respect to cysteamine in vitro, demonstrated a charge shift of the apolipoprotein E isoelectric focusing pattern from the E2 to the normal E3 and E4 positions. Two children treated for cystinosis with cysteamine each exhibited some charge alteration of their apoE3 to a form migrating in the apoE4 position. The use of thiol reagents such as cysteamine to specifically alter selected mutant human proteins, such as antithrombin III Toyama, may be added to our therapeutic armamentarium in the treatment of life-threatening metabolic disorders.

摘要

由于半胱氨酸替代精氨酸而存在突变蛋白的先天性代谢缺陷可能可用游离硫醇半胱胺进行治疗。这方面的证据来自III型高脂蛋白血症患者,他们是载脂蛋白E2的纯合子,基于单个这样的氨基酸替代,其电荷和体外功能有所不同。III型高脂蛋白血症患者的血浆在体外相对于半胱胺达到至少50微摩尔时,载脂蛋白E等电聚焦模式的电荷从E2转移到正常的E3和E4位置。两名用半胱胺治疗胱氨酸病的儿童,其各自的载脂蛋白E3均出现了一些电荷改变,变为在载脂蛋白E4位置迁移的形式。使用硫醇试剂如半胱胺来特异性改变选定的突变人类蛋白质,如抗凝血酶III富山型,可能会被添加到我们治疗危及生命的代谢紊乱的治疗手段中。

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