人类和啮齿动物肝脏应激蛋白作为潜在生物标志物的比较二维电泳图谱。

F A Witzmann, C Fultz, J Lipscomb
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摘要

啮齿类动物的毒理学研究表明,蛋白质的二维聚丙烯酰胺凝胶电泳(2DE)通过在分子水平上提供细胞状态的信息,在化学毒性的检测和评估中非常有用。为了开发基于电泳的测试系统,需要识别一组特定的暴露或影响的生物标志物,并对特定的啮齿动物和人类目标组织具有倾向性。在这方面,应激蛋白,如热休克和葡萄糖调节蛋白(Hsp和Grp),是合适的候选人。目前的研究是在人类和大鼠肝脏匀浆的常规二维电泳凝胶模式上鉴定这些应激蛋白。鉴定了以下应激蛋白,绘制了它们的x、y坐标位置,确定了它们的丰度,并对这些数据进行了统计分析和比较:Hsp25、Hsp32、Hsp60、Hsc70、Hsp70、Hsp90、Grp75、Grp78、Grp94、蛋白二硫异构酶(PDI)和ER-60。除了Hsp25和Hsp32外,所检测的应激蛋白在非应激的人和大鼠肝脏中均以可检测的水平组成性表达;几乎完全相同的图案。根据我们的研究结果,人类肝脏2DE应激蛋白模式似乎非常适合毒理学筛选,特别是在体外应用和通过啮齿动物暴露的推断。
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Comparative 2D-electrophoretic mapping of human and rodent hepatic stress proteins as potential biomarkers.

Toxicologic studies in rodents demonstrate that two-dimensional polyacrylamide gel electrophoresis of proteins (2DE) is very useful in the detection and evaluation of chemical toxicity by providing information regarding cellular status at the molecular level. Identification of a set of specific biomarkers of exposure or effect, with a proclivity for both a particular rodent and human target tissue, is required for development of an electrophoretically based testing system. In this regard, stress proteins, such as the heat shock and glucose-regulated proteins (Hsp and Grp), are appropriate candidates. The present investigation was undertaken to identify these stress proteins on conventional two-dimensional electrophoretic gel patterns of human and rat liver homogenates. The following stress proteins were identified, their x, y coordinate positions mapped, and abundances determined, and these data statistically analyzed and compared: Hsp25, Hsp32, Hsp60, Hsc70, Hsp70, Hsp90, Grp75, Grp78, Grp94, protein disulfide isomerase (PDI), and ER-60. With the exception of Hsp25 and Hsp32, the stress proteins examined were constitutively expressed at detectable levels in both unstressed human and rat liver; in virtually identical patterns. Based on our results, the human hepatic 2DE stress protein pattern seems well-suited to toxicologic screening particularly in in vitro applications and via extrapolations from rodent exposures.

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