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氟烷相关性肝炎患者血清中抗人肝内质网自身抗体的检测

Detection of autoantibodies directed against human hepatic endoplasmic reticulum in sera from patients with halothane-associated hepatitis.

作者信息

Kitteringham N R, Kenna J G, Park B K

机构信息

Department of Pharmacology and Therapeutics, University of Liverpool, London.

出版信息

Br J Clin Pharmacol. 1995 Oct;40(4):379-86. doi: 10.1111/j.1365-2125.1995.tb04560.x.

Abstract
  1. Previous studies have demonstrated the presence of antibodies to trifluoroacetylated hepatic proteins (TFA-proteins) in sera from patients with the severe form of halothane-associated hepatitis (halothane hepatitis). The TFA-proteins are produced via cytochrome P450-mediated metabolism of halothane to the reactive species TFA-chloride. 2. To investigate the presence of autoantibodies (which recognize various non-TFA-modified human hepatic polypeptides) in patients with halothane hepatitis immunoblotting experiments were performed using microsomal fractions prepared freshly from livers of five different (halothane-free) tissue donors. Blots were developed using 15 well-characterised sera from patients with halothane hepatitis. 3. Autoantibodies to human hepatic polypeptides were detected in most, but not all, of the patients' sera. The pattern of antibody reactivity varied markedly between sera. Although no common pattern of antibody recognition was observed, polypeptides of molecular mass between 60 and 80 kDa were the predominant targets. A similar protein recognition pattern was seen when each positive serum was tested against the five individual human liver samples. 4. Such autoantibodies were not detected in sera from 16 normal human blood donors, but were detected in three of six sera from patients exposed to halothane without developing hepatitis. 5. The autoantibodies are thought to arise in patients exposed to halothane as a consequence of a halothane-induced immune response to chemically-modified proteins. Such antibodies could contribute to the complex pathological processes involved in halothane hepatitis.
摘要
  1. 先前的研究已证实在患有严重型氟烷相关性肝炎(氟烷肝炎)患者的血清中存在针对三氟乙酰化肝蛋白(TFA - 蛋白)的抗体。TFA - 蛋白是通过细胞色素P450介导的氟烷代谢生成反应性物质三氟乙酰氯而产生的。2. 为了研究氟烷肝炎患者中自身抗体(识别各种非TFA修饰的人肝多肽)的存在情况,使用从五个不同(无氟烷)组织供体的肝脏新鲜制备的微粒体组分进行了免疫印迹实验。使用来自氟烷肝炎患者的15份特征明确的血清对印迹进行显影。3. 在大多数但并非所有患者血清中检测到了针对人肝多肽的自身抗体。血清之间抗体反应模式差异明显。尽管未观察到共同的抗体识别模式,但分子量在60至80 kDa之间的多肽是主要靶标。当每份阳性血清针对五个单独的人肝样本进行检测时,观察到类似的蛋白质识别模式。4. 在16名正常人类献血者的血清中未检测到此类自身抗体,但在六名接触氟烷但未患肝炎的患者的血清中有三份检测到了。5. 这些自身抗体被认为是在接触氟烷的患者中由于氟烷诱导的对化学修饰蛋白的免疫反应而产生的。此类抗体可能促成了氟烷肝炎所涉及的复杂病理过程。
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8a84/1365157/c1dd28849aa0/brjclinpharm00003-0092-a.jpg

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