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通过对活的人表皮进行胰蛋白酶消化释放出的落叶型天疱疮抗原的可溶性且具有免疫反应性的片段。

A soluble and immunoreactive fragment of pemphigus foliaceus antigen released by trypsinization of viable human epidermis.

作者信息

Martins C R, Labib R S, Rivitti E A, Diaz L A

机构信息

Department of Dermatology, Medical College of Wisconsin, Milwaukee.

出版信息

J Invest Dermatol. 1990 Aug;95(2):208-12. doi: 10.1111/1523-1747.ep12478018.

Abstract

Pemphigus foliaceus (PF) antigen is a transmembrane desmosomal glycoprotein (desmoglein I), part of which is located on the keratinocyte surface. Previous studies have shown that after trypsinization of viable human epidermis, this antigen is no longer detected on the surface of detached keratinocytes. It was not known, however, if this loss of antigenic activity was due to destruction, internalization, or cleavage of the antigen itself. In the present study we investigated the fate of the PF antigen after trypsinization of viable human skin. By using Concanavalin-A agarose affinity chromatography, we could partially purify an antigenic glycoprotein fraction that was released by trypsinization into the medium. This antigenic fraction was radiolabeled and tested by immunoprecipitation using sera from endemic pemphigus foliaceus or fogo selvagem (FS), non-endemic pemphigus foliaceus (NEPF), pemphigus vulgaris (PV), and bullous pemphigoid (BP) patients, and sera from normal subjects as controls. Immunoprecipitated labeled proteins were analyzed by SDS-PAGE and autoradiography. All FS sera (20 of 20 FS and five of five NEPF) and 46% of the PV sera (six of 13) immunoprecipitated a band of 45-kD molecular weight. Sera from FS patients in prolonged clinical and serological remission (seven of 10), sera from BP patients (five of five), and sera from normal donors (nine of nine) did not precipitate this 45-kD band. This study showed that a fragment of the PF antigen is released by trypsinization of human skin as a soluble immunoreactive glycopeptide of 45-kD molecular weight. Additionally, this procedure has generated sufficient quantities of the PF antigen for further biochemical characterization.

摘要

落叶型天疱疮(PF)抗原是一种跨膜桥粒糖蛋白(桥粒芯糖蛋白I),其部分位于角质形成细胞表面。先前的研究表明,对活的人表皮进行胰蛋白酶消化后,在脱离的角质形成细胞表面不再检测到这种抗原。然而,尚不清楚这种抗原活性的丧失是由于抗原本身的破坏、内化还是裂解。在本研究中,我们调查了对活的人皮肤进行胰蛋白酶消化后PF抗原的去向。通过使用伴刀豆球蛋白A琼脂糖亲和层析,我们能够部分纯化一种抗原性糖蛋白组分,该组分在胰蛋白酶消化后释放到培养基中。对该抗原性组分进行放射性标记,并使用来自地方性落叶型天疱疮或丛林型天疱疮(FS)、非地方性落叶型天疱疮(NEPF)、寻常型天疱疮(PV)和大疱性类天疱疮(BP)患者的血清以及来自正常受试者的血清作为对照,通过免疫沉淀进行检测。通过SDS - PAGE和放射自显影分析免疫沉淀的标记蛋白。所有FS血清(20份FS血清中的20份和5份NEPF血清中的5份)以及46%的PV血清(13份中的6份)免疫沉淀出一条分子量为45 kD的条带。处于长期临床和血清学缓解期的FS患者血清(10份中的7份)、BP患者血清(5份中的5份)以及正常供体血清(9份中的9份)未沉淀出这条45 kD的条带。本研究表明,人皮肤经胰蛋白酶消化后会释放出PF抗原的一个片段,其为一种分子量为45 kD的可溶性免疫反应性糖肽。此外,该方法产生了足够量的PF抗原用于进一步的生化特性分析。

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