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格雷夫斯眼眶组织中的免疫球蛋白A:通过聚合酶链反应进行脱氧核糖核酸扩增

Immunoglobulin A in Graves' orbital tissue: deoxyribonucleic acid amplification by polymerase chain reaction.

作者信息

McLachlan S M, Prummel M F, Jaume J C, Rapoport B

机构信息

Thyroid Molecular Biology Unit, V.A. Medical Center, San Francisco, California.

出版信息

J Endocrinol Invest. 1994 Apr;17(4):247-52. doi: 10.1007/BF03348969.

Abstract

A role for IgA autoantibodies in Graves' ophthalmopathy is suggested by the presence of immunoglobulins of this class in Graves' orbital tissue, as detected by immunohistochemistry. We, therefore, investigated the possibility of using the polymerase chain reaction (PCR) to amplify IgA immunoglobulin genes from plasma cells infiltrating Graves' eye tissue. Template cDNA was reverse-transcribed from orbital muscle (M) mRNA of one patient (#7) and from orbital connective tissue/fat (F) mRNA of two patients (#1 and #7), both undergoing surgery for exophthalmos because of severe infiltrative ophthalmopathy. Preliminary studies to establish the PCR procedure were performed for kappa light chain DNA amplification. With the very small amount of orbital tissue template available, the sensitive "hot start" modification of the PCR was necessary to amplify significant amounts of kappa light chain DNA. Using this procedure, IgA heavy chain DNA was amplified from both connective tissue/fat (F7) and muscle (M7) cDNA of patient #7. The DNA yield was less for IgA than for IgG using the same template. There was no significant IgA (or IgG) DNA product using the connective tissue/fat cDNA of patient #1. While not implying that IgA-infiltrating plasma cells are specific for Graves' orbital tissue, our studies nevertheless demonstrate the feasibility of amplifying the genes coding for IgA antibodies from Graves' orbital tissue plasma cells. Expression of these immunoglobulin genes in future studies will make it possible to determine the antigen specificity of the antibodies expressed by Graves' orbital tissue plasma cells.

摘要

免疫组织化学检测发现格雷夫斯眼眶组织中存在此类免疫球蛋白,提示IgA自身抗体在格雷夫斯眼病中发挥作用。因此,我们研究了利用聚合酶链反应(PCR)从浸润格雷夫斯眼组织的浆细胞中扩增IgA免疫球蛋白基因的可能性。模板cDNA是从一名患者(#7)的眼眶肌肉(M)mRNA以及两名因严重浸润性眼病接受眼球突出症手术的患者(#1和#7)的眼眶结缔组织/脂肪(F)mRNA反转录而来。为进行κ轻链DNA扩增开展了建立PCR程序的初步研究。鉴于可用的眼眶组织模板量极少,有必要对PCR采用灵敏的“热启动”改良法来扩增足量的κ轻链DNA。采用此程序,从患者#7的结缔组织/脂肪(F7)和肌肉(M7)cDNA中均扩增出了IgA重链DNA。使用相同模板时,IgA的DNA产量低于IgG。患者#1的结缔组织/脂肪cDNA未产生显著的IgA(或IgG)DNA产物。虽然这并不意味着浸润IgA的浆细胞对格雷夫斯眼眶组织具有特异性,但我们的研究仍证明了从格雷夫斯眼眶组织浆细胞中扩增编码IgA抗体的基因的可行性。在未来研究中这些免疫球蛋白基因的表达将有助于确定格雷夫斯眼眶组织浆细胞所表达抗体的抗原特异性。

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