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Etiopathogenesis of primary biliary cirrhosis 被引量:9
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作者 Ana Lleo Pietro Invernizzi +3 位作者 Ian R Mackay Harry Prince Ren-Qian Zhong M Eric Gershwin 《World Journal of Gastroenterology》 SCIE CAS CSCD 2008年第21期3328-3337,共10页
Primary biliary cirrhosis(PBC) is an autoimmune disease of the liver characterized by progressive bile duct destruction eventually leading to cirrhosis and liver failure.The serological hallmark of the disease is the ... Primary biliary cirrhosis(PBC) is an autoimmune disease of the liver characterized by progressive bile duct destruction eventually leading to cirrhosis and liver failure.The serological hallmark of the disease is the presence of circulating antimitochondrial antibodies(AMA).These reflect the presence of autoreactive T and B cells to the culprit antigens,the E2 subunits of mitochondrial 2-oxo-acid dehydrogenase enzymes,chiefly pyruvate dehydrogenase(PDC-E2).The disease results from a combination of genetic and environmental risk factors.Genetic predisposition is indicated by the higher familial incidence of the disease particularly among siblings and the high concordance rate among monozygotic twins.Environmental triggering events appear crucial to disrupt a pre-existing unstable immune tolerance of genetic origin allowing,after a long latency,the emergence of clinical disease.Initiating mimetopes of the vulnerable epitope of the PDC-E2 autoantigen can be derived from microbes that utilize the PDC enzyme or,alternatively,environmental xenobiotics/chemical compounds that modify the structure of native proteins to make them immunogenic.A further alternative as a source of antigen is PDC-E2 derived from apoptotic cells.In the effector phase the biliary ductular cell,by reason of itsproclivity to express the antigen PDC-E2 in the course of apoptosis,undergoes a multilineage immune attack comprised of CD4+ and CD8+ T cells and antibody.In this article,we critically review the available evidence on etiopathogenesis of PBC and present interpretations of complex data,new developments and theories,and nominate directions for future research. 展开更多
关键词 AUTOANTIBODIES Autoreactive T cells 2-oxoacid dehydrogenase Biliary epithelial cells Primary biliary cirrhosis
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捻转血矛线虫BLAODA蛋白单克隆抗体的制备及在诊断中的初步应用 被引量:3
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作者 卡力比夏提·艾木拉江 文兆海 +4 位作者 陆明敏 徐立新 宋小凯 李祥瑞 严若峰 《中国兽医科学》 CAS CSCD 北大核心 2022年第6期753-760,共8页
为了研究捻转血矛线虫排泄分泌蛋白生物素脂酰结合和2-氧酸脱氢酶酰基转移酶(BLAODA)在捻转血矛线虫病诊断中的应用,以重组捻转血矛线虫BLAODA为免疫原,通过杂交瘤细胞技术,筛出4株稳定分泌抗BLAODA单克隆抗体细胞株,分别命名为1B2、1G4... 为了研究捻转血矛线虫排泄分泌蛋白生物素脂酰结合和2-氧酸脱氢酶酰基转移酶(BLAODA)在捻转血矛线虫病诊断中的应用,以重组捻转血矛线虫BLAODA为免疫原,通过杂交瘤细胞技术,筛出4株稳定分泌抗BLAODA单克隆抗体细胞株,分别命名为1B2、1G4、2E3和5B4。将这4株杂交瘤细胞分别接种小鼠腹腔,制备腹水,用层析柱纯化抗体并建立双抗体夹心ELISA方法。结果显示:筛选出的1B2、1G4、2E3和5B4细胞株产生的抗体效价高、特异性强,其抗体亚型均为Ig G1型,轻链均为kappa型,纯化的小鼠腹水的效价均可达1∶2^(22);基于抗捻转血矛线虫BLAODA的单抗1B2、5B4建立了双抗体夹心ELISA检测方法,其敏感性为90.6%,特异性为90.6%。本研究获得了捻转血矛线虫抗BLAODA单克隆抗体并建立了双抗体夹心ELISA方法,为捻转血矛线虫诊断试剂盒的开发奠定了基础。 展开更多
关键词 捻转血矛线虫 BLAODA蛋白 单克隆抗体 双抗体夹心ELISA
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