Differential isotype recognition of two centromere associated polypeptides by immunoblotting in connective tissue disease.

机译：在结缔组织疾病中通过免疫印迹对两种着丝粒相关多肽的差异同种型识别。

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On investigating the immunoblotting profile of 65 systemic sclerosis patients, a 140 kD polypeptide was recognised by sera from 16, when immunoblotted against a nuclear-enriched K562 cell sonicate. All 16 sera contained anticentromere antibodies (ACA) detected by immunofluorescence (IF) and 15 of 16 also recognized a 19 kD polypeptide on immunoblotting. Two ACA positive sera failed to recognize the 140 kD polypeptide but one of these recognized the 19 kD polypeptide. The 140 kD polypeptide identified a group with more limited skin involvement (P less than 0.05) and all 16 had Raynaud's phenomenon. The sera from three of 100 systemic lupus erythematosus (SLE) patients also recognized both polypeptides. On investigating the isotype specificity, the 140 kD polypeptide was strongly detected by an IgM autoantibody and the 19 kD polypeptide by an IgG autoantibody.

机译：在调查65例系统性硬化症患者的免疫印迹图谱时，当对富含核的K562细胞超声处理免疫印迹时，血清中可识别出140 kD多肽。所有16个血清均包含通过免疫荧光（IF）检测到的抗着丝粒抗体（ACA），并且16个血清中的15个在免疫印迹时也识别了19 kD多肽。两个ACA阳性血清无法识别140 kD多肽，但其中一个识别19 kD多肽。 140 kD多肽鉴定出一组皮肤受累程度有限（P小于0.05），并且全部16人都有雷诺现象。 100例系统性红斑狼疮（SLE）患者中有3例的血清也识别了这两种多肽。在研究同种型特异性时，通过IgM自身抗体强烈检测到140 kD多肽，通过IgG自身抗体强烈检测到19 kD多肽。

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期刊名称 Clinical and Experimental Immunology
作者
N J McHugh; I E James; P J Maddison;
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作者单位

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年(卷),期 1988(72),3
年度 1988
页码 457–464
总页数 8
原文格式 PDF
正文语种
中图分类免疫学;
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1. Rheumatoid factor isotypes in mixed connective tissue disease. [J] . Mimura Y, Ihn H, Jinnin M, Clinical rheumatology . 2006,第4期

机译：混合性结缔组织病中的类风湿因子同种型。
2. U1-RNP and TLR receptors in the pathogenesis of mixed connective tissue disease. Part I. The U1-RNP complex and its biological significance in the pathogenesis of mixed connective tissue disease [J] . Agnieszka Paradowska-Gorycka Reumatologia . 2015,第2期

机译：U1-RNP和TLR受体在混合性结缔组织病的发病机理中。第一部分：U1-RNP复合物及其在混合性结缔组织病发病机理中的生物学意义
3. Early undifferentiated connective tissue disease. V. An inception cohort 5 years later: disease remissions and changes in diagnoses in well established and undifferentiated connective tissue diseases. [J] . Williams HJ, Alarcon GS, Neuner R, The Journal of rheumatology . 1998,第2期

机译：早期未分化的结缔组织病。 V. 5年后的一个初始队列：疾病的缓解和确诊和未分化的结缔组织疾病的诊断改变。
4. Microscopic resolution imaging and proteomics correlation athistogeographically identical location:Point by point correlation between ex vivo tissue imaging with high field MRIand multiplex tissue immunoblotting for proteomics profiling [C] . Kant M. Matsuda, Joon-Yong Chung, Kris Ylaya, SPIE Conference on Biomedical applications in molecular, structural, and functional imaging . 2010

机译：显微分辨率成像和蛋白质组学相关性athistogegraphy相同的位置：通过对蛋白质组学分析的高场Mriand复用组织免疫印迹的前体内组织成像之间的点相关性
5. Studies on connective and neurological tissues in relation to disease. [D] . Madhurapantula, Rama Sashank. 2015

机译：与疾病有关的结缔组织和神经组织的研究。
6. Anti-A2/RA33 autoantibodies are directed to the RNA binding region of the A2 protein of the heterogeneous nuclear ribonucleoprotein complex. Differential epitope recognition in rheumatoid arthritis systemic lupus erythematosus and mixed connective tissue disease. [O] . K Skriner, W H Sommergruber, V Tremmel, 1997

机译：抗A2 / RA33自身抗体针对异质核核糖核蛋白复合物的A2蛋白的RNA结合区域。类风湿关节炎系统性红斑狼疮和混合性结缔组织病中的差异表位识别。
7. Anti-A2/RA33 autoantibodies are directed to the RNA binding region of the A2 protein of the heterogeneous nuclear ribonucleoprotein complex. Differential epitope recognition in rheumatoid arthritis, systemic lupus erythematosus, and mixed connective tissue disease. [O] . Skriner, K, Sommergruber, W H, Tremmel, V, 1997

机译：抗A2 / RA33自身抗体针对异质核核糖核蛋白复合物的A2蛋白的RNA结合区域。类风湿关节炎，系统性红斑狼疮和混合性结缔组织病中的差异表位识别。

Differential isotype recognition of two centromere associated polypeptides by immunoblotting in connective tissue disease.

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