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人类髓系抗原(gp160,95;gp150;gp67)的进一步特性分析:使用属于CD-11b、CD-13和CD-33的单克隆抗体组研究表位异质性和非造血分布。

Further characterization of human myeloid antigens (gp160,95; gp150; gp67): investigation of epitopic heterogeneity and non-haemopoietic distribution using panels of monoclonal antibodies belonging to CD-11b, CD-13 and CD-33.

作者信息

Favaloro E J, Bradstock K F, Kabral A, Grimsley P, Zowtyj H, Zola H

机构信息

Department of Haematology, ICPMR, Westmead Hospital, NSW, Australia.

出版信息

Br J Haematol. 1988 Jun;69(2):163-71. doi: 10.1111/j.1365-2141.1988.tb07618.x.

Abstract

We have investigated the binding of over 30 different monoclonal antibodies (MAB) belonging to three distinct clusters of differentiation (CD-11b; CD-13; CD-33; as defined by the Third International Workshop on Leucocyte Differentiation Antigens (ILWS), 1986), and which are reactive with three distinct myeloid restricted surface antigens ('gp160,95'; 'gp150'; 'gp67'). By investigating reactivity with non-haemopoietic cells, we have confirmed that CD-11b and CD-33 MAB reactivity is largely restricted to haemopoietic cells, whilst CD-13 MAB showed additional binding to a wide range of non-haemopoietic cells. Epitopic heterogeneity was also investigated within each cluster of differentiation. Tested anti-CR3 (CD-11b) MAB varied in their ability to block the binding of complement coated sheep red blood cells and zymosan particles. A more detailed analysis of MAB binding heterogeneity was performed by competitive inhibition assays. It was demonstrated that MAB from both CD-11b and CD-13 bind to several distinct epitopes (at least six and five respectively) on their respective antigen molecules. In contrast, CD-33 MAB appear to bind to only a single site on 'gp67'. These data may allow for a clearer appreciation of the disparate functional effects obtained using different MAB reagents to individual myeloid antigens, as reported by a number of workers.

摘要

我们研究了30多种不同的单克隆抗体(MAB)的结合情况,这些抗体属于三个不同的分化簇(CD-11b、CD-13、CD-33;根据1986年第三届白细胞分化抗原国际研讨会(ILWS)的定义),并且与三种不同的髓系限制性表面抗原(“gp160,95”、“gp150”、“gp67”)发生反应。通过研究与非造血细胞的反应性,我们证实CD-11b和CD-33单克隆抗体的反应性主要局限于造血细胞,而CD-13单克隆抗体则显示出与多种非造血细胞有额外的结合。我们还研究了每个分化簇内的表位异质性。测试的抗CR3(CD-11b)单克隆抗体在阻断补体包被的绵羊红细胞和酵母聚糖颗粒结合的能力上有所不同。通过竞争抑制试验对单克隆抗体结合异质性进行了更详细的分析。结果表明,来自CD-11b和CD-13的单克隆抗体分别与其各自抗原分子上的几个不同表位结合(分别至少有六个和五个)。相比之下,CD-33单克隆抗体似乎只与“gp67”上的一个位点结合。正如许多研究人员所报道的,这些数据可能有助于更清楚地理解使用不同的单克隆抗体制剂针对个体髓系抗原所获得的不同功能效应。

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