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恶性人类B细胞表达两种p24表面抗原群体。

Malignant human B cells express two populations of p24 surface antigens.

作者信息

Pesando J M, Hoffman P, Conrad T

出版信息

J Immunol. 1986 Apr 1;136(7):2709-14.

PMID:3485154
Abstract

Monoclonal antibodies (MoAb) to a leukemia-associated p24 cell surface antigen are currently being used to purge bone marrow of malignant cells before autologous transplantation for acute lymphoblastic leukemia (ALL). Their use as potential diagnostic reagents for hematologic disorders is also under investigation. It has been assumed throughout these investigations that the p24-specific MoAb produced by different laboratories all identify the same antigen. Our present studies indicate that at least two populations of p24 antigens, having different chemical properties and cellular distributions, exist on malignant B cells. For example, eight MoAb raised to ALL cells (ALL-MoAb) identify a p24 antigen on these cells but do not react with the Burkitt's lymphoma cell line Ramos. In contrast, six MoAb raised to Ramos (Ramos-MoAb) identify a p24 antigen on both Ramos and ALL cells. Quantitative binding of both sets of MoAb to ALL cells is comparable. The ALL-MoAb react with platelets, granulocytes, and activated but not resting T lymphocytes, whereas the Ramos-MoAb react with both resting and activated T lymphocytes but not with platelets or granulocytes. The ALL-MoAb react with 11 of 34 human hematopoietic cell lines tested; the Ramos-MoAb react with all 34. Both sets of MoAb react with most of the nonhematopoietic human cell lines tested. Reciprocal exhaustive radioimmune precipitation experiments performed with an ALL cell line indicate that the antigenic determinants recognized by these two sets of MoAb are present on different molecules. Similarly, proteolytic digests of iodinated antigens identified by these two sets of MoAb on ALL cells confirm the unique chemical identities of these molecules and suggest that they reflect the products of different genetic loci. The presence of the antigen identified by the Ramos-MoAb on every cell population tested except granulocytes suggests that it may serve an important cellular function. The existence of two populations of p24 antigens on at least some hematopoietic cells indicates the need for caution when comparing the results of studies of these antigens by groups employing different MoAb.

摘要

目前,针对白血病相关p24细胞表面抗原的单克隆抗体(MoAb)正被用于在急性淋巴细胞白血病(ALL)自体移植前清除骨髓中的恶性细胞。它们作为血液系统疾病潜在诊断试剂的用途也在研究中。在这些研究中一直假定,不同实验室产生的p24特异性MoAb都识别同一抗原。我们目前的研究表明,恶性B细胞上存在至少两种具有不同化学性质和细胞分布的p24抗原群体。例如,针对ALL细胞产生的8种MoAb(ALL - MoAb)识别这些细胞上的一种p24抗原,但不与伯基特淋巴瘤细胞系Ramos反应。相反,针对Ramos产生的6种MoAb(Ramos - MoAb)识别Ramos和ALL细胞上的一种p24抗原。两组MoAb与ALL细胞的定量结合相当。ALL - MoAb与血小板、粒细胞以及活化但非静止的T淋巴细胞反应,而Ramos - MoAb与静止和活化的T淋巴细胞都反应,但不与血小板或粒细胞反应。ALL - MoAb与所测试的34种人类造血细胞系中的11种反应;Ramos - MoAb与所有34种反应。两组MoAb都与所测试的大多数非造血人类细胞系反应。用一个ALL细胞系进行的相互彻底放射免疫沉淀实验表明,这两组MoAb识别的抗原决定簇存在于不同分子上。同样,这两组MoAb在ALL细胞上识别的碘化抗原的蛋白水解消化证实了这些分子独特的化学特性,并表明它们反映了不同基因座的产物。除粒细胞外,在每个测试细胞群体上都存在Ramos - MoAb识别的抗原,这表明它可能具有重要的细胞功能。至少在一些造血细胞上存在两种p24抗原群体,这表明在比较使用不同MoAb的研究组对这些抗原的研究结果时需要谨慎。

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