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B 细胞慢性淋巴细胞白血病中的循环单克隆 IgM 蛋白:其鉴定、特征及其与膜 IgM 的关系。

Circulating monoclonal IgM proteins in B cell chronic lymphocytic leukemia: their identification, characterization and relationship to membrane IgM.

作者信息

Qian G X, Fu S M, Solanki D L, Rai K R

出版信息

J Immunol. 1984 Dec;133(6):3396-400.

PMID:6333459
Abstract

Accumulated evidence indicates that there is a circulating monoclonal Ig protein related to the leukemic cell-associated Ig in the majority of patients with B cell chronic lymphocytic leukemia (CLL) despite the failure to demonstrate such a protein by conventional serum electrophoresis. Methodology has been developed to reveal these hidden monoclonal bands and to show that they are related to the leukemia-associated membrane Ig (mIg). Of nine CLL cases with stainable mIgM and without discernable plasma Ig bands, marked hypogammaglobulinemia was evident in six. In the other three, a significant amount of protein was present in the gamma region. IgM was isolated from the plasma of these patients by affinity chromatography with Sepharose-4B, conjugated with affinity purified anti-human IgM antibodies. One to 3 mg were isolated from 20 to 40 ml of plasma. Agarose electrophoresis revealed a monoclonal Ig band in the isolated IgM in all cases. Eight of these IgM proteins were analyzed by high-pressure liquid chromatography. Five were found to be pentameric IgM. In the remaining three, various amounts of monomeric IgM were detected. Attempts to make anti-idiotypic antibodies to the isolated proteins have been successful. Thus far, a rabbit anti-idiotypic antiserum was obtained in one case and two mouse monoclonal anti-idiotypic antibodies in two additional cases. Immunofluorescence analysis revealed that plasma IgM and mIgM shared similar idiotypic determinants. One other monoclonal antibody was shown to be specific for a V region marker of a minor Ig population. These findings indicate that B leukemic lymphocytes do secrete a small amount of IgM and lend further support to the thesis that the maturation defect in CLL is incomplete. It is also feasible to isolate the secreted IgM and to produce anti-idiotypic antibodies to them. In view of the potential therapeutic effect of anti-idiotypic antibodies, this may offer an alternative and efficient approach to generate a large panel of anti-idiotypic antibodies for clinical trials. The possibility also exists that this approach is applicable to other B cell proliferative disorders such as the non-Hodgkin B cell lymphomas.

摘要

越来越多的证据表明,在大多数B细胞慢性淋巴细胞白血病(CLL)患者中,存在一种与白血病细胞相关免疫球蛋白(Ig)有关的循环单克隆Ig蛋白,尽管通过传统血清电泳未能检测到这种蛋白。现已开发出相关方法来揭示这些隐藏的单克隆条带,并表明它们与白血病相关膜免疫球蛋白(mIg)有关。在9例可染色mIgM且无明显血浆Ig条带的CLL病例中,6例有明显的低丙种球蛋白血症。另外3例在γ区存在大量蛋白质。通过用偶联了亲和纯化抗人IgM抗体的琼脂糖凝胶4B亲和层析从这些患者的血浆中分离出IgM。从20至40毫升血浆中分离出1至3毫克。琼脂糖凝胶电泳显示所有病例中分离出的IgM均有单克隆Ig条带。其中8种IgM蛋白通过高压液相色谱进行分析。发现5种为五聚体IgM。其余3种检测到不同量的单体IgM。制备针对分离蛋白的抗独特型抗体的尝试已获成功。到目前为止,1例获得了兔抗独特型抗血清,另外2例获得了2种小鼠单克隆抗独特型抗体。免疫荧光分析显示血浆IgM和mIgM具有相似的独特型决定簇。另一种单克隆抗体被证明对一小部分Ig群体的V区标志物具有特异性。这些发现表明B淋巴细胞白血病细胞确实分泌少量IgM,并进一步支持了CLL成熟缺陷不完全的论点。分离分泌的IgM并制备针对它们的抗独特型抗体也是可行的。鉴于抗独特型抗体的潜在治疗作用,这可能为生成大量用于临床试验的抗独特型抗体提供一种替代且有效的方法。这种方法也有可能适用于其他B细胞增殖性疾病,如非霍奇金B细胞淋巴瘤。

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