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佛波酯对慢性淋巴细胞白血病细胞的表型调节:IgM分泌的诱导及B细胞相关表面抗原表达的变化

Phenotypic modulation of chronic lymphocytic leukemia cells by phorbol ester: induction of IgM secretion and changes in the expression of B cell-associated surface antigens.

作者信息

Gordon J, Mellstedt H, Aman P, Biberfeld P, Klein G

出版信息

J Immunol. 1984 Jan;132(1):541-7.

PMID:6606672
Abstract

Freshly explanted neoplastic populations from 22 cases of phenotypically well-characterized chronic type B lymphocytic leukemia were studied for their capacity to respond to the phorbol ester TPA in vitro. In all but four cases the secretion of IgM was either induced or increased, often to a high level. In contrast, the export of free immunoglobulin (Ig) light chains, an almost consistent feature of the B lymphocytic leukemias, remained relatively constant after TPA treatment. Parallel changes in leukemic cell surface phenotype were probed with both "conventional" and monoclonal antibodies, revealing some modulation of markers in every case investigated. A diminution in the level of surface Ig (preferentially IgD) and the accumulation of cytoplasmic Ig observed after phorbol ester treatment were accompanied by a corresponding reduction or loss of the B1 antigen and usually of B2 when present. The most consistent change induced by TPA was the appearance of BB-1, a marker of activated B lymphocytes, which was rarely expressed on fresh leukemic cells. Another marker of activated lymphocytes, LB-1, was also often induced or increased in its expression after exposure of the cells to TPA. The magnitude of the TPA response appeared to relate to the stage of maturation arrest of the individual leukemic clones rather than to any clinical parameter explored. The significance of the findings to normal B cell differentiation and their potential clinical utility are discussed.

摘要

对22例表型特征明确的慢性B淋巴细胞白血病新鲜分离的肿瘤细胞群进行了体外对佛波酯TPA反应能力的研究。除4例病例外,其余所有病例中IgM的分泌均被诱导或增加,且常达到高水平。相比之下,游离免疫球蛋白(Ig)轻链的输出,这是B淋巴细胞白血病几乎一致的特征,在TPA处理后保持相对恒定。用“传统”抗体和单克隆抗体检测白血病细胞表面表型的平行变化,发现在每例研究病例中标志物都有一些调节。佛波酯处理后观察到表面Ig(优先为IgD)水平降低和细胞质Ig积累,同时B1抗原相应减少或缺失,若存在B2抗原通常也会如此。TPA诱导的最一致变化是出现BB - 1,这是活化B淋巴细胞的标志物,在新鲜白血病细胞上很少表达。另一个活化淋巴细胞的标志物LB - 1在细胞暴露于TPA后其表达也常被诱导或增加。TPA反应的程度似乎与各个白血病克隆的成熟停滞阶段有关,而不是与所探索的任何临床参数有关。讨论了这些发现对正常B细胞分化的意义及其潜在的临床应用价值。

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