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增殖性骨髓瘤细胞的B细胞表面表型:免疫治疗的靶抗原

B-cell surface phenotypes of proliferating myeloma cells: target antigens for immunotherapy.

作者信息

Chan C S, Wormsley S B, Pierce L E, Peter J B, Schechter G P

机构信息

Hematology Section, Veterans Administration Medical Center, Washington, DC 20422.

出版信息

Am J Hematol. 1990 Feb;33(2):101-9. doi: 10.1002/ajh.2830330206.

DOI:10.1002/ajh.2830330206
PMID:2301368
Abstract

Dual-parameter flow cytometric analysis of B-cell antigens and DNA content was used to determine the phenotypes of proliferating tumor cells (S-phase cells) from 30 patients with multiple myeloma. B4 (CD19), J5 (CALLA, CD10), B1 (CD20), and monotypic surface immunoglobulin (Slg) were expressed heterogeneously in 24 patients. J5 and monotypic Slg were found most frequently but were always expressed on a significantly lower percentage of cells than the antigens typically associated with plasma cells, cytoplasmic immunoglobulin (Clg) and T10 (CD38). S-phase cells were found in each antigen(+) subset. B antigen(+) cycling cells were demonstrated in 16 patients whose marrow or blood cells expressed B antigens exclusively in the hyperdiploid fraction and therefore were certainly part of the myeloma clone. Similar to the low level of proliferative activity of the T10(+), Clg(+), and PCA1(+) subsets, the percentages of cycling cells of the preplasma cell B-antigen-bearing myeloma subsets ranged from less than 1% to 12%. The tumor cells of four patients were also studied with dual-color surface antigen analysis and demonstrated independent expression of B antigens, with only rare coexpression of T10 and monotypic Slg, J5, or B4. These findings are consistent with the presence of distinct myeloma subsets bearing differing B phenotypes in the same tumor and provide evidence that the proliferation in myeloma is occurring at various developmental stages in the malignant B lineage. These antigens may be important targets for immunologic therapy aimed at eliminating the entire proliferating compartment of this B-cell tumor.

摘要

采用双参数流式细胞术分析B细胞抗原和DNA含量,以确定30例多发性骨髓瘤患者增殖肿瘤细胞(S期细胞)的表型。B4(CD19)、J5(CALLA,CD10)、B1(CD20)和单型表面免疫球蛋白(Slg)在24例患者中呈异质性表达。J5和单型Slg最为常见,但在细胞上的表达百分比始终显著低于通常与浆细胞相关的抗原,即细胞质免疫球蛋白(Clg)和T10(CD38)。在每个抗原阳性亚群中均发现了S期细胞。在16例患者中发现了B抗原阳性的循环细胞,这些患者的骨髓或血细胞仅在超二倍体部分表达B抗原,因此肯定是骨髓瘤克隆的一部分。与T10阳性、Clg阳性和PCA1阳性亚群的低增殖活性相似,前浆细胞B抗原阳性骨髓瘤亚群的循环细胞百分比范围为不到1%至12%。对4例患者的肿瘤细胞也进行了双色表面抗原分析,结果显示B抗原独立表达,T10与单型Slg、J5或B4仅罕见共表达。这些发现与同一肿瘤中存在具有不同B表型的不同骨髓瘤亚群一致,并提供了证据表明骨髓瘤的增殖发生在恶性B细胞系的不同发育阶段。这些抗原可能是旨在消除这种B细胞肿瘤整个增殖区室的免疫治疗的重要靶点。

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引用本文的文献

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Med Oncol. 1996 Mar;13(1):1-7. doi: 10.1007/BF02988835.
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The bone marrow of multiple myeloma patients contains B cell populations at different stages of differentiation that are clonally related to the malignant plasma cell.多发性骨髓瘤患者的骨髓中含有处于不同分化阶段的B细胞群体,这些群体与恶性浆细胞存在克隆相关性。
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