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在一项多维流式细胞术分析中,骨髓瘤患者CD19 + B淋巴细胞中未检测到肿瘤特异性非整倍体。

Tumor-specific aneuploidy not detected in CD19+ B-lymphoid cells from myeloma patients in a multidimensional flow cytometric analysis.

作者信息

McSweeney P A, Wells D A, Shults K E, Nash R A, Bensinger W I, Buckner C D, Loken M R

机构信息

Clinical Research Division, Fred Hutchinson Cancer Research Center, Seattle, WA 98104, USA.

出版信息

Blood. 1996 Jul 15;88(2):622-32.

PMID:8695810
Abstract

Aneuploidy and lg light chain restriction were used as separate, independent tumor specific markers to study 26 patients with multiple myeloma to determine whether bone marrow B cells, as defined by CD19 expression, are clonally related to myeloma plasma cells. Specimens were characterized using multidimensional flow cytometry to identify the presence of clonality in both the B lymphoid and plasma cell populations using both surface and cytoplasmic staining with antibodies specific for kappa or lambda lg light chain In none of the patients with multiple myeloma were CD19+ cells found to be clonally restricted to kappa or lambda. The monoclonal plasma cells (MPC) were found to be uniformly negative for CD10, CD19, and CD34, while the CD19+ B lymphoid cells present within the samples expressed normal intensities and relationships of these antigens, which allowed them to serve as internal positive controls. Combined analysis of call surface antigen expression and DNA content allowed plasma cell populations to be characterized for aneuploidy without interference from normal bone marrow cells. The MPC, detected on the basis of bright CD38 expression (CD38+2), demonstrated DNA aneuploidy in 65% of cases (DNA index range of 0.9 to 1.3). These aneuploid DNA distributions had typical cell cycle profiles (including G1,S and G2+M) expected of a proliferating population. In all cases, DNA aneuploidy was confined almost entirely to the CD38+2, CD19- malignant plasma cells, while cells expressing CD19 were diploid. These results support the concept that myeloma is a disease process mediated by self-replicating, late compartments of B-cell ontogeny.

摘要

非整倍体和Ig轻链限制被用作单独的、独立的肿瘤特异性标志物,以研究26例多发性骨髓瘤患者,确定由CD19表达定义的骨髓B细胞是否与骨髓瘤浆细胞存在克隆相关性。使用多维流式细胞术对标本进行表征,通过用针对kappa或lambda Ig轻链的抗体进行表面和细胞质染色,来鉴定B淋巴细胞和浆细胞群体中克隆性的存在。在所有多发性骨髓瘤患者中,均未发现CD19+细胞在kappa或lambda上存在克隆限制。发现单克隆浆细胞(MPC)对CD10、CD19和CD34均呈均匀阴性,而样本中存在的CD19+B淋巴细胞表达这些抗原的强度和关系正常,这使其能够作为内部阳性对照。对所有表面抗原表达和DNA含量的联合分析,使得浆细胞群体能够在不受正常骨髓细胞干扰的情况下进行非整倍体特征分析。基于明亮的CD38表达(CD38+2)检测到的MPC,在65%的病例中表现出DNA非整倍体(DNA指数范围为0.9至1.3)。这些非整倍体DNA分布具有增殖群体预期的典型细胞周期图谱(包括G1、S和G2+M)。在所有病例中,DNA非整倍体几乎完全局限于CD38+2、CD19-恶性浆细胞,而表达CD19的细胞为二倍体。这些结果支持了骨髓瘤是一种由B细胞个体发育的自我复制晚期阶段介导的疾病过程这一概念。

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Tumor-specific aneuploidy not detected in CD19+ B-lymphoid cells from myeloma patients in a multidimensional flow cytometric analysis.在一项多维流式细胞术分析中,骨髓瘤患者CD19 + B淋巴细胞中未检测到肿瘤特异性非整倍体。
Blood. 1996 Jul 15;88(2):622-32.
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In multiple myeloma, clonotypic B lymphocytes are detectable among CD19+ peripheral blood cells expressing CD38, CD56, and monotypic Ig light chain.在多发性骨髓瘤中,在表达CD38、CD56和单型Ig轻链的CD19⁺外周血细胞中可检测到克隆型B淋巴细胞。
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Plasma cells composing plasmacytoma have phenotypes different from those of myeloma cells.构成浆细胞瘤的浆细胞具有与骨髓瘤细胞不同的表型。
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In multiple myeloma clonotypic CD38- /CD19+ / CD27+ memory B cells recirculate through bone marrow, peripheral blood and lymph nodes.在多发性骨髓瘤中,克隆型CD38 - /CD19 + /CD27 +记忆B细胞通过骨髓、外周血和淋巴结进行再循环。
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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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Phenotypic analysis of plasma cells in bone marrow using flow cytometry in AL amyloidosis.采用流式细胞术对AL型淀粉样变性患者骨髓中的浆细胞进行表型分析。
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Individual CD34+CD38lowCD19-CD10- progenitor cells from human cord blood generate B lymphocytes and granulocytes.来自人类脐带血的单个CD34+CD38低CD19-CD10-祖细胞可生成B淋巴细胞和粒细胞。
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Purified CD34+ Lin- Thy+ stem cells do not contain clonal myeloma cells.纯化的CD34+ Lin- Thy+干细胞不包含克隆性骨髓瘤细胞。
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The incidence of DNA aneuploidy in multiple myeloma does not correlate with stage of disease.
Am J Clin Pathol. 1998 Feb;109(2):226-32. doi: 10.1093/ajcp/109.2.226.

引用本文的文献

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Stemness of B-cell progenitors in multiple myeloma bone marrow.多发性骨髓瘤骨髓中 B 细胞祖细胞的干性。
Clin Cancer Res. 2012 Nov 15;18(22):6155-68. doi: 10.1158/1078-0432.CCR-12-0531. Epub 2012 Sep 17.
2
Phenotypic detection of clonotypic B cells in multiple myeloma by specific immunoglobulin ligands reveals their rarity in multiple myeloma.通过特异性免疫球蛋白配体对多发性骨髓瘤中克隆型 B 细胞的表型检测揭示了它们在多发性骨髓瘤中的稀有性。
PLoS One. 2012;7(2):e31998. doi: 10.1371/journal.pone.0031998. Epub 2012 Feb 22.
3
Homing behaviour of the malignant cell clone in multiple myeloma.
多发性骨髓瘤中恶性细胞克隆的归巢行为。
Med Oncol. 1998 Sep;15(3):154-64. doi: 10.1007/BF02821934.