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CD2+CD19+急性淋巴细胞白血病中的双表型白血病淋巴细胞前体及其在人类胎儿造血组织中的假定正常对应物。

Biphenotypic leukemic lymphocyte precursors in CD2+CD19+ acute lymphoblastic leukemia and their putative normal counterparts in human fetal hematopoietic tissues.

作者信息

Uckun F M, Muraguchi A, Ledbetter J A, Kishimoto T, O'Brien R T, Roloff J S, Gajl-Peczalska K, Provisor A, Koller B

机构信息

Department of Therapeutic Radiology-Radiation Oncology, University of Minnesota Health Sciences Center, Minneapolis 55455.

出版信息

Blood. 1989 Mar;73(4):1000-15.

PMID:2784064
Abstract

During detailed immunophenotypic analyses of marrow blasts from 336 acute lymphoblastic leukemia (ALL) patients, a very small percentage of cases reactive with B-cell-directed as well as T-cell-directed monoclonal antibodies (MoAbs) were identified. Five ALL cases were biphenotypic since they coexpressed CD2 (Tp50) and CD19 (Bp95) antigens at the single-cell level. The composite immunophenotype of these biphenotypic ALL cases was [TdT+HLA-ABC+CD2+CD3-CD10+CD13-CD14-CD16-CD19+CD20+ ++-CD21-CD33-CD34+Bgp95-C mu- slg-]. Low-molecular-weight B-cell growth factor (LMW-BCGF), recombinant interleukin-2 (rIL-2), and rIL-3 stimulated the proliferative activity of biphenotypic leukemic lymphocyte precursors without inducing differentiation. In the presence of the phorbol ester TPA, leukemic blasts from two cases differentiated along the B precursor pathway to the [CD2-CD10+CD19+CD20+C mu+slg-] pre-B cell stage. Biphenotypic ALL cases did not share a common configuration and gene rearrangement pattern of the immunoglobulin heavy chain genes or T-cell receptor (TCR) genes. Three cases had rearranged C mu genes but germline TCR genes, one case showed rearrangement of both C mu and TCR genes, and the remaining case had rearranged TCR genes but germline C mu genes. All five patients attained prompt remission after standard induction chemotherapy. Three to four years after initial diagnosis, four patients are now off chemotherapy and remain alive in their first remission. One patient relapsed at 3 years, 7 months, but promptly achieved complete remission after reinduction chemotherapy and remains in second remission off chemotherapy greater than 3 years after her reinduction therapy. With two-color immunofluorescence staining techniques and multiparameter flow cytometric analyses, we identified a small population of CD2+CD19+ lymphoid cells in fetal livers (FLs) and fetal bone marrows (FBMs), which may represent the putative normal counterparts of biphenotypic ALL blasts. A CD2+CD19+ normal biphenotypic lymphoid precursor cell line, designated FL 8.2 CD2+, was established from an FL of 8-weeks of gestational age by Epstein-Barr virus (EBV)-induced blastoid transformation. The composite immunophenotype of FL 8.2 CD2+ cell line was [TdT+HLA-ABC+HLA-DR+ CD2+CD5-CD7-CD10+/-CD13-CD19+CD20-CD21+ CD22+CD33-CD34+/-Bgp95-CDw40+C mu-slgD-slgM-]. FL 8.2 CD2+ cells showed germline patterns of immunoglobulin heavy-chain joining region, heavy-chain constant region, kappa light-chain constant region genes, and TCR beta-chain genes. Cross-linking of CD2 as well as CD19 antigens on FL 8.2 CD2+ cells caused an increase of intracellular ionized calcium.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

在对336例急性淋巴细胞白血病(ALL)患者的骨髓原始细胞进行详细免疫表型分析过程中,发现了一小部分病例可同时与B细胞定向及T细胞定向单克隆抗体(MoAbs)发生反应。5例ALL病例为双表型,因为它们在单细胞水平上共表达CD2(Tp50)和CD19(Bp95)抗原。这些双表型ALL病例的复合免疫表型为[末端脱氧核苷酸转移酶(TdT)阳性+人白细胞抗原ABC(HLA-ABC)阳性+CD2阳性+CD3阴性+CD10阳性+CD13阴性+CD14阴性+CD16阴性+CD19阳性+CD20阳性++-CD21阴性+CD33阴性+CD34阳性+Bgp95阴性-Cμ阴性-表面免疫球蛋白(slg)阴性]。低分子量B细胞生长因子(LMW-BCGF)、重组白细胞介素-2(rIL-2)和rIL-3可刺激双表型白血病淋巴细胞前体的增殖活性,而不诱导分化。在佛波酯TPA存在的情况下,两例患者的白血病原始细胞沿B前体途径分化至[CD2阴性+CD10阳性+CD19阳性+CD20阳性+Cμ阳性+slg阴性]前B细胞阶段。双表型ALL病例在免疫球蛋白重链基因或T细胞受体(TCR)基因方面没有共同的构型和基因重排模式。3例患者的Cμ基因发生重排,但TCR基因为种系基因;1例患者的Cμ和TCR基因均发生重排;其余1例患者的TCR基因发生重排,但Cμ基因为种系基因。所有5例患者在标准诱导化疗后均迅速缓解。初次诊断后3至4年,4例患者现已停止化疗,仍处于首次缓解期存活。1例患者在3年7个月时复发,但再次诱导化疗后迅速达到完全缓解,再次诱导治疗后3年多来一直处于第二次缓解期且未接受化疗。通过双色免疫荧光染色技术和多参数流式细胞术分析,我们在胎儿肝脏(FLs)和胎儿骨髓(FBMs)中鉴定出一小群CD2阳性+CD1阴性9淋巴细胞,它们可能代表双表型ALL原始细胞的假定正常对应物。从妊娠8周的FL中通过爱泼斯坦-巴尔病毒(EBV)诱导的母细胞样转化建立了一个CD2阳性+CD19阳性正常双表型淋巴细胞前体细胞系,命名为FL 8.2 CD2阳性。FL 8.2 CD2阳性细胞系的复合免疫表型为[TdT阳性+HLA-ABC阳性+HLA-DR阳性+CD2阳性+CD5阴性+CD7阴性+CD10阳性/-CD13阴性+CD19阳性+CD20阴性+CD21阳性+CD22阳性+CD33阴性+CD34阳性/-Bgp95阴性+CDw40阳性+Cμ阴性-slgD阴性-slgM阴性]。FL 8.2 CD2阳性细胞在免疫球蛋白重链连接区、重链恒定区、κ轻链恒定区基因和TCRβ链基因方面显示种系模式。FL 8.2 CD2阳性细胞上CD2以及CD19抗原的交联导致细胞内游离钙增加。(摘要截短于400字)

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