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细胞毒性疗法诱导的骨髓再生障碍恢复过程中的T细胞表型特征及集落形成

T-cell phenotypic profile and colony formation during recovery from cytotoxic therapy-induced marrow aplasia.

作者信息

Ashkenazi Y J, Barth K C, Elfenbein G J

出版信息

Cancer Res. 1985 Dec;45(12 Pt 1):6513-8.

PMID:3933827
Abstract

Lymphocytes which appeared in the peripheral blood early (approximately 4 weeks) after complete bone marrow aplasia were studied in two groups of patients. Twenty-two allogeneic bone marrow transplant recipients and 12 acute nonlymphocytic leukemia patients (entering remission) were compared to 70 healthy control subjects studied during the same time interval. Studies performed included phenotyping T-cells using monoclonal antibodies and T-cell colony formation in response to phytohemagglutinin. The phenotypic profile for the two patient groups differed from each other and from that of the healthy controls. The total number of circulating cells reactive with OKT4 were significantly depressed in marrow graft recipients while only mildly, but significantly, depressed in leukemic patients. The number of circulating cells reactive with OKT8 were depressed in leukemic patients but were essentially normal in marrow graft recipients. The number of circulating cells reactive with OKla1 and OKT10 were significantly elevated in marrow graft recipients while significantly depressed in leukemic patients. The T4:T8 ratio was significantly depressed for marrow transplant recipients and significantly elevated for leukemic patients. T-cell colony formation in agarose without and with added interleukin-2 was decreased for both groups, more so for marrow graft recipients who virtually lacked the ability to make colonies without exogenous interleukin 2. These phenotypic and functional data suggest that T-cell reconstitution after bone marrow aplasia and profound lymphopenia takes quite different pathways for leukemic patients recovering from remission induction therapy and for recipients of bone marrow transplants. We were unable to correlate T-cell functional response in T-cell colony formation with the phenotypic profile of peripheral blood T-cells.

摘要

对两组患者在完全性骨髓再生障碍后早期(约4周)出现在外周血中的淋巴细胞进行了研究。将22例同种异体骨髓移植受者和12例急性非淋巴细胞白血病患者(进入缓解期)与同期研究的70名健康对照者进行比较。进行的研究包括使用单克隆抗体对T细胞进行表型分析以及对植物血凝素的T细胞集落形成。两组患者的表型特征彼此不同,也与健康对照者不同。与OKT4反应的循环细胞总数在骨髓移植受者中显著降低,而在白血病患者中仅轻度但显著降低。与OKT8反应的循环细胞数量在白血病患者中降低,但在骨髓移植受者中基本正常。与OKla1和OKT10反应的循环细胞数量在骨髓移植受者中显著升高,而在白血病患者中显著降低。骨髓移植受者的T4:T8比值显著降低,白血病患者的该比值显著升高。两组在无白细胞介素-2和添加白细胞介素-2的情况下在琼脂糖中的T细胞集落形成均减少,骨髓移植受者减少得更多,他们在没有外源性白细胞介素-2时几乎没有形成集落的能力。这些表型和功能数据表明,在骨髓再生障碍和严重淋巴细胞减少后,白血病患者从缓解诱导治疗中恢复和骨髓移植受者的T细胞重建途径截然不同。我们无法将T细胞集落形成中的T细胞功能反应与外周血T细胞的表型特征相关联。

相似文献

1
T-cell phenotypic profile and colony formation during recovery from cytotoxic therapy-induced marrow aplasia.细胞毒性疗法诱导的骨髓再生障碍恢复过程中的T细胞表型特征及集落形成
Cancer Res. 1985 Dec;45(12 Pt 1):6513-8.
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Abrogation of bone marrow allograft resistance in mice by increased total body irradiation correlates with eradication of host clonable T cells and alloreactive cytotoxic precursors.通过增加全身照射消除小鼠骨髓同种异体移植抗性与宿主可克隆T细胞和同种异体反应性细胞毒性前体的根除相关。
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Long-lasting decrease of marrow and circulating long-term culture initiating cells after allogeneic bone marrow transplant.异基因骨髓移植后骨髓及循环长期培养起始细胞的持久减少。
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Recombinant human interleukin-2 restores in vitro T-cell colony formation by peripheral blood mononuclear cells after autologous bone marrow transplantation.重组人白细胞介素-2可恢复自体骨髓移植后外周血单个核细胞的体外T细胞集落形成。
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The influence of T lymphocyte subsets and humoral factors on colony formation by human bone marrow and blood megakaryocyte progenitor cells in vitro.T淋巴细胞亚群和体液因子对人骨髓及血液巨核细胞祖细胞体外集落形成的影响。
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引用本文的文献

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Blood. 2011 Jan 13;117(2):608-17. doi: 10.1182/blood-2010-04-277939. Epub 2010 Oct 8.
2
Pathology of the thymus after allogeneic bone marrow transplantation in man. A histologic immunohistochemical study of 36 patients.人类同种异体骨髓移植后胸腺的病理学。对36例患者的组织学免疫组化研究。
Am J Pathol. 1987 Nov;129(2):242-56.