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白细胞介素4抑制白血病和正常人B细胞前体的体外增殖。

Interleukin 4 inhibits in vitro proliferation of leukemic and normal human B cell precursors.

作者信息

Pandrau D, Saeland S, Duvert V, Durand I, Manel A M, Zabot M T, Philippe N, Banchereau J

机构信息

Laboratory for Immunological Research, Schering-Plough, Dardilly, France.

出版信息

J Clin Invest. 1992 Nov;90(5):1697-706. doi: 10.1172/JCI116042.

Abstract

In the present study, we have investigated the effects of IL-4 on the proliferation and differentiation of leukemic and normal human B cell precursors (BCP). We have demonstrated that IL-4 significantly inhibited spontaneous [3H]thymidine ([3H]-TdR) incorporation by leukemic blasts from some B lineage acute lymphoblastic leukemia (BCP-ALL) patients (8 of 14). Furthermore, IL-4 was found to suppress the spontaneous and factor-dependent (IL-7 and IL-3) proliferation of normal BCP (CD10+ surface [s] IgM- cells) isolated from fetal bone marrow. Maximum growth inhibition of either leukemic or normal BCP was reached at low IL-4 concentrations (10 U/ml), and the effect was specifically neutralized by anti-IL-4 antibody. IL-4 was further found to induce the expression of CD20 antigen on BCP-ALL cells from a number of the cases examined (5 of 8), but in contrast to leukemic cells, IL-4 failed to induce CD20 antigen on normal BCP. Finally, IL-4 was found to induce neither the expression of cytoplasmic mu chain, nor the appearance of sIgM+ cells in cultures of normal or leukemic BCP. Our data indicate that IL-4 has the potential to inhibit cell proliferation in leukemic and normal human B lymphopoiesis but is unable to drive the transition from BCP to mature B cells.

摘要

在本研究中,我们调查了白细胞介素-4(IL-4)对白血病和正常人B细胞前体(BCP)增殖和分化的影响。我们已证明,IL-4能显著抑制一些B系急性淋巴细胞白血病(BCP-ALL)患者(14例中的8例)白血病原始细胞的自发性[3H]胸腺嘧啶核苷([3H]-TdR)掺入。此外,发现IL-4可抑制从胎儿骨髓分离的正常BCP(CD10+表面[s]IgM-细胞)的自发性增殖以及因子依赖性(IL-7和IL-3)增殖。在低IL-4浓度(10 U/ml)时,白血病或正常BCP的生长抑制达到最大值,且该效应可被抗IL-4抗体特异性中和。在一些检测的病例(8例中的5例)中,还发现IL-4可诱导BCP-ALL细胞上CD20抗原的表达,但与白血病细胞不同,IL-4未能在正常BCP上诱导CD20抗原的表达。最后,发现IL-4既不诱导正常或白血病BCP培养物中细胞质μ链的表达,也不诱导sIgM+细胞的出现。我们的数据表明,IL-4有潜力抑制白血病和正常人B淋巴细胞生成中的细胞增殖,但无法驱动BCP向成熟B细胞的转变。

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