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体内T细胞增殖机制:淋巴再生过程中IL-2受体表达及c-myc和c-myb癌基因激活的分析

Mechanism of T cell proliferation in vivo: analysis of IL-2 receptor expression and activation of c-myc and c-myb oncogenes during lymphatic regeneration.

作者信息

Sihvola M, Sistonen L, Alitalo K, Hurme M

机构信息

Department of Bacteriology, University of Helsinki, Finland.

出版信息

Biochem Biophys Res Commun. 1989 Apr 14;160(1):181-8. doi: 10.1016/0006-291x(89)91638-0.

DOI:10.1016/0006-291x(89)91638-0
PMID:2496686
Abstract

The mechanism of T cell proliferation was studied using in vivo lymphatic regeneration as the model. Lymphatic regeneration was induced by injecting a sublethal dose (300 mg/kg) of cyclophosphamide (Cy) into mice. Majority of the regenerating splenic T cells were found to be in the cell cycle, nearly 30% being found in S/G2+M phases resembling the ratio obtained for mitogen activated T cells in vitro. Expression of interleukin-2 receptor (IL-2R) was defined by the monoclonal anti-IL-2R antibody, AMT-13. Only 1-3% of regenerating T cells were IL-2R positive (while about 30% of the in vitro activated T cells were IL-2R positive). Accordingly, these cells did not respond to IL-2 in vitro. However, when the freshly isolated regenerating T cells were cultured in the presence of Con A or PMA + ionophore A 23187, IL-2R was readily induced. The regenerating T cells were further analyzed for the expression of the cellular oncogenes c-myc and c-myb. These cells expressed about three times more c-myb mRNA than Con A-stimulated T cells and the levels were comparable to those seen in thymocytes. By contrast, the amount of c-myc mRNA was similar in the regenerating T cells and in Con A-activated T cells, but weak or barely detectable in splenocytes and thymocytes. Taken together, our results imply that the vigorous T cell proliferation during cyclophosphamide-induced lymphatic regeneration is independent of the IL-2/IL-2R hormone system, like T-cell precursor proliferation in the thymus, and is characterized by both high c-myb expression typical for thymocytes and high c-myc expression typical for in vitro proliferation-activated T cells.

摘要

以体内淋巴再生为模型研究了T细胞增殖机制。通过向小鼠注射亚致死剂量(300mg/kg)的环磷酰胺(Cy)诱导淋巴再生。发现大多数再生脾T细胞处于细胞周期中,近30%处于S/G2+M期,这一比例与体外有丝分裂原激活的T细胞所获得的比例相似。用单克隆抗IL-2R抗体AMT-13确定白细胞介素-2受体(IL-2R)的表达。只有1%-3%的再生T细胞为IL-2R阳性(而约30%的体外激活T细胞为IL-2R阳性)。因此,这些细胞在体外对IL-2无反应。然而,当新鲜分离的再生T细胞在Con A或PMA+离子载体A 23187存在下培养时,IL-2R很容易被诱导。对再生T细胞进一步分析细胞癌基因c-myc和c-myb的表达。这些细胞表达的c-myb mRNA比Con A刺激的T细胞多约三倍,其水平与胸腺细胞中的水平相当。相比之下,再生T细胞和Con A激活的T细胞中c-myc mRNA的量相似,但在脾细胞和胸腺细胞中较弱或几乎检测不到。综上所述,我们的结果表明,环磷酰胺诱导的淋巴再生过程中T细胞的旺盛增殖独立于IL-2/IL-2R激素系统,就像胸腺中T细胞前体的增殖一样,其特征是具有胸腺细胞典型的高c-myb表达和体外增殖激活的T细胞典型的高c-myc表达。

相似文献

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Mechanism of T cell proliferation in vivo: analysis of IL-2 receptor expression and activation of c-myc and c-myb oncogenes during lymphatic regeneration.体内T细胞增殖机制:淋巴再生过程中IL-2受体表达及c-myc和c-myb癌基因激活的分析
Biochem Biophys Res Commun. 1989 Apr 14;160(1):181-8. doi: 10.1016/0006-291x(89)91638-0.
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Regulation of T lymphocyte proliferation. Interleukin 2-mediated induction of c-myb gene expression is dependent on T lymphocyte activation state.T淋巴细胞增殖的调节。白细胞介素2介导的c-myb基因表达的诱导依赖于T淋巴细胞的激活状态。
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Requirements for the simultaneous presence of phorbol esters and calcium ionophores in the expression of human T lymphocyte proliferation-related genes.人T淋巴细胞增殖相关基因表达中佛波酯和钙离子载体同时存在的要求。
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Distinct signals are required for proliferation and lymphokine gene expression in murine T cell clones.在小鼠T细胞克隆中,增殖和淋巴因子基因表达需要不同的信号。
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c-myc gene expression and activation of human thymocytes.
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Early precursor thymocytes can produce interleukin 2 upon stimulation with calcium ionophore and phorbol ester.早期前体胸腺细胞在用钙离子载体和佛波酯刺激后可产生白细胞介素2。
Proc Natl Acad Sci U S A. 1986 Mar;83(6):1862-6. doi: 10.1073/pnas.83.6.1862.

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