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Pim1 和 Myc 可使鼠类前体 B 淋巴细胞可逆地转化,但不能使成熟 B 淋巴细胞转化。

Pim1 and Myc reversibly transform murine precursor B lymphocytes but not mature B lymphocytes.

机构信息

Department of Lymphocyte Development, MPI for Infection Biology, Berlin, Germany.

出版信息

Eur J Immunol. 2012 Feb;42(2):522-32. doi: 10.1002/eji.201141987. Epub 2011 Dec 19.

Abstract

The proto-oncogenes Myc and Pim1, which are deregulated in many types of cancers, are known to cooperate in B lymphoma development. Here we show that overexpression of retrovirally transduced, doxycycline-inducible Myc alone in IL-7-deprived, growth-arrested pre-B cells enhanced cell cycle entry without impairing apoptosis. Overexpression of Pim1 decreased apoptosis, but had no effect on cell cycle entry. Co-expression of Pim1 and Myc inhibited apoptosis and led to IL-7-independent proliferation of the transduced pre-B cells in vitro, while blocking their differentiation to IgM(+) immature cells. Transplantation of Pim1/Myc overexpressing pre-BI cells into B-cell-deficient mice expanded the pre-B-cell compartments up to 100-fold within 4-8 weeks. Transformation remained dependent on the expression of both oncogenes, as removal of doxycycline in vitro and in vivo terminated proliferation and induced differentiation to IgM(+) B cells. In contrast, Pim1/Myc-transduced mature B cells that developed from the oncogene-transduced pre-BI cells in the absence of oncogene overexpression in vivo were not capable of long-term proliferation after induction of Pim and Myc overexpression, neither in vivo nor in vitro, neither with nor without stimulation by polyclonal activators.

摘要

原癌基因 Myc 和 Pim1 在许多类型的癌症中都被发现存在失调,它们在 B 淋巴瘤的发展中被证实具有合作关系。在这里,我们发现,在缺乏白细胞介素-7(IL-7)且生长停滞的前 B 细胞中,过表达经逆转录病毒转导的、可被强力霉素诱导的 Myc,可增强细胞周期进入,而不损害细胞凋亡。Pim1 的过表达降低了细胞凋亡,但对细胞周期进入没有影响。Pim1 和 Myc 的共表达抑制了细胞凋亡,并导致转导的前 B 细胞在体外进行 IL-7 非依赖性增殖,同时阻止其分化为 IgM(+)幼稚细胞。将过表达 Pim1/Myc 的前 BI 细胞移植到 B 细胞缺陷小鼠中,可在 4-8 周内使前 B 细胞群扩大 100 倍。转化仍然依赖于两个癌基因的表达,因为体外和体内去除强力霉素可终止增殖,并诱导分化为 IgM(+) B 细胞。相比之下,在体内缺乏癌基因过表达的情况下,由 Pim1/Myc 转导的前 BI 细胞发育而来的成熟 B 细胞,在诱导 Pim 和 Myc 过表达后,无论是在体内还是体外,无论是有还是没有多克隆激活剂的刺激,都不能进行长期增殖。

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