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v-myc 转化小鼠单核细胞后的肿瘤进展:获得永生化和致瘤性。

Tumor progression following transformation of murine monocytes by v-myc: acquisition of immortalization and tumorigenicity.

作者信息

Stapleton P, Takayama Y, Hartshorn A, Kalaizis A, Rowe P B, Symonds G

机构信息

Leukaemia Research and Viral Pathology Unit, Children's Medical Research Foundation, Camperdown, Sydney, NSW, Australia.

出版信息

Oncogene. 1991 May;6(5):807-17.

PMID:1711191
Abstract

Monocyte transformation by the v-myc oncogene has been used to study myelomonocytic tumor progression in vitro. Murine monocytes transformed by a recombinant retrovirus containing MC29 v-myc were found to exhibit a proliferative burst to day 28-40 post-infection. There-after growth slowed and cell number remained relatively static to day 80-90 post-infection. During both the proliferative and quiescent periods, the cells were dependent on the myelomonocytic growth factor CSF-1 for growth and viability. Analysis of this transformation revealed that the initial transformants were polyclonal, non-immortal, and non-tumorigenic in syngeneic mice. At day 80-90 post infection, a fresh round of cellular proliferation occurred and, in contrast to the initial burst, growth was sustained allowing the establishment of cell lines. These lines were found to be monoclonal, immortal, growth factor independent and, in certain cases, tumorigenic in syngeneic mice. Associated with the establishment of growth factor independent cell lines was the constitutive synthesis of the myelomonocytic growth factor, CSF-1. Proto-oncogene screening of the initial transformants and the cell lines also revealed the expression of c-raf and the CSF-1 receptor, c-fms. Our results indicate that, following transformation by v-myc, monocytes can progress in vitro to become growth factor independent and immortal and that both monocyte transformation and immortalization can be dissociated from tumorigenicity.

摘要

v-myc癌基因介导的单核细胞转化已被用于体外研究骨髓单核细胞肿瘤的进展。通过含有MC29 v-myc的重组逆转录病毒转化的小鼠单核细胞在感染后第28 - 40天表现出增殖爆发。此后生长减缓,细胞数量在感染后第80 - 90天保持相对稳定。在增殖期和静止期,细胞的生长和存活均依赖于骨髓单核细胞生长因子CSF-1。对这种转化的分析表明,初始转化体是多克隆的,在同基因小鼠中不具有永生性和致瘤性。在感染后第80 - 90天,新一轮细胞增殖发生,与初始爆发不同的是,生长得以持续,从而建立了细胞系。这些细胞系被发现是单克隆的、永生的、不依赖生长因子的,并且在某些情况下,在同基因小鼠中具有致瘤性。与不依赖生长因子的细胞系建立相关的是骨髓单核细胞生长因子CSF-1的组成型合成。对初始转化体和细胞系的原癌基因筛选还揭示了c-raf和CSF-1受体c-fms的表达。我们的结果表明,v-myc转化后,单核细胞在体外可进展为不依赖生长因子且具有永生性,并且单核细胞转化和永生化都可与致瘤性分离。

相似文献

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Tumor progression following transformation of murine monocytes by v-myc: acquisition of immortalization and tumorigenicity.v-myc 转化小鼠单核细胞后的肿瘤进展:获得永生化和致瘤性。
Oncogene. 1991 May;6(5):807-17.
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