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N-myc与c-myc在小鼠浆细胞瘤发生中的功能同源性:N-myc转基因小鼠中的浆细胞瘤发展

Functional homology between N-myc and c-myc in murine plasmacytomagenesis: plasmacytoma development in N-myc transgenic mice.

作者信息

Wang Y, Sugiyama H, Axelson H, Panda C K, Babonits M, Ma A, Steinberg J M, Alt F W, Klein G, Wiener F

机构信息

Department of Tumor Biology, Karolinska Institute, Stockholm, Sweden.

出版信息

Oncogene. 1992 Jun;7(6):1241-7.

PMID:1375720
Abstract

Mouse plasmacytomas induced by pristane oil alone, or in combination with Abelson murine leukemia virus (A-MuLV), regularly carry one of three alternative chromosomal translocations that juxtapose c-myc to immunoglobulin heavy- or light-chain loci. E mu-c-myc transgenic mice develop translocation-free plasmacytomas after induction by pristane oil and/or A-MuLV [Sugiyama, H., Silva, S., Wang, Y., Weber, G., Babonits, M., Rosen, A., Wiener, F. & Klein, G. (1990). Int. J. Cancer, 46, 845-852]. In order to test whether another member of the myc family, N-myc, could play a similar role as c-myc, we treated E mu-N-myc transgenic mice with pristane and helper-free A-MuLV. Of 20 mice that received a single pristane injection followed by A-MuLV, 17 developed plasmacytomas with a mean latency period of 54 +/- 20 days. In a corresponding group that only received a single pristane injection, five out of six transgenic mice developed plasmacytomas with a mean latency period of 142 +/- 32 days. However, after three monthly injections of pristane, all 15 transgenic mice developed plasmacytomas with a mean latency period of 128 +/- 20 days. All plasmacytomas expressed the N-myc transgene, while none of them expressed either c-myc or endogenous N-myc. None of the tumors carried the usual plasmacytoma-associated translocations.

摘要

单独由 pristane 油诱导或与 Abelson 鼠白血病病毒(A-MuLV)联合诱导的小鼠浆细胞瘤,通常携带三种替代染色体易位中的一种,这些易位使 c-myc 与免疫球蛋白重链或轻链基因座并列。Eμ-c-myc 转基因小鼠在经 pristane 油和/或 A-MuLV 诱导后会发生无易位的浆细胞瘤[Sugiyama, H., Silva, S., Wang, Y., Weber, G., Babonits, M., Rosen, A., Wiener, F. & Klein, G. (1990). Int. J. Cancer, 46, 845 - 852]。为了测试 myc 家族的另一个成员 N-myc 是否能发挥与 c-myc 类似的作用,我们用 pristane 和无辅助病毒的 A-MuLV 处理 Eμ-N-myc 转基因小鼠。在 20 只接受单次 pristane 注射后再接种 A-MuLV 的小鼠中,17 只发生了浆细胞瘤,平均潜伏期为 54±20 天。在相应的仅接受单次 pristane 注射的组中,6 只转基因小鼠中有 5 只发生了浆细胞瘤,平均潜伏期为 142±32 天。然而,在每月注射三次 pristane 后,所有 15 只转基因小鼠都发生了浆细胞瘤,平均潜伏期为 128±20 天。所有浆细胞瘤都表达 N-myc 转基因,而它们均未表达 c-myc 或内源性 N-myc。没有一个肿瘤携带通常与浆细胞瘤相关的易位。

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