首页> 外文期刊>Mutation Research: International Journal on Mutagenesis, Chromosome Breakage and Related Subjects >Inducible mutagenesis in TEPC 2372, a mouse plasmacytoma cell line that harbors the transgenic shuttle vector lambdaLIZ.
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Inducible mutagenesis in TEPC 2372, a mouse plasmacytoma cell line that harbors the transgenic shuttle vector lambdaLIZ.

机译:TEPC 2372中的可诱导诱变,TEPC 2372是一种小鼠浆细胞瘤细胞系,具有转基因穿梭载体lambdaLIZ。

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摘要

The plasmacytoma cell line, TEPC 2372, was derived from a malignant plasma cell tumor that developed in the peritoneal cavity of a BALB/c mouse that harbored the transgenic shuttle vector for the assessment of mutagenesis in vivo, lambdaLIZ. TEPC 2372 was found to display the typical features of a BALB/c plasmacytoma. It consisted of pleomorphic plasma cells that secreted a monoclonal immunoglobulin (IgG2b/lambda), was initially dependent on the presence of IL-6 to grow in cell culture, contained a hyperdiploid chromosome complement with a tendency to undergo tetraploidization, and harbored a constitutively active c-myc gene by virtue of a T(6;15) chromosomal translocation. TEPC 2372 was further characterized by the ability to respond to in vitro exposure with 4-NQO (4-nitroquinoline-1-oxide), an oxidative model mutagen, with a vigorous dose-dependent increase in mutagenesis that peaked at a 7.85-fold elevation of mutant rates in lambdaLIZ when compared to background mutant rates in untreated controls. Cotreatment with 4-NQO and BSO (buthionine sulfoximine), a glutathione-depleting compound that causes endogenous oxidative stress, resulted in a 9.03-fold increase in the mutant frequency in lambdaLIZ. These results demonstrated that TEPC 2372, the malignant plasma cell counterpart of the lambdaLIZ-based in vivo mutagenesis assay, may be useful as an in vitro reference point for the further elucidation of oxidative mutagenesis in lymphoid tissues.
机译:浆细胞瘤细胞系TEPC 2372源自在BALB / c小鼠腹膜腔内发育的恶性浆细胞瘤,该瘤具有转基因穿梭载体lambdaLIZ,用于评估体内诱变。发现TEPC 2372具有BALB / c浆细胞瘤的典型特征。它由分泌单克隆免疫球蛋白(IgG2b / lambda)的多形浆细胞组成,最初依赖于细胞培养中IL-6的存在而生长,包含具有二倍体化趋势的超二倍体染色体补体,并具有组成性活性c-myc基因依靠T(6; 15)染色体易位。 TEPC 2372的特征还在于能够对氧化型诱变剂4-NQO(4-硝基喹啉-1-氧化物)的体外暴露产生响应,并且诱变的剂量依赖性增加幅度很大,最高可达7.85倍。与未经处理的对照的背景突变率相比,lambdaLIZ中的突变率更高。与4-NQO和BSO(丁硫氨酸亚砜亚胺)(一种引起内源性氧化应激的谷胱甘肽消耗化合物)共同处理导致lambdaLIZ中突变频率增加9.03倍。这些结果表明,TEPC 2372是基于lambdaLIZ的体内诱变测定的恶性浆细胞对应物,可用作进一步阐明淋巴组织中氧化诱变的体外参考点。

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