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Mutations in the Epstein-Barr virus latent membrane protein-1 (BNLF-1) gene in spontaneous lymphoblastoid cell lines: effect on in vitro transformation associated parameters and tumorigenicity in SCID and nude mice

机译:自发性淋巴母细胞细胞系中爱泼斯坦-巴尔病毒潜伏膜蛋白-1(BNLF-1)基因的突变:对SCID和裸鼠体外转化相关参数和致瘤性的影响

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摘要

Aims—(1) To study the frequency of putative malignancy associated point mutations and a 30 base pair (bp) deletion in exon 3 of the C-terminus of the Epstein-Barr virus (EBV) encoded latent membrane protein (LMP)-1 (BNLF-1) gene in wild type EBV strains. (2) To assess the influence of these mutations on the tumorigenicity of lymphoblastoid cell lines (LCL).Methods—Eight spontaneous EBV (wild type) infected LCL were established from seven subjects. Deletions and single base mutations in the C-terminus of the BNLF-1 gene were demonstrated using bi-directional solid phase dideoxy sequencing following PCR amplification of viral DNA from the LCL. Tumorigenicity of the LCL was assessed in SCID and nude mice. Serum dependent growth and ability to form colonies in soft agarose were assessed for representative LCL.Results—All LCL showed sequence differences compared with the prototypic EBV strain B95-8. The 30 bp deletion could be detected in three of eight LCL and a 69 bp deletion (including the 30 bp deletion) was identified in an additional LCL. A range of single base mutations (including those described previously in association with EBV related neoplasias) was also seen in some of the LCL. In transformation studies, the genetic variations did not seem to influence the in vitro behaviour of the LCL. In the tumorigenicity studies, the presence of the 30 bp deletion had no influence on the behaviour of the LCL which were, as expected, tumorigenic in SCID mice but not in nude mice. In contrast, the LCL carrying the 69 bp deletion was tumorigenic in both SCID and nude mice.Conclusions—Genetic changes described previously in the C-terminus of the LMP-1 gene in various malignancy derived EBV strains are also present frequently in wild type viruses and do not simply define tumour specific EBV strains. Changes within this region may, however, still be important for the tumorigenicity of LMP-1 and thus play a role in EBV oncogenesis.
机译:目的—(1)研究Epstein-Barr病毒(EBV)编码的潜伏膜蛋白(LMP)-1的C末端外显子3的假定的恶性肿瘤相关点突变的频率和30个碱基对(bp)的缺失野生型EBV株中的(BNLF-1)基因。 (2)评估这些突变对淋巴母细胞样细胞系(LCL)致瘤性的影响。方法—从7名受试者中建立了8个自发感染EBV(野生型)的LCL。 PCR扩增LCL病毒DNA后,使用双向固相双脱氧测序法证实了BNLF-1基因C末端的缺失和单碱基突变。在SCID和裸鼠中评估了LCL的致瘤性。对代表性的LCL评估了血清依赖性生长和在软琼脂糖中形成菌落的能力。结果-与原型EBV菌株B95-8相比,所有LCL均显示出序列差异。可以在八个LCL中的三个中检测到30 bp的缺失,在另一个LCL中鉴定出一个69 bp的缺失(包括30 bp的缺失)。在某些LCL中也发现了一系列单碱基突变(包括先前与EBV相关瘤形成相关的描述)。在转化研究中,遗传变异似乎并未影响LCL的体外行为。在致瘤性研究中,30 bp缺失的存在对LCL的行为没有影响,正如预期的那样,LCL的行为在SCID小鼠中是致瘤的,而在裸鼠中则没有。相比之下,携带69 bp缺失的LCL在SCID和裸鼠中均具有致瘤性。结论-先前在各种恶性肿瘤衍生EBV株中LMP-1基因C端描述的遗传变化也经常出现在野生型病毒中并且不能简单地定义肿瘤特异性EBV株。然而,该区域内的变化对于LMP-1的致瘤性可能仍然很重要,因此在EBV肿瘤发生中起作用。

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