首页> 外文期刊>Toxicologic pathology >Spontaneous and irradiation-induced tumor susceptibility in BRCA2 germline mutant mice and cooperative effects with a p53 germline mutation.
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Spontaneous and irradiation-induced tumor susceptibility in BRCA2 germline mutant mice and cooperative effects with a p53 germline mutation.

机译:BRCA2种系突变小鼠的自发和辐射诱导的肿瘤敏感性以及与p53种系突变的协同作用。

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摘要

Mutations in both p53 and BRCA2 are commonly seen together in human tumors suggesting that the loss of both genes enhances tumor development. To elucidate this interaction in an animal model, mice lacking the carboxy terminal domain of Brca2 were crossed with p53 heterozygous mice. Females from this intercross were then irradiated with an acute dose of 5 Gy ionizing radiation at 5 weeks of age and compared to nonirradiated controls. We found decreased survival and timing of tumor onsets, and significantly higher overall tumor incidences and prevalence of particular tumors, including stomach tumors and squamous cell carcinomas, associated with the homozygous loss of Brca2, independent of p53 status. The addition of a p53 mutation had a further impact on overall survival, incidence of osteosarcomas and stomach tumors, and tumor latency. The spectrum of tumors observed for this Brca2 germline mouse model suggest that it faithfully recapitulates some human disease phenotypes associated with BRCA2 loss. In addition, these findings include extensive in vivo data demonstrating that germline Brca2 and p53 mutations cooperatively affect animal survivals, tumor susceptibilities, and tumor onsets.
机译:p53和BRCA2的突变通常在人类肿瘤中同时出现,这表明这两个基因的缺失会促进肿瘤的发展。为了在动物模型中阐明这种相互作用,将缺少Brca2羧基末端结构域的小鼠与p53杂合小鼠杂交。然后,在5周龄时,对来自这种杂交的雌性进行5 Gy电离辐射的急性剂量辐照,并与未辐照的对照进行比较。我们发现,肿瘤发作的生存时间和时机降低,并且总体肿瘤发生率和特定肿瘤(包括胃肿瘤和鳞状细胞癌)的患病率显着升高,与纯合的Brca2丢失相关,而与p53状态无关。 p53突变的增加对总体存活率,骨肉瘤和胃肿瘤的发生率以及肿瘤潜伏期有进一步的影响。此Brca2种系小鼠模型观察到的肿瘤光谱表明,它忠实地概括了一些与BRCA2丢失相关的人类疾病表型。此外,这些发现包括广泛的体内数据,证明种系Brca2和p53突变可协同影响动物的存活率,肿瘤易感性和肿瘤发作。

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