首页> 美国卫生研究院文献>Molecular and Cellular Biology >Targeted Genomic Disruption of H-ras and N-ras Individually or in Combination Reveals the Dispensability of Both Loci for Mouse Growth and Development
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Targeted Genomic Disruption of H-ras and N-ras Individually or in Combination Reveals the Dispensability of Both Loci for Mouse Growth and Development

机译:H-ras和N-ras的靶向基因组破坏单独或组合揭示了两个基因座对小鼠生长和发育的可分配性

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摘要

Mammalian cells harbor three highly homologous and widely expressed members of the ras family (H-ras, N-ras, and K-ras), but it remains unclear whether they play specific or overlapping cellular roles. To gain insight into such functional roles, here we generated and analyzed H-ras null mutant mice, which were then also bred with N-ras knockout animals to ascertain the viability and properties of potential double null mutations in both loci. Mating among heterozygous H-ras+/− mice produced H-ras−/− offspring with a normal Mendelian pattern of inheritance, indicating that the loss of H-ras did not interfere with embryonic and fetal viability in the uterus. Homozygous mutant H-ras−/− mice reached sexual maturity at the same age as their littermates, and both males and females were fertile. Characterization of lymphocyte subsets in the spleen and thymus showed no significant differences between wild-type and H-ras−/− mice. Analysis of neuronal markers in the brains of knockout and wild-type H-ras mice showed that disruption of this locus did not impair or alter neuronal development. Breeding between our H-ras mutant animals and previously available N-ras null mutants gave rise to viable double knockout (H-ras−/−/N-ras−/−) offspring expressing only K-ras genes which grew normally, were fertile, and did not show any obvious phenotype. Interestingly, however, lower-than-expected numbers of adult, double knockout animals were consistently obtained in Mendelian crosses between heterozygous N-ras/H-ras mice. Our results indicate that, as for N-ras, H-ras gene function is dispensable for normal mouse development, growth, fertility, and neuronal development. Additionally, of the three ras genes, K-ras appears to be not only essential but also sufficient for normal mouse development.
机译:哺乳动物细胞具有ras家族的三个高度同源且表达广泛的成员(H-ras,N-ras和K-ras),但尚不清楚它们是否发挥特定或重叠的细胞作用。为了深入了解这些功能角色,我们在这里生成并分析了H-ras null突变小鼠,然后将它们与N-ras基因敲除动物进行繁殖,以确定两个基因座中潜在的double null突变的活力和特性。在杂合的H-ras +/- 小鼠中交配产生了具有正常孟德尔遗传模式的H-ras -/-后代,这表明H-ras的丧失并没有干扰子宫中的胚胎和胎儿活力。纯合突变型H-ras -/-小鼠在与同窝同龄的同龄动物中达到了性成熟,雄性和雌性都可以生育。野生型和H-ras -/-小鼠的脾脏和胸腺中的淋巴细胞亚群的表征没有显着差异。对基因敲除和野生型H-ras小鼠大脑中神经元标记物的分析表明,破坏该基因座不会损害或改变神经元发育。我们的H-ras突变动物与先前可用的N-ras null突变体之间的育种产生了可行的双敲除(H-ras -/- / N-ras -/- )仅表达正常生长的K- ras 基因的后代,可育且没有显示任何明显的表型。有趣的是,在杂合的N- ras / H- ras 小鼠之间的孟德尔杂交中始终获得低于预期数量的成年双基因敲除动物。我们的结果表明,就N- ras 而言,H- ras 基因功能对于正常的小鼠发育,生长,繁殖力和神经元发育是必不可少的。此外,在三个 ras 基因中,K- ras 似乎不仅对正常小鼠发育必不可少,而且足够。

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