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Generation of a highly efficient and tissue-specific tryptophan hydroxylase 1 knockout mouse model

机译:高效和组织特异性色氨酸羟化酶1基因敲除小鼠模型的生成。

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Recent studies on tissue-autonomous serotonin (5-hydroxytryptamine [5-HT]) function have identified new roles for 5-HT in peripheral organs. Most of these studies were performed by crossing mice carrying the Tph1tm1Kry allele with tissue specific Cre mice. In the present study, we found that 5-HT production was not completely abolished in Tph1tm1Kry KO mice. The residual 5-HT production in Tph1tm1Kry KO mice is attributed to the expression of a truncated form of TPH1 containing the catalytic domain. Hence, in an effort to obtain mice with a Tph1 null phenotype, we generated mice harboring a new Tph1 floxed allele, Tph1tm1c, targeting exons 5 and 6 which encode the catalytic domain of TPH1. By crossing the new Tph1 floxed mice with villin-Cre or insulin-Cre mice, we observed near-complete ablation of 5-HT production in the intestine and β cells. In conclusion, this improved Tph1 floxed mouse model will serve as useful and accurate tool for analyzing peripheral 5-HT system.
机译:组织自主性5-羟色胺(5-羟色胺[5-HT])功能的最新研究发现了5-HT在周围器官中的新作用。这些研究大多数是通过将携带Tph1tm1Kry等位基因的小鼠与组织特异性Cre小鼠杂交而进行的。在本研究中,我们发现Tph1tm1Kry KO小鼠中5-HT的产生没有完全消除。 Tph1tm1Kry KO小鼠体内5-HT残留的产生是由于含有催化结构域的TPH1的截短形式的表达。因此,为了获得具有Tph1无效表型的小鼠,我们生成了具有新的Tph1固定等位基因Tph1tm1c的小鼠,它们靶向编码TPH1催化域的外显子5和6。通过将新的Tph1固着小鼠与villin-Cre或胰岛素-Cre小鼠杂交,我们观察到肠和β细胞中5-HT产生的消融几乎完全。总之,这种改良的Tph1小鼠模型将成为分析外围5-HT系统的有用且准确的工具。

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