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To broadly enable the application of Cas9 in vivo, we established a Cre-dependent Cas9 knockin mouse.
We demonstrated in vivo as well as ex vivo genome editing using adeno-associated virus (AAV)-, lentivirus-, or particle-mediated delivery of guide RNA in neurons, immune cells, and endothelial cells.
Using these mice, we simultaneously modeled the dynamics of KRAS, p53, and LKB1, the top three significantly mutated genes in lung adenocarcinoma.
Delivery of a single AAV vector in the lung generated loss-of-function mutations in p53 and Lkb1, as well as homology-directed repair-mediated KrasG12D mutations, leading to macroscopic tumors of adenocarcinoma pathology.
Together, these results suggest that Cas9 mice empower a wide range of biological and disease modeling applications.以上资料由西亚试剂:http://www.xiyashiji.com/提供