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Correction of PTEN mutations in glioblastoma cell lines via AAV-mediated gene editing.

PLoS One.. 2017-05; 
Hill VK,Kim JS,James CD,Waldman T.
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Gene Synthesis ... contains wild-type genomic sequence corresponding to intron 1, exon 2, and the first 200 nucleotides of intron 2. The right homology arm (RHA; ~1 kb) contains wild-type genomic sequence corresponding to intron 2. Homology arms were synthesized by Genscript and cloned ... Get A Quote

摘要

PTEN is among the most commonly mutated tumor suppressor genes in human cancer. However, studying the role of PTEN in the pathogenesis of cancer has been limited, in part, by the paucity of human cell-based isogenic systems that faithfully model PTEN loss. In an effort to remedy this problem, gene editing was used to correct an endogenous mutant allele of PTEN in two human glioblastoma multiforme (GBM) cell lines- 42MGBA and T98G. PTEN correction resulted in reduced cellular proliferation that was Akt-dependent in 42MGBA cells and Akt-independent in T98G cells. This is the first report of human cancer cell lines in which mutant PTEN has been corrected by gene editing. The isogenic sets of gene edited cell lines... More

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