A Cas9 Ribonucleoprotein Platform for Functional Genetic Studies of HIV-Host Interactions in Primary Human T Cells
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文摘

Cas9 RNP editing of CXCR4 and CCR5 protects primary human T cells from HIV

Arrayed delivery of RNPs confirms LEDGF and TNPO3 as HIV dependency factors

Method allows for efficient, one-step generation of double-knockout primary cells

Screen of 45 predicted integrase interactors validates new HIV host factors

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