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Engineering HIV-resistant, anti-HIV chimeric antigen receptor T cells.

Mol Ther.. 2017; 
Malika Hale, Taylor Mesojednik, Guillermo S. Romano Ibarra, Jaya Sahni, Alison, Bernard, Karen Sommer, Andrew M. Scharenberg, David J. Rawlings, Thor A. Wagner. Center for Global Infectious Disease Research, Seattle Children's Research Institute, 1900 Ninth Avenue, Seattle, WA 98101.
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摘要

The treatment or cure of HIV infection by cell and gene therapy has been a goal for decades. Recent advances in both gene editing and chimeric antigen receptor (CAR) technology have created new therapeutic possibilities for a variety of diseases. Broadly neutralizing monoclonal antibodies (bNAb) with specificity for the HIV envelope glycoprotein provide a promising means of targeting HIV-infected cells. Here we show that primary human T cells engineered to express anti-HIV CARs based on bNAbs (HIVCAR) show specific activation and killing of HIV-infected versus uninfected cells in the absence of HIV replication. We also show that homology-directed recombination of the HIVCAR gene expression cassette into the CCR... More

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