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Effective Targeting of TAG72 Peritoneal Ovarian Tumors via Regional Delivery of CAR-Engineered T Cells.

Front Immunol. 2018; 
MuradJohn P,KozlowskaAnna K,LeeHee Jun,RamamurthyMaya,ChangWen-Chung,YazakiPaul,ColcherDavid,ShivelyJohn,CristeaMihaela,FormanStephen J,PricemanSa
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Recombinant Proteins … BioLegend, Clone: 30-F11), CD45 (BD Biosciences, Clone: 2D1), CD69 (BD Biosciences, Clone: L78), CD137 (BD Biosciences, Clone: 4B4-1), MUC1 (BioLegend, Clone 16A), MUC16 (Abcam, Clone X75 or EPSISR23), biotinylated Protein-L (GenScript USA) (25), TAG72 … Get A Quote

摘要

Impressive clinical efficacy of chimeric antigen receptor (CAR)-engineered T cell therapy for hematological malignancies have prompted significant efforts in achieving similar responses in solid tumors. The lack of truly restricted and uniform expression of tumor-associated antigens, as well as limited T cell persistence and/or tumor trafficking pose major challenges for successful translation of CAR T cell therapy in solid tumors. Recent studies have demonstrated that aberrantly glycosylated cell surface proteins on tumor cells are amenable CAR targets. Tumor-associated glycoprotein 72 (TAG72) antigen is the sialyl-Tn found on multiple O-glycoproteins expressed at high levels on the surface of several cancer... More

关键词

STn,TAG72,adoptive cellular immunotherapy,chimeric antigen receptor,ovarian cancer,regional intraperitoneal delivery,sialyl-Tn,tumor-associated glycoprot
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