Development of a Clinically Relevant Reporter for Chimeric Antigen Receptor T-cell Expansion, Trafficking, and Toxicity

开发用于嵌合抗原受体T细胞扩增、迁移和毒性的临床相关报告基因

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作者:Reona Sakemura ,Aditya Bansal ,Elizabeth L Siegler ,Mehrdad Hefazi ,Nan Yang ,Roman H Khadka ,Alysha N Newsom ,Michael J Hansen ,Michelle J Cox ,Claudia Manriquez Roman ,Kendall J Schick ,Ismail Can ,Erin E Tapper ,Wendy K Nevala ,Mohamad M Adada ,Evandro D Bezerra ,Lionel Aurelien Kankeu Fonkoua ,Paulina Horvei ,Michael W Ruff ,Sameer A Parikh ,Mukesh K Pandey ,Timothy R DeGrado ,Lukkana Suksanpaisan ,Neil E Kay ,Kah-Whye Peng ,Stephen J Russell ,Saad S Kenderian

Abstract

Although chimeric antigen receptor T (CART)-cell therapy has been successful in treating certain hematologic malignancies, wider adoption of CART-cell therapy is limited because of minimal activity in solid tumors and development of life-threatening toxicities, including cytokine release syndrome (CRS). There is a lack of a robust, clinically relevant imaging platform to monitor in vivo expansion and trafficking to tumor sites. To address this, we utilized the sodium iodide symporter (NIS) as a platform to image and track CART cells. We engineered CD19-directed and B-cell maturation antigen (BCMA)-directed CART cells to express NIS (NIS+CART19 and NIS+BCMA-CART, respectively) and tested the sensitivity of 18F-TFB-PET to detect trafficking and expansion in systemic and localized tumor models and in a CART-cell toxicity model. NIS+CART19 and NIS+BCMA-CART cells were generated through dual transduction with two vectors and demonstrated exclusive 125I uptake in vitro. 18F-TFB-PET detected NIS+CART cells in vivo to a sensitivity level of 40,000 cells. 18F-TFB-PET confirmed NIS+BCMA-CART-cell trafficking to the tumor sites in localized and systemic tumor models. In a xenograft model for CART-cell toxicity, 18F-TFB-PET revealed significant systemic uptake, correlating with CART-cell in vivo expansion, cytokine production, and development of CRS-associated clinical symptoms. NIS provides a sensitive, clinically applicable platform for CART-cell imaging with PET scan. 18F-TFB-PET detected CART-cell trafficking to tumor sites and in vivo expansion, correlating with the development of clinical and laboratory markers of CRS. These studies demonstrate a noninvasive, clinically relevant method to assess CART-cell functions in vivo.

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