The Contribution of the Minimal Promoter Element to the Activity of Synthetic Promoters Mediating CAR Expression in the Tumor Microenvironment

Yariv Greenshpan; Omri Sharabi; Ksenia M. Yegodayev; Ofra Novoplansky; Moshe Elkabets; Roi Gazit; Angel Porgador

doi:10.3390/ijms23137431

The Contribution of the Minimal Promoter Element to the Activity of Synthetic Promoters Mediating CAR Expression in the Tumor Microenvironment

Yariv Greenshpan, Omri Sharabi, Ksenia M. Yegodayev, Ofra Novoplansky, Moshe Elkabets, Roi Gazit, Angel Porgador

Research output: Contribution to journal › Article › peer-review

5 Scopus citations

Abstract

Harnessing immune effector cells to benefit cancer patients is becoming more and more prevalent in recent years. However, the increasing number of different therapeutic approaches, such as chimeric antigen receptors and armored chimeric antigen receptors, requires constant adjustments of the transgene expression levels. We have previously demonstrated it is possible to achieve spatial and temporal control of transgene expression as well as tailoring the inducing agents using the Chimeric Antigen Receptor Tumor Induced Vector (CARTIV) platform. Here we describe the next level of customization in our promoter platform. We have tested the functionality of three different minimal promoters, representing three different promoters’ strengths, leading to varying levels of CAR expression and primary T cell function. This strategy shows yet another level of CARTIV gene regulation that can be easily integrated into existing CAR T systems.

Original language	English
Article number	7431
Journal	International Journal of Molecular Sciences
Volume	23
Issue number	13
DOIs	https://doi.org/10.3390/ijms23137431
State	Published - 4 Jul 2022

Keywords

CARTIV
chimeric antigen receptor
minimal promoter
synthetic promoter

ASJC Scopus subject areas

Catalysis
Molecular Biology
Spectroscopy
Computer Science Applications
Physical and Theoretical Chemistry
Organic Chemistry
Inorganic Chemistry

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.3390/ijms23137431

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title = "The Contribution of the Minimal Promoter Element to the Activity of Synthetic Promoters Mediating CAR Expression in the Tumor Microenvironment",

abstract = "Harnessing immune effector cells to benefit cancer patients is becoming more and more prevalent in recent years. However, the increasing number of different therapeutic approaches, such as chimeric antigen receptors and armored chimeric antigen receptors, requires constant adjustments of the transgene expression levels. We have previously demonstrated it is possible to achieve spatial and temporal control of transgene expression as well as tailoring the inducing agents using the Chimeric Antigen Receptor Tumor Induced Vector (CARTIV) platform. Here we describe the next level of customization in our promoter platform. We have tested the functionality of three different minimal promoters, representing three different promoters{\textquoteright} strengths, leading to varying levels of CAR expression and primary T cell function. This strategy shows yet another level of CARTIV gene regulation that can be easily integrated into existing CAR T systems.",

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author = "Yariv Greenshpan and Omri Sharabi and Yegodayev, {Ksenia M.} and Ofra Novoplansky and Moshe Elkabets and Roi Gazit and Angel Porgador",

note = "Funding Information: Funding: This research was funded by: Israel Science Foundation grant: 2484/19 (A.P.) and 883/21 (R.G.); ISF-NRF: 3127/19 (A.P.); DKFZ-MOST grant: CA194 (A.P.); United States-Israel Binational Science Foundation: 2019377 (A.P.); Ministry of Health: 3-15080 (R.G. and A.P.). Publisher Copyright: {\textcopyright} 2022 by the authors. Licensee MDPI, Basel, Switzerland.",

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language = "English",

volume = "23",

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AU - Greenshpan, Yariv

AU - Sharabi, Omri

AU - Yegodayev, Ksenia M.

AU - Novoplansky, Ofra

AU - Elkabets, Moshe

AU - Gazit, Roi

AU - Porgador, Angel

N1 - Funding Information: Funding: This research was funded by: Israel Science Foundation grant: 2484/19 (A.P.) and 883/21 (R.G.); ISF-NRF: 3127/19 (A.P.); DKFZ-MOST grant: CA194 (A.P.); United States-Israel Binational Science Foundation: 2019377 (A.P.); Ministry of Health: 3-15080 (R.G. and A.P.). Publisher Copyright: © 2022 by the authors. Licensee MDPI, Basel, Switzerland.

PY - 2022/7/4

Y1 - 2022/7/4

N2 - Harnessing immune effector cells to benefit cancer patients is becoming more and more prevalent in recent years. However, the increasing number of different therapeutic approaches, such as chimeric antigen receptors and armored chimeric antigen receptors, requires constant adjustments of the transgene expression levels. We have previously demonstrated it is possible to achieve spatial and temporal control of transgene expression as well as tailoring the inducing agents using the Chimeric Antigen Receptor Tumor Induced Vector (CARTIV) platform. Here we describe the next level of customization in our promoter platform. We have tested the functionality of three different minimal promoters, representing three different promoters’ strengths, leading to varying levels of CAR expression and primary T cell function. This strategy shows yet another level of CARTIV gene regulation that can be easily integrated into existing CAR T systems.

AB - Harnessing immune effector cells to benefit cancer patients is becoming more and more prevalent in recent years. However, the increasing number of different therapeutic approaches, such as chimeric antigen receptors and armored chimeric antigen receptors, requires constant adjustments of the transgene expression levels. We have previously demonstrated it is possible to achieve spatial and temporal control of transgene expression as well as tailoring the inducing agents using the Chimeric Antigen Receptor Tumor Induced Vector (CARTIV) platform. Here we describe the next level of customization in our promoter platform. We have tested the functionality of three different minimal promoters, representing three different promoters’ strengths, leading to varying levels of CAR expression and primary T cell function. This strategy shows yet another level of CARTIV gene regulation that can be easily integrated into existing CAR T systems.

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The Contribution of the Minimal Promoter Element to the Activity of Synthetic Promoters Mediating CAR Expression in the Tumor Microenvironment

Abstract

Keywords

ASJC Scopus subject areas

UN SDGs

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