Reversing T Cell Exhaustion by Converting Membrane Pd-1 to Its Soluble Form in Jurkat Cells; Applying the Crispr/Cas9 Exon Skipping Strategy

Science Communicator Platform

Stay connected! Follow us on X network (Twitter):

Share By

Reversing T Cell Exhaustion by Converting Membrane Pd-1 to Its Soluble Form in Jurkat Cells; Applying the Crispr/Cas9 Exon Skipping Strategy Publisher

Yousefinajafabadi Z^{1, 2} ; Mehmandoostli Z² ; Asgari Y¹ ; Kaboli S³ ; Falak R⁴ ; Kardar GA^{1, 2}

Source: Cell Journal Published:2023

Abstract

Objective: T-cells express two functional forms of the programmed cell death protein 1 (PD-1): membrane (mPD-1) and soluble (sPD-1). The binding of mPD-1 and its ligand (PD-L1) on tumor cells could lead activated lymphocytes toward exhaustion. Selective deletion of the transmembrane domain via alternative splicing of exon-3 in PD-1 mRNA could generate sPD-1. Overexpression of sPD-1 could disrupt the mPD-1/PD-L1 interaction in tumor-specific T cells. We investigated the effect of secreted sPD-1 from pooled engineered and non-engineered T cell supernatant on survival and proliferation of lymphocytes in the tumor microenvironment (TME). Materials and Methods: In this experimental study, we designed two sgRNA sequences upstream and downstream of exon-3 in the PDCD1 gene. The lentiCRISPRv2 puro vector was used to clone the dual sgRNAs and produce lentiviral particles to transduce Jurkat T cells. Analysis assays were used to clarify the change in PD-1 expression pattern in the pooled (engineered and non-engineered) Jurkat cells. Co-culture conditions were established with PD-L1+ cancer cells and lymphocytes. Results: CRISPR/Cas9 could delete exon-3 of the PDCD1 gene in the engineered cells based on the tracking of indels by decomposition (TIDE) and interference of CRISPR edit (ICE) sequencing analysis reports. Our results showed a 12% reduction in mPD-1 positive cell population after CRISPR manipulation and increment in sPD-1 concentration in the supernatant. The increased sPD-1 confirmed its positive effect on proliferation of lymphocytes co-cultured with PDL1+ cancer cells. The survival percent of lymphocytes co-cultured with the pooled cells supernatant was 12.5% more than the control. Conclusion: The CRISPR/Cas9 exon skipping approach could be used in adoptive cell immunotherapies to change PD-1 expression patterns and overcome exhaustion. © 2023 Royan Institute (ACECR). All rights reserved.

Related Docs

View other Related Docs

1. Pd-1 and Cancer: Molecular Mechanisms and Polymorphisms, Immunogenetics (2018)

2. Gene-Knocked Out Chimeric Antigen Receptor (Car) T Cells: Tuning up for the Next Generation Cancer Immunotherapy, Cancer Letters (2018)

3. How Micrornas Affect the Pd-L1 and Its Synthetic Pathway in Cancer, International Immunopharmacology (2020)

Experts (# of related papers)

View all Related Experts

Nima Rezaei (4)

Hamid Reza Mirzaei (2)

Other Related Docs

4. Blockage of Immune Checkpoint Molecules Increases T-Cell Priming Potential of Dendritic Cell Vaccine, Immunology (2020)

5. A Vhh-Based Anti-Muc1 Chimeric Antigen Receptor for Specific Retargeting of Human Primary T Cells to Muc1-Positive Cancer Cells, Cell Journal (2021)

6. Pd-1/Pd-L1 Pathway: Basic Biology and Role in Cancer Immunotherapy, Journal of Cellular Physiology (2019)

7. The Molecular Landscape of T Cell Exhaustion in the Tumor Microenvironment and Reinvigoration Strategies, International Reviews of Immunology (2024)

8. Transcript-Level Regulation of Malat1-Mediated Cell Cycle and Apoptosis Genes Using Dual Mek/Aurora Kinase Inhibitor “Bi-847325” on Anaplastic Thyroid Carcinoma, DARU# Journal of Pharmaceutical Sciences (2019)

9. Immune Checkpoint Inhibitor (Ici) Therapy in Central Nervous System Cancers: State-Of-The-Art and Future Outlook, International Immunopharmacology (2025)

10. Casilico: A Versatile Crispr Package for in Silico Crispr Rna Designing for Cas12, Cas13, and Cas14, Frontiers in Bioengineering and Biotechnology (2022)

11. Crispr/Cas9 Revitalizes Adoptive T-Cell Therapy for Cancer Immunotherapy, Journal of Experimental and Clinical Cancer Research (2021)

12. Scrutinizing the Expression and Blockade of Inhibitory Molecules Expressed on T Cells From Acute Myeloid Leukemia Patients, Iranian Journal of Allergy# Asthma and Immunology (2018)

13. The Potential of T Cell Immunoglobulin and Mucin-Domain Containing-3 (Tim-3) in Designing Novel Immunotherapy for Bladder Cancer, Endocrine# Metabolic and Immune Disorders - Drug Targets (2021)

14. Effects of Valproic Acid and Pioglitazone on Cell Cycle Progression and Proliferation of T-Cell Acute Lymphoblastic Leukemia Jurkat Cells, Iranian Journal of Basic Medical Sciences (2016)

15. Implication of T Cell Exhaustion in Neuropsychiatric Disorders: Neuroimmunopathology and Treatment Strategies, Integrated Science (2024)

16. Chimeric Antigen Receptor-Natural Killer Cells: A Promising Sword Against Insidious Tumor Cells, Human Cell (2023)

17. Design of an Expression System for Rapid Production of Tri-Functional Antibody Substitution of Hybrid Hybridoma Technology, Acta Medica Iranica (2018)

18. Soluble and Immobilized Anti-Cd3/28 Distinctively Expand and Differentiate Primary Human T Cells: An Implication for Adoptive T Cell Therapy, Iranian Journal of Allergy# Asthma and Immunology (2022)

19. Macrophage Polarity in Cancer: A Review, Journal of Cellular Biochemistry (2019)

20. Downregulation of Immunosuppressive Molecules, Pd-1 and Pd-L1 But Not Pd-L2, in the Patients With Multiple Sclerosis, Iranian Journal of Allergy# Asthma and Immunology (2016)

Style	Citing Format
MLA	Yousefinajafabadi Z, et al.. "Reversing T Cell Exhaustion by Converting Membrane Pd-1 to Its Soluble Form in Jurkat Cells; Applying the Crispr/Cas9 Exon Skipping Strategy." Cell Journal, vol. 25, no. 9, 2023, pp. 633-644.
APA	Yousefinajafabadi Z, Mehmandoostli Z, Asgari Y, Kaboli S, Falak R, Kardar GA (2023). Reversing T Cell Exhaustion by Converting Membrane Pd-1 to Its Soluble Form in Jurkat Cells; Applying the Crispr/Cas9 Exon Skipping Strategy. Cell Journal, 25(9), 633-644.
Chicago	Yousefinajafabadi Z, Mehmandoostli Z, Asgari Y, Kaboli S, Falak R, Kardar GA. "Reversing T Cell Exhaustion by Converting Membrane Pd-1 to Its Soluble Form in Jurkat Cells; Applying the Crispr/Cas9 Exon Skipping Strategy." Cell Journal 25, no. 9 (2023): 633-644.
Harvard	Yousefinajafabadi Z et al. (2023) 'Reversing T Cell Exhaustion by Converting Membrane Pd-1 to Its Soluble Form in Jurkat Cells; Applying the Crispr/Cas9 Exon Skipping Strategy', Cell Journal, 25(9), pp. 633-644.
Vancouver	Yousefinajafabadi Z, Mehmandoostli Z, Asgari Y, Kaboli S, Falak R, Kardar GA. Reversing T Cell Exhaustion by Converting Membrane Pd-1 to Its Soluble Form in Jurkat Cells; Applying the Crispr/Cas9 Exon Skipping Strategy. Cell Journal. 2023;25(9):633-644.
BibTex	@article{ author = {Yousefinajafabadi Z and Mehmandoostli Z and Asgari Y and Kaboli S and Falak R and Kardar GA}, title = {Reversing T Cell Exhaustion by Converting Membrane Pd-1 to Its Soluble Form in Jurkat Cells; Applying the Crispr/Cas9 Exon Skipping Strategy}, journal = {Cell Journal}, volume = {25}, number = {9}, pages = {633-644}, year = {2023} }
RIS	TY - JOUR AU - Yousefinajafabadi Z AU - Mehmandoostli Z AU - Asgari Y AU - Kaboli S AU - Falak R AU - Kardar GA TI - Reversing T Cell Exhaustion by Converting Membrane Pd-1 to Its Soluble Form in Jurkat Cells; Applying the Crispr/Cas9 Exon Skipping Strategy JO - Cell Journal VL - 25 IS - 9 SP - 633 EP - 644 PY - 2023 ER -

Science Communicator Platform

Authors

Abstract