论文信息 - CRISPR-Cas, a robust gene-editing technology in the era of modern cancer immunotherapy

CRISPR-Cas, a robust gene-editing technology in the era of modern cancer immunotherapy

Cancer immunotherapy has been emerged as a promising strategy for treatment of a broad spectrum of malignancies ranging from hematological to solid tumors. One of the principal approaches of cancer immunotherapy is transfer of natural or engineered tumor-specific T-cells into patients, a so called “adoptive cell transfer”, or ACT, process. Construction of allogeneic T-cells is dependent on the employment of a gene-editing tool to modify donor-extracted T-cells and prepare them to specifically act against tumor cells with enhanced function and durability and least side-effects. In this context, CRISPR technology can be used to produce universal T-cells, equipped with recombinant T cell receptor (TCR) or chimeric antigen receptor (CAR), through multiplex genome engineering using Cas nucleases. The robust potential of CRISPR-Cas in preparing the building blocks of ACT immunotherapy has broaden the application of such therapies and some of them have gotten FDA approvals. Here, we have collected the last investigations in the field of immuno-oncology conducted in partnership with CRISPR technology. In addition, studies that have addressed the challenges in the path of CRISPR-mediated cancer immunotherapy, as well as pre-treatment applications of CRISPR-Cas have been mentioned in detail.

[1] A. Jemal,et al. Global cancer statistics 2018: GLOBOCAN estimates of incidence and mortality worldwide for 36 cancers in 185 countries , 2018, CA: a cancer journal for clinicians.

[2] B. Cullen,et al. Gene Editing: A New Tool for Viral Disease. , 2017, Annual review of medicine.

[3] Aaron J Johnson,et al. GM-CSF inhibition reduces cytokine release syndrome and neuroinflammation but enhances CAR-T cell function in xenografts. , 2019, Blood.

[4] C. Seeger,et al. Targeting Hepatitis B Virus With CRISPR/Cas9 , 2014, Molecular therapy. Nucleic acids.

[5] Wendell A Lim,et al. Engineering Therapeutic T Cells: From Synthetic Biology to Clinical Trials. , 2017, Annual review of pathology.

[6] Anob M. Chakrabarti,et al. Target-Specific Precision of CRISPR-Mediated Genome Editing , 2018, bioRxiv.

[7] Česlovas Venclovas,et al. Spatiotemporal Control of Type III-A CRISPR-Cas Immunity: Coupling DNA Degradation with the Target RNA Recognition. , 2016, Molecular cell.

[8] Sita J. Saunders,et al. An updated evolutionary classification of CRISPR–Cas systems , 2015, Nature Reviews Microbiology.

[9] Xiaojing Ma,et al. CRISPR/Cas9-mediated PD-1 disruption enhances human mesothelin-targeted CAR T cell effector functions , 2018, Cancer Immunology, Immunotherapy.

[10] F. Ossendorp,et al. PD-L1 expression on malignant cells is no prerequisite for checkpoint therapy , 2017, Oncoimmunology.

[11] A. Sher,et al. Foreign antigen-independent memory-phenotype CD4+ T cells: a new player in innate immunity? , 2018, Nature Reviews Immunology.

[12] E. Morris,et al. Optimizing T-cell receptor gene therapy for hematologic malignancies. , 2016, Blood.

[13] Vaccination with CD47 deficient tumor cells elicits an antitumor immune response in mice , 2020, Nature Communications.

[14] Shawna Benston. Everything in moderation, even hype: learning from vaccine controversies to strike a balance with CRISPR , 2017, Journal of Medical Ethics.

[15] Matthew D. Hellmann,et al. Immune‐Related Adverse Events Associated with Immune Checkpoint Blockade , 2018, The New England journal of medicine.

[16] M. Geyer,et al. CD19-targeted CAR T-cell therapeutics for hematologic malignancies: interpreting clinical outcomes to date. , 2016, Blood.

[17] A. Huang,et al. Chemokines as Cancer Vaccine Adjuvants , 2013, Vaccines.

[18] Haoyi Wang,et al. Gene editing in T cell therapy. , 2017, Journal of genetics and genomics = Yi chuan xue bao.

[19] Hans Clevers,et al. Efficient Intracellular Delivery of Native Proteins , 2015, Cell.

[20] W. Cho,et al. The rise of human stem cell-derived natural killer cells for cancer immunotherapy , 2019, Expert opinion on biological therapy.

[21] David A. Scott,et al. Double Nicking by RNA-Guided CRISPR Cas9 for Enhanced Genome Editing Specificity , 2013, Cell.

[22] Kira S. Makarova,et al. Diversity and evolution of class 2 CRISPR–Cas systems , 2017, Nature Reviews Microbiology.

[23] S. Rahman,et al. CRISPR/Cas9: the Jedi against the dark empire of diseases , 2018, Journal of Biomedical Science.

[24] Freeman Lan,et al. Nanoparticle delivery of Cas9 ribonucleoprotein and donor DNA in vivo induces homology-directed DNA repair , 2017, Nature Biomedical Engineering.

[25] Chao Wang,et al. Self-assembled DNA nanoclews for the efficient delivery of CRISPR-Cas9 for genome editing. , 2015, Angewandte Chemie.

[26] P. Khanal,et al. The Hippo Pathway Component TAZ Promotes Immune Evasion in Human Cancer through PD-L1. , 2018, Cancer research.

[27] John G. Doench,et al. In vivo CRISPR screening identifies Ptpn2 as a cancer immunotherapy target , 2017, Nature.

[28] N. Palaniyar,et al. NET balancing: a problem in inflammatory lung diseases , 2013, Front. Immun..

[29] Carl H. June,et al. Multiplex Genome Editing to Generate Universal CAR T Cells Resistant to PD1 Inhibition , 2016, Clinical Cancer Research.

[30] Kole T. Roybal,et al. Precision Tumor Recognition by T Cells With Combinatorial Antigen-Sensing Circuits , 2016, Cell.

[31] A. Ghaemi,et al. Combination of the toll like receptor agonist and α-Galactosylceramide as an efficient adjuvant for cancer vaccine , 2016, Journal of Biomedical Science.

[32] Yuquan Wei,et al. Tumor cells induce LAMP2a expression in tumor-associated macrophage for cancer progression , 2019, EBioMedicine.

[33] Jia Wei,et al. CRISPR-Cas9-mediated disruption of PD-1 on human T cells for adoptive cellular therapies of EBV positive gastric cancer , 2017, Oncoimmunology.

[34] Eugene V Koonin,et al. Diversity, classification and evolution of CRISPR-Cas systems. , 2017, Current opinion in microbiology.

[35] Jian Chen,et al. Efficient homology-directed gene editing by CRISPR/Cas9 in human stem and primary cells using tube electroporation , 2018, Scientific Reports.

[36] O. Mo. CRISPR-Cas9 Human Genome Editing: Challenges, Ethical Concerns and Implications , 2015 .

[37] J. Falkenburg,et al. Simultaneous Deletion of Endogenous TCRαβ for TCR Gene Therapy Creates an Improved and Safe Cellular Therapeutic. , 2020, Molecular therapy : the journal of the American Society of Gene Therapy.

[38] Chun Jimmie Ye,et al. CRISPR/Cas9-mediated PD-1 disruption enhances anti-tumor efficacy of human chimeric antigen receptor T cells , 2016, Scientific Reports.

[39] S. Rosenberg,et al. Augmented Lymphocyte Expansion from Solid Tumors With Engineered Cells for Costimulatory Enhancement , 2011, Journal of immunotherapy.

[40] Xingxu Huang,et al. Nucleofection with Plasmid DNA for CRISPR/Cas9-Mediated Inactivation of Programmed Cell Death Protein 1 in CD133-Specific CAR T Cells. , 2018, Human gene therapy.

[41] Charles A Gersbach,et al. Increasing the specificity of CRISPR systems with engineered RNA secondary structures , 2019, Nature Biotechnology.

[42] P. Gregory,et al. Comparison of Zinc Finger Nucleases Versus CRISPR-Specific Nucleases for Genome Editing of the Wiskott-Aldrich Syndrome Locus. , 2017, Human gene therapy.

[43] A. Ghaemi,et al. Synergistic effect of programmed cell death protein 1 blockade and secondary lymphoid tissue chemokine in the induction of anti-tumor immunity by a therapeutic cancer vaccine , 2017, Archives of Virology.

[44] N. Lemoine,et al. CRISPR-Cas9 as a Powerful Tool for Efficient Creation of Oncolytic Viruses , 2016, Viruses.

[45] C. Klein,et al. Leukemia-induced dysfunctional TIM-3+CD4+ bone marrow T cells increase risk of relapse in pediatric B-precursor ALL patients , 2020, Leukemia.

[46] J. Keith Joung,et al. 731. High-Fidelity CRISPR-Cas9 Nucleases with No Detectable Genome-Wide Off-Target Effects , 2016 .

[47] Kira S. Makarova,et al. Cas13d is a compact RNA-targeting type VI CRISPR effector positively modulated by a WYL domain-containing accessory protein , 2018, Molecular cell.

[48] Anita C. Schürch,et al. CRISPR/Cas9-Mediated Genome Editing of Herpesviruses Limits Productive and Latent Infections , 2016, PLoS pathogens.

[49] T. Aittokallio,et al. Integrated drug profiling and CRISPR screening identify essential pathways for CAR T cell cytotoxicity. , 2019, Blood.

[50] Jussi Taipale,et al. CRISPR–Cas9 genome editing induces a p53-mediated DNA damage response , 2018, Nature Medicine.

[51] G. Freeman,et al. LSD1 Ablation Stimulates Anti-tumor Immunity and Enables Checkpoint Blockade , 2018, Cell.

[52] Yunzi Luo,et al. Blossom of CRISPR technologies and applications in disease treatment , 2018, Synthetic and systems biotechnology.

[53] R. Bak,et al. Gene Editing on Center Stage. , 2018, Trends in genetics : TIG.

[54] A. Rolfe,et al. Genetic screen in myeloid cells identifies TNF-α autocrine secretion as a factor increasing MDSC suppressive activity via Nos2 up-regulation , 2018, Scientific Reports.

[55] Baorui Liu,et al. Engineered cells for costimulatory enhancement combined with IL-21 enhance the generation of PD-1-disrupted CTLs for adoptive immunotherapy. , 2017, Cellular immunology.

[56] K. Brown,et al. Tumor immune evasion arises through loss of TNF sensitivity , 2018, Science Immunology.

[57] Ya-Fen Hsu,et al. A Novel Hydroxamate-Based Compound WMJ-J-09 Causes Head and Neck Squamous Cell Carcinoma Cell Death via LKB1-AMPK-p38MAPK-p63-Survivin Cascade , 2018, Front. Pharmacol..

[58] Gregory Lizée,et al. Harnessing the power of the immune system to target cancer. , 2013, Annual review of medicine.

[59] S. Paczesny,et al. Immunotherapy through T-cell receptor gene transfer induces severe graft-versus-host disease. , 2010, Immunotherapy.

[60] E. Westra,et al. Evolution and Ecology of CRISPR , 2016 .

[61] S. Albelda,et al. CAR T Cell Therapy for Solid Tumors. , 2017, Annual review of medicine.

[62] E. Eyras,et al. CD133-directed CAR T-cells for MLL leukemia: on-target, off-tumor myeloablative toxicity , 2019, Leukemia.

[63] Jean-Claude Tardif,et al. Human genetic variation alters CRISPR-Cas9 on- and off-targeting specificity at therapeutically implicated loci , 2017, Proceedings of the National Academy of Sciences.

[64] R. Sathishkumar,et al. Stress-Induced Accumulation of DcAOX1 and DcAOX2a Transcripts Coincides with Critical Time Point for Structural Biomass Prediction in Carrot Primary Cultures (Daucus carota L.) , 2016, Front. Genet..

[65] Stephan Marquardt,et al. Emerging functional markers for cancer stem cell-based therapies: Understanding signaling networks for targeting metastasis. , 2018, Seminars in cancer biology.

[66] Erik J Sontheimer,et al. A Compact, High-Accuracy Cas9 with a Dinucleotide PAM for In Vivo Genome Editing. , 2019, Molecular cell.

[67] Matthew J. Frigault,et al. CRISPR-Cas9 disruption of PD-1 enhances activity of universal EGFRvIII CAR T cells in a preclinical model of human glioblastoma , 2019, Journal of Immunotherapy for Cancer.

[68] B. Levine,et al. Adoptive immunotherapy for cancer or viruses. , 2014, Annual review of immunology.

[69] Eugene V Koonin,et al. Discovery and Functional Characterization of Diverse Class 2 CRISPR-Cas Systems. , 2015, Molecular cell.

[70] J. Vogel,et al. CRISPR RNA maturation by trans-encoded small RNA and host factor RNase III , 2011, Nature.

[71] W. Cho,et al. Trastuzumab emtansine for advanced HER2-positive breast cancer and beyond: genome landscape-based targets , 2013, Expert review of anticancer therapy.

[72] W. Cho,et al. Atezolizumab in non-small cell lung cancer: the era of precision immuno-oncology. , 2017, Annals of translational medicine.

[73] C. Zhang,et al. A Novel Anti-LILRB4 CAR-T Cell for the Treatment of Monocytic AML. , 2018, Molecular therapy : the journal of the American Society of Gene Therapy.

[74] Ge Zhang,et al. In Vivo Delivery Systems for Therapeutic Genome Editing , 2016, International journal of molecular sciences.

[75] Mithat Gönen,et al. Targeting a CAR to the TRAC locus with CRISPR/Cas9 enhances tumour rejection , 2017, Nature.

[76] A. Ghaemi,et al. Antitumor effect of therapeutic HPV DNA vaccines with chitosan-based nanodelivery systems , 2014, Journal of Biomedical Science.

[77] C. Gersbach,et al. Engineering Delivery Vehicles for Genome Editing. , 2016, Annual review of chemical and biomolecular engineering.

[78] David R. Liu,et al. Fusion of catalytically inactive Cas9 to FokI nuclease improves the specificity of genome modification , 2014, Nature Biotechnology.

[79] F. Baylis. Counterpoint: The Potential Harms of Human Gene Editing Using CRISPR-Cas9. , 2018, Clinical chemistry.

[80] C. Caux,et al. Cold Tumors: A Therapeutic Challenge for Immunotherapy , 2019, Front. Immunol..

[81] Matthew J. Frigault,et al. Chimeric Antigen Receptor T Cells Targeting CD79b Show Efficacy in Lymphoma with or without Cotargeting CD19 , 2019, Clinical Cancer Research.

[82] Seokjoong Kim,et al. CRISPR/Cas9-Mediated Knockout of DGK Improves Antitumor Activities of Human T Cells. , 2018, Cancer research.

[83] Carl H. June,et al. A versatile system for rapid multiplex genome-edited CAR T cell generation , 2017, Oncotarget.

[84] Hui Wang,et al. Gene-edited stem cells enable CD33-directed immune therapy for myeloid malignancies , 2019, Proceedings of the National Academy of Sciences.

[85] I. Nakagawa,et al. Effect of CRISPR/Cas9-Mediated PD-1-Disrupted Primary Human Third-Generation CAR-T Cells Targeting EGFRvIII on In Vitro Human Glioblastoma Cell Growth , 2020, Cells.

[86] M. Stevanović,et al. Exopolysaccharide Produced by Probiotic Strain Lactobacillus paraplantarum BGCG11 Reduces Inflammatory Hyperalgesia in Rats , 2018, Front. Pharmacol..

[87] A. Ashworth,et al. Genome-wide CRISPR Screens in Primary Human T Cells Reveal Key Regulators of Immune Function , 2018, Cell.

[88] G. Freeman,et al. In vivo epigenetic CRISPR screen identifies Asf1a as an immunotherapeutic target in Kras-mutant lung adenocarcinoma. , 2019, Cancer discovery.

[89] Henry W. Long,et al. A major chromatin regulator determines resistance of tumor cells to T cell–mediated killing , 2018, Science.

[90] Hans Clevers,et al. Modeling Human Digestive Diseases With CRISPR-Cas9-Modified Organoids. , 2019, Gastroenterology.

[91] Hua Jiang,et al. Disruption of PD-1 Enhanced the Anti-tumor Activity of Chimeric Antigen Receptor T Cells Against Hepatocellular Carcinoma , 2018, Front. Pharmacol..

[92] Ding Ma,et al. Nanoparticles Based on Poly (β-Amino Ester) and HPV16-Targeting CRISPR/shRNA as Potential Drugs for HPV16-Related Cervical Malignancy. , 2018, Molecular therapy : the journal of the American Society of Gene Therapy.

[93] A. Han,et al. Cancer Immunosurveillance by T Cells. , 2019, International review of cell and molecular biology.

[94] Chenfeng Xu,et al. Cdk5 knocking out mediated by CRISPR-Cas9 genome editing for PD-L1 attenuation and enhanced antitumor immunity , 2019, Acta pharmaceutica Sinica. B.

[95] J. Doudna,et al. RNA and DNA Targeting by a Reconstituted Thermus thermophilus Type III-A CRISPR-Cas System , 2017, PloS one.

[96] P. Greenberg,et al. Obstacles Posed by the Tumor Microenvironment to T cell Activity: A Case for Synergistic Therapies. , 2017, Cancer cell.

[97] S. Nik-Zainal,et al. Use of CRISPR-modified human stem cell organoids to study the origin of mutational signatures in cancer , 2017, Science.

[98] David A. Scott,et al. Functionally diverse type V CRISPR-Cas systems , 2019, Science.

[99] Yu-Quan Wei,et al. Challenges in CRISPR/CAS9 Delivery: Potential Roles of Nonviral Vectors. , 2015, Human gene therapy.

[100] S. Kiani,et al. Engineered CRISPR Systems for Next Generation Gene Therapies. , 2017, ACS synthetic biology.

[101] M. Stetler-Stevenson,et al. Preclinical Development of Bivalent Chimeric Antigen Receptors Targeting Both CD19 and CD22 , 2018, Molecular therapy oncolytics.

[102] Androulla N. Miliotou,et al. CAR T-cell Therapy: A New Era in Cancer Immunotherapy. , 2018, Current pharmaceutical biotechnology.

[103] C. June,et al. Emerging Cellular Therapies for Cancer. , 2019, Annual review of immunology.

[104] S. Ramakrishna,et al. Different Methods of Delivering CRISPR/Cas9 Into Cells. , 2018, Progress in molecular biology and translational science.

[105] W. Cho,et al. Implementation and new insights in molecular diagnostics for HIV infection , 2018, Expert review of molecular diagnostics.

[106] Luigi Naldini,et al. A foundation for universal T-cell based immunotherapy: T cells engineered to express a CD19-specific chimeric-antigen-receptor and eliminate expression of endogenous TCR. , 2012, Blood.

[107] James E Haber,et al. The democratization of gene editing: Insights from site-specific cleavage and double-strand break repair. , 2016, DNA repair.

[108] Kaitlyn Gayvert,et al. Broad Targeting Specificity during Bacterial Type III CRISPR-Cas Immunity Constrains Viral Escape. , 2017, Cell host & microbe.

[109] W. Han,et al. TGFβ inhibition via CRISPR promotes the long-term efficacy of CAR-T cells against solid tumors. , 2020, JCI insight.

[110] H. Abken,et al. Of CARs and TRUCKs: chimeric antigen receptor (CAR) T cells engineered with an inducible cytokine to modulate the tumor stroma , 2014, Immunological reviews.

[111] Mengsu Yang,et al. Efficient RNA drug delivery using red blood cell extracellular vesicles , 2018, Nature Communications.

[112] K. Clark,et al. Genome Engineering with TALE and CRISPR Systems in Neuroscience , 2016, Front. Genet..

[113] E. McCarthy. The toxins of William B. Coley and the treatment of bone and soft-tissue sarcomas. , 2006, The Iowa orthopaedic journal.

[114] A. Varki,et al. Myeloid precursors and acute myeloid leukemia cells express multiple CD33-related Siglecs. , 2006, Experimental hematology.

[115] Guoping Cai,et al. Impaired HLA Class I Antigen Processing and Presentation as a Mechanism of Acquired Resistance to Immune Checkpoint Inhibitors in Lung Cancer. , 2017, Cancer discovery.

[116] スティーブンジェイ．ブレイクモア，,et al. How to treat cancer , 2013 .

[117] A. Banham,et al. CRISPR/Cas9-Mediated Foxp1 Silencing Restores Immune Surveillance in an Immunocompetent A20 Lymphoma Model , 2020, Frontiers in Oncology.

[118] R. Weissleder,et al. Identification and validation of a tumor-infiltrating Treg transcriptional signature conserved across species and tumor types , 2018, Proceedings of the National Academy of Sciences.

[119] P. Hwu,et al. Tumor-Infiltrating Lymphocyte Therapy for Melanoma: Rationale and Issues for Further Clinical Development , 2014, BioDrugs.

[120] M. Donia,et al. Genome-wide CRISPR-Cas9 Screening Reveals Ubiquitous T cell Cancer Targeting via the monomorphic MHC class I related protein MR1 , 2019, Nature Immunology.

[121] F. Baylis,et al. First-in-human Phase 1 CRISPR Gene Editing Cancer Trials:Are We Ready? , 2017, Current gene therapy.

[122] Michel Sadelain,et al. Combinatorial antigen recognition with balanced signaling promotes selective tumor eradication by engineered T cells , 2012, Nature Biotechnology.

[123] F. Watt,et al. Expression of a Chimeric Antigen Receptor Specific for Donor HLA Class I Enhances the Potency of Human Regulatory T Cells in Preventing Human Skin Transplant Rejection , 2017, American journal of transplantation : official journal of the American Society of Transplantation and the American Society of Transplant Surgeons.

[124] W. Lim,et al. The Principles of Engineering Immune Cells to Treat Cancer , 2017, Cell.

[125] P. Glaser,et al. Analysis of the type II-A CRISPR-Cas system of Streptococcus agalactiae reveals distinctive features according to genetic lineages , 2015, Front. Genet..

[126] Christof von Kalle,et al. Evaluation of TCR Gene Editing Achieved by TALENs, CRISPR/Cas9, and megaTAL Nucleases. , 2016, Molecular therapy : the journal of the American Society of Gene Therapy.

[127] Lixia Chen,et al. Checkpoint-modulating immunotherapies in tumor treatment: Targets, drugs, and mechanisms. , 2019, International immunopharmacology.

[128] Hilde van der Togt,et al. Publisher's Note , 2003, J. Netw. Comput. Appl..

[129] Christof von Kalle,et al. Genome-wide Specificity of Highly Efficient TALENs and CRISPR/Cas9 for T Cell Receptor Modification , 2017, Molecular therapy. Methods & clinical development.

[130] Melissa J. Fullwood,et al. Roles, Functions, and Mechanisms of Long Non-coding RNAs in Cancer , 2016, Genom. Proteom. Bioinform..

[131] Adam Bagg,et al. Genetic Inactivation of CD33 in Hematopoietic Stem Cells to Enable CAR T Cell Immunotherapy for Acute Myeloid Leukemia , 2018, Cell.

[132] Junhan Yang,et al. The construction of a new oncolytic herpes simplex virus expressing murine interleukin‐15 with gene‐editing technology , 2020, Journal of medical virology.

[133] G. Kvalheim,et al. A TCR-based Chimeric Antigen Receptor , 2017, Scientific Reports.

[134] H. Abken,et al. Antigen-Specific T-Cell Activation Independently of the MHC: Chimeric Antigen Receptor-Redirected T Cells , 2013, Front. Immunol..

[135] John G. Doench,et al. Targeting REGNASE-1 programs long-lived effector T cells for cancer therapy , 2019, Nature.

[136] J. Doudna,et al. Applications of CRISPR-Cas Enzymes in Cancer Therapeutics and Detection. , 2018, Trends in cancer.

[137] M. Boccadoro,et al. Clinical Applications and Future Directions of Minimal Residual Disease Testing in Multiple Myeloma , 2020, Frontiers in Oncology.

[138] S. Rives,et al. Development of a Novel Anti-CD19 Chimeric Antigen Receptor: A Paradigm for an Affordable CAR T Cell Production at Academic Institutions , 2018, Molecular therapy. Methods & clinical development.

[139] Emmanuelle Charpentier,et al. The Biology of CRISPR-Cas: Backward and Forward , 2018, Cell.

[140] D. Kranz,et al. Adoptive T Cell Therapies: A Comparison of T Cell Receptors and Chimeric Antigen Receptors. , 2016, Trends in pharmacological sciences.

[141] M. Nishimura,et al. Strategies to genetically engineer T cells for cancer immunotherapy , 2016, Cancer Immunology, Immunotherapy.

[142] Neil Humphryes-Kirilov,et al. Long Terminal Repeat CRISPR-CAR-Coupled "Universal" T Cells Mediate Potent Anti-leukemic Effects. , 2018, Molecular therapy : the journal of the American Society of Gene Therapy.

[143] H. Kaufman,et al. Integrating oncolytic viruses in combination cancer immunotherapy , 2018, Nature Reviews Immunology.

[144] Lynda Chin,et al. Post-translational Regulation of Cas9 during G1 Enhances Homology-Directed Repair. , 2016, Cell reports.

[145] Jennifer A. Doudna,et al. Programmed DNA destruction by miniature CRISPR-Cas14 enzymes , 2018, Science.

[146] Dekun Chen,et al. Methodologies for Improving HDR Efficiency , 2019, Front. Genet..

[147] P. Bayrak-Toydemir,et al. Hereditary hemorrhagic telangiectasia: genetics and molecular diagnostics in a new era , 2015, Front. Genet..

[148] A. Jarry,et al. Increased antitumor efficacy of PD-1-deficient melanoma-specific human lymphocytes , 2020, Journal for ImmunoTherapy of Cancer.

[149] A. Ghaemi,et al. Oncolytic paramyxoviruses-induced autophagy; a prudent weapon for cancer therapy , 2019, Journal of Biomedical Science.

[150] K. Wucherpfennig,et al. Genetic screens to study the immune system in cancer. , 2016, Current opinion in immunology.

[151] Yanchun Peng,et al. Genetic abrogation of immune checkpoints in antigen-specific cytotoxic T-lymphocyte as a potential alternative to blockade immunotherapy , 2018, Scientific Reports.

[152] I. Papangeli,et al. CRISPR/Cas9 gene-editing: Research technologies, clinical applications and ethical considerations. , 2018, Seminars in perinatology.

[153] A. Sewell,et al. CRISPR-mediated TCR replacement generates superior anticancer transgenic T cells. , 2018, Blood.

[154] W. Cho,et al. Immune checkpoint blockade as a potential therapeutic target in non-small cell lung cancer , 2016, Expert opinion on biological therapy.

[155] C. Ramos,et al. CD7 CAR T Cells for the Therapy of Acute Myeloid Leukemia. , 2019, Molecular therapy : the journal of the American Society of Gene Therapy.

[156] Dario Campana,et al. A novel method to generate T-cell receptor-deficient chimeric antigen receptor T cells. , 2018, Blood advances.

[157] Bryan R. Cullen,et al. Inactivation of the Human Papillomavirus E6 or E7 Gene in Cervical Carcinoma Cells by Using a Bacterial CRISPR/Cas RNA-Guided Endonuclease , 2014, Journal of Virology.