Your search keyword '"Gregory, Pd"' showing total 10 results

1. 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

Author

Dean A. Lee, Helen Huls, Michael C. Holmes, Pei-Qi Liu, Chiara Bonini, Laurence J.N. Cooper, Partow Kebriaei, Yuanyue Zhou, Sourindra Maiti, Richard E. Champlin, Edward J. Rebar, Luigi Naldini, Brian Rabinovitch, Hiroki Torikai, Philip D. Gregory, Ling Zhang, Andreas Reik, Jeffrey C. Miller, Torikai, H1, Reik, A, Liu, Pq, Zhou, Y, Zhang, L, Maiti, S, Huls, H, Miller, Jc, Kebriaei, P, Rabinovitch, B, Lee, Da, Champlin, Re, Bonini, MARIA CHIARA, Naldini, Luigi, Rebar, Ej, Gregory, Pd, Holmes, Mc, and Cooper, Lj

Subjects

Adult, CD3 Complex, T-Lymphocytes, T cell, Antigens, CD19, Immunology, Receptors, Antigen, T-Cell, Antigen-Presenting Cells, Streptamer, Biology, Lymphocyte Activation, Biochemistry, Epitopes, Gene Knockout Techniques, 03 medical and health sciences, 0302 clinical medicine, CD28 Antigens, Antigens, Neoplasm, medicine, Humans, Cytotoxic T cell, IL-2 receptor, Antigen-presenting cell, Cells, Cultured, 030304 developmental biology, 0303 health sciences, T-cell receptor, Zinc Fingers, Gene Therapy, Cell Biology, Hematology, Endonucleases, Molecular biology, Recombinant Proteins, Chimeric antigen receptor, 3. Good health, Cell biology, medicine.anatomical_structure, Immunotherapy, Genetic Engineering, K562 Cells, CD8, 030215 immunology

Abstract

Clinical-grade T cells are genetically modified ex vivo to express a chimeric antigen receptor (CAR) to redirect specificity to a tumor associated antigen (TAA) thereby conferring antitumor activity in vivo. T cells expressing a CD19-specific CAR recognize B-cell malignancies in multiple recipients independent of major histocompatibility complex (MHC) because the specificity domains are cloned from the variable chains of a CD19 monoclonal antibody. We now report a major step toward eliminating the need to generate patient-specific T cells by generating universal allogeneic TAA-specific T cells from one donor that might be administered to multiple recipients. This was achieved by genetically editing CD19-specific CAR+ T cells to eliminate expression of the endogenous αβ T-cell receptor (TCR) to prevent a graft-versus-host response without compromising CAR-dependent effector functions. Genetically modified T cells were generated using the Sleeping Beauty system to stably introduce the CD19-specific CAR with subsequent permanent deletion of α or β TCR chains with designer zinc finger nucleases. We show that these engineered T cells display the expected property of having redirected specificity for CD19 without responding to TCR stimulation. CAR+TCRneg T cells of this type may potentially have efficacy as an off-the-shelf therapy for investigational treatment of B-lineage malignancies.

Published

2012

2. TCR Gene Editing Results in Effective Immunotherapy of Leukemia without the Development of GvHD

Author

Maurilio Ponzoni, Giulia Casorati, Andreas Reik, Philip D. Greenberg, Barbara Camisa, Luigi Naldini, Michael C. Holmes, Angelo Lombardo, Fabio Ciceri, Claudio Bordignon, Pei-Qi Liu, Pietro Genovese, Philip D. Gregory, Chiara Bonini, Lei Zhang, J. Kuball, David Paschon, Elena Provasi, Victoria Chu, Zulma Magnani, Attilio Bondanza, Provasi, E, Genovese, P, Lombardo, A, Magnani, Z, Liu, Pq, Reik, A, Chu, V, Paschon, De, Zhang, L, Kuball, J, Camisa, B, Bondanza, Attilio, Casorati, G, Ponzoni, Maurilio, Ciceri, Fabio, Bordignon, Claudio, Greenberg, Pd, Holmes, Mc, Gregory, Pd, Naldini, L, Bonini, MARIA CHIARA, Liu, P, and Paschon, D. E.

Subjects

T cell receptor complex, biology, CD3, T cell, medicine.medical_treatment, Immunology, T-cell receptor, CD28, Cell Biology, Hematology, Immunotherapy, Biochemistry, Cell biology, medicine.anatomical_structure, Antigen, biology.protein, medicine, CD8

Abstract

Abstract 667 Transfer of high-avidity T-cell receptor (TCR) genes isolated from rare tumor-specific lymphocytes into polyclonal CD8+ T cells is an attractive strategy for targeted cancer immunotherapy. However, the successful implementation of this approach is limited by technical and safety issues, including inefficient gene transfer, unstable transgene expression, exhaustion of gene-modified cells and most importantly, the unpredictable results of mispairing between the endogenous and exogenous TCR chains. Indeed, co-expression of the endogenous and exogenous TCR in the same cell not only reduces cell-surface expression of the introduced tumor-specific TCR, but also drives the potential for these gene-modified T cells to acquire autoreactive specificities. Such TCR mispairing has been shown to result in autoreactive T cells in animal models [Bendle et al., Nat Med. 2010]. To partially overcome these limitations, we have developed a novel strategy based on zinc finger nucleases (ZFNs) that permits editing of T cell specificity at the DNA level, combining the disruption of the endogenous TCR chain genes with the transfer of a tumor-specific TCR. Two sets of ZFNs were designed targeting the constant regions of the α (TRAC-ZFN) and β (TRBC-ZFN) TCR chain genes, respectively. We transiently delivered these ZFNs into primary T lymphocytes activated with anti-CD3 and anti-CD28 antibody-conjugated beads and cultured with low doses of IL-7 and IL-15, to promote the survival and expansion of the ZFN-modified cells. ZFN delivery into activated T lymphocytes abrogated expression of the CD3/TCR complex on the cell surface (% of CD3neg cells with TRAC-ZFN: 34%±11 and with TRBC-ZFN: 30%±9). No phenotypic differences were observed in CD3pos and CD3neg lymphocytes, which displayed a similar CD4/CD8 ratio while displaying an early T-cell differentiation phenotype, as evidenced by high expression of CD62L, CD27, CD28 and IL-7Rα markers. Sorted CD3neg cells proved stable in culture (demonstrating that ZFN exposure was well tolerated), and did not respond to TCR-dependent stimulation with the mitogen PHA, as expected for cells carrying a disrupted TCR gene. CD3neg cells were efficiently transduced with a lentiviral vector encoding a tumor-specific exogenous TCR chain, resulting in the restoration of cell surface translocation of CD3, thus facilitating the selective expansion of TCR-transduced cells by polyclonal stimulation. To demonstrate the antitumor activity of these modified cells we selected an HLA-A2 restricted, codon-optimized cysteine-modified TCR specific for the Wilms' tumor antigen 1 (WT1). To achieve complete editing of T cell specificity, we established a protocol that sequentially disrupted the endogenous TCR α and β chains with high efficiency (averages: 36% and 18%), followed by lentiviral transfer of the tumor-specific TCR α and β chains (average efficiencies: 65% and 25%). This procedure resulted in a population of TCR-edited lymphocytes encoding only the tumor-specific TCR that, in the absence of competition from the endogenous receptor, was expressed at high physiological levels. Accordingly, TCR-edited lymphocytes were superior to conventional TCR-transferred cells in promoting specific recognition of WT1-expressing targets, including primary leukemias, and most importantly, were devoid of residual endogenous TCR reactivity including alloreactivity. Finally, in a humanized GvHD model, we showed that, at a variance with 100% of mice infused with unmanipulated T cells, and 80% of mice receiving TCR-transferred lymphocytes developing lethal GvHD, no GvHD was observed upon infusion of matched TCR-edited cells, despite robust T cell engraftment rates across all groups. These data demonstrate that the successful genetic re-programming of T cell specificity in primary lymphocytes results in a functionally superior target specific killing activity and thus has the potential to greatly improve the safety and therapeutic benefit of cancer immunotherapy, without triggering its potentially negative effects. (Provasi and Genovese: equal contribution). Disclosures: Liu: Sangamo Biosciences: Employment. Reik:Sangamo Biosciences: Employment. Chu:Sangamo Biosciences: Employment. Paschon:Sangamo Biosciences: Employment. Zhang:Sangamo Biosciences: Employment. Bordignon:Molmed: Employment. Holmes:Sangamo Biosciences: Employment. Gregory:Sangamo Biosciences: Employment. Bonini:Molmed: Consultancy.

Published

2011

3. T Cell Receptor Gene Transfer into Naive and Central Memory Lymphocytes by Lentiviral Vectors for a Safe and Effective Adoptive Immune Therapy of Leukemia

Author

Oscar M. Pello, Angelo Lombardo, Zulma Magnani, Jurgen Kuball, Philip D. Gregory, Chiara Bonini, Claudio Bordignon, Elena Provasi, Attilio Bondanza, Michael C. Holmes, Phil Greenberg, Luigi Naldini, Provasi, E, Pello, Om, Magnani, Z, Kuball, J, Lombardo, ANGELO LEONE, Bondanza, Attilio, Gregory, Pd, Bordignon, Claudio, Holmes, Mc, Greenberg, Pd, Naldini, Luigi, and Bonini, MARIA CHIARA

Subjects

Adoptive cell transfer, T cell, Immunology, T-cell receptor, CD28, hemic and immune systems, chemical and pharmacologic phenomena, Cell Biology, Hematology, Biology, Biochemistry, Cell biology, Viral vector, Transplantation, medicine.anatomical_structure, Antigen, medicine, Cytotoxic T cell

Abstract

The potency of cellular adoptive immunotherapy against cancer has been revealed by persistent and complete clinical responses obtained with allogeneic hemopoietic cell transplantation (allo-HSCT) followed by the adoptive transfer of donor T lymphocytes and by initial clinical responses observed with the adoptive transfer of tumor specific cytotoxic T lymphocytes (CTLs) in cancer patients. Major hurdles limiting adoptive T cell therapy relate to toxicity (i.e. graft-versus-host disease-GvHD in allo-HSCT) and efficacy (i.e. difficulty in expanding rare, high-avidity tumor-specific CTLs in conditions that can preserve their function and prevent exhaustion). The transfer of the T cell receptor (TCR) from high-avidity tumor-specific CTLs to polyclonal lymphocytes may overcome these difficulties, but is still limited by low and transient transgene expression, unpredictable pairing of the exogenous and endogenous TCR chains and poor survival and expansion potential of gene-modified effector lymphocytes. To overcome these limitations, we cloned genes encoding a high-avidity TCR specific for an HLA-A2-restricted peptide from the oncogenic Wilms tumor antigen 1 (WT1126-135), in a third generation lentiviral vector under the control of a bi-directional PGK or a bi-directional EF1α promoter. To increase TCR expression and facilitate appropriate TCR pairing, we used a codon-optimized TCR, modified with point mutations to introduce cysteines into the constant regions of the α and 7β chains. Human T lymphocytes were efficiently transduced by both vectors, following activation with anti-CD3 and anti-CD28 antibody-conjugated beads (bCD3/CD28) and culture with low doses of IL-7/IL-15. However, the PGK promoter was superior to EF1α in sustaining stochiometric expression of WT1-specific TCR chains, at levels appropriate for efficient HLA-A2/WT1 pentamer binding (16%), for up to 50 days, in the absence of further T cell stimulation. Additionally, we observed that a phenotype consistent with early (naïve and central memory) T cell differentiation (CD45RA−/+CD62L+, CD28+CD27+, IL7Ra+, IL-2+ γIFN±) was preserved in TCR-modified lymphocytes generated in these culture conditions. Sorted naïve (CD45RA+/CD62L+) and central memory (CD45RA−/CD62L+) lymphocytes were efficiently transduced by TCR-LV and maintained the original T cell phenotype. Accordingly, TCR-modified lymphocytes showed excellent survival and expansion capacity, and, upon antigenic stimulation mediated high WT1-specific γIFN production and cytotoxic activity. To improve the safety of the strategy, we attempted sitespecific integration of transgenes using of the ZFN technology. Adenoviral transfer of a set of ZFN specific for the putative safe-harbor locus CCR5 coupled with integrase defective lentiviral vectors carrying the donor DNA flanked transgene, enables efficient site-specific integration in human lymphocytes resulting in stable transgene expression. Analyses of sorted gene-modified cells is currently ongoing. Site-specific integration of an optimized, leukemia-specific TCR into both naïve and central memory lymphocytes may represent an effective method for the generation of robust engineered tumor-specific CTLs.

Published

2008

4. Long-term multilineage engraftment of autologous genome-edited hematopoietic stem cells in nonhuman primates.

Author

Peterson CW, Wang J, Norman KK, Norgaard ZK, Humbert O, Tse CK, Yan JJ, Trimble RG, Shivak DA, Rebar EJ, Gregory PD, Holmes MC, and Kiem HP

Subjects

Amino Acid Sequence, Animals, Cell Line, Electroporation, Feasibility Studies, Gene Knockdown Techniques, Graft Survival, Hematopoietic Stem Cells cytology, Hematopoietic Stem Cells metabolism, Molecular Sequence Data, Mutation, Polymerase Chain Reaction methods, RNA, Messenger genetics, Receptors, CCR5 deficiency, Sequence Analysis, DNA, Transplantation Conditioning, Transplantation, Autologous, Whole-Body Irradiation, Zinc Fingers, Bone Marrow Transplantation, Cell Lineage, Gene Editing, Hematopoietic Stem Cell Transplantation, Macaca nemestrina genetics, Receptors, CCR5 genetics

Abstract

Genome editing in hematopoietic stem and progenitor cells (HSPCs) is a promising novel technology for the treatment of many human diseases. Here, we evaluated whether the disruption of the C-C chemokine receptor 5 (CCR5) locus in pigtailed macaque HSPCs by zinc finger nucleases (ZFNs) was feasible. We show that macaque-specific CCR5 ZFNs efficiently induce CCR5 disruption at levels of up to 64% ex vivo, 40% in vivo early posttransplant, and 3% to 5% in long-term repopulating cells over 6 months following HSPC transplant. These genome-edited HSPCs support multilineage engraftment and generate progeny capable of trafficking to secondary tissues including the gut. Using deep sequencing technology, we show that these ZFNs are highly specific for the CCR5 locus in primary cells. Further, we have adapted our clonal tracking methodology to follow individual CCR5 mutant cells over time in vivo, reinforcing that CCR5 gene-edited HSPCs are capable of long-term engraftment. Together, these data demonstrate that genome-edited HSPCs engraft, and contribute to multilineage repopulation after autologous transplantation in a clinically relevant large animal model, an important step toward the development of stem cell-based genome-editing therapies for HIV and potentially other diseases as well., (© 2016 by The American Society of Hematology.)

Published

2016

5. In vivo genome editing of the albumin locus as a platform for protein replacement therapy.

Author

Sharma R, Anguela XM, Doyon Y, Wechsler T, DeKelver RC, Sproul S, Paschon DE, Miller JC, Davidson RJ, Shivak D, Zhou S, Rieders J, Gregory PD, Holmes MC, Rebar EJ, and High KA

Subjects

Albumins metabolism, Animals, Dependovirus genetics, Endonucleases, Fabry Disease genetics, Fabry Disease therapy, Factor IX genetics, Factor VIII genetics, Gaucher Disease genetics, Gaucher Disease therapy, Genetic Vectors administration & dosage, Hemophilia A genetics, Hemophilia A therapy, Hemophilia B genetics, Hemophilia B therapy, High-Throughput Nucleotide Sequencing, Humans, Lysosomes enzymology, Mice, Mice, Inbred C57BL, Mucopolysaccharidosis I genetics, Mucopolysaccharidosis I therapy, Mucopolysaccharidosis II genetics, Mucopolysaccharidosis II therapy, Promoter Regions, Genetic genetics, RNA Editing, RNA, Messenger genetics, Real-Time Polymerase Chain Reaction, Reverse Transcriptase Polymerase Chain Reaction, Zinc Fingers, Albumins genetics, Enzyme Replacement Therapy, Genetic Therapy, Genome, Liver metabolism, Transgenes physiology

Abstract

Site-specific genome editing provides a promising approach for achieving long-term, stable therapeutic gene expression. Genome editing has been successfully applied in a variety of preclinical models, generally focused on targeting the diseased locus itself; however, limited targeting efficiency or insufficient expression from the endogenous promoter may impede the translation of these approaches, particularly if the desired editing event does not confer a selective growth advantage. Here we report a general strategy for liver-directed protein replacement therapies that addresses these issues: zinc finger nuclease (ZFN) -mediated site-specific integration of therapeutic transgenes within the albumin gene. By using adeno-associated viral (AAV) vector delivery in vivo, we achieved long-term expression of human factors VIII and IX (hFVIII and hFIX) in mouse models of hemophilia A and B at therapeutic levels. By using the same targeting reagents in wild-type mice, lysosomal enzymes were expressed that are deficient in Fabry and Gaucher diseases and in Hurler and Hunter syndromes. The establishment of a universal nuclease-based platform for secreted protein production would represent a critical advance in the development of safe, permanent, and functional cures for diverse genetic and nongenetic diseases., (© 2015 by The American Society of Hematology.)

Published

2015

6. Correction of the sickle cell disease mutation in human hematopoietic stem/progenitor cells.

Author

Hoban MD, Cost GJ, Mendel MC, Romero Z, Kaufman ML, Joglekar AV, Ho M, Lumaquin D, Gray D, Lill GR, Cooper AR, Urbinati F, Senadheera S, Zhu A, Liu PQ, Paschon DE, Zhang L, Rebar EJ, Wilber A, Wang X, Gregory PD, Holmes MC, Reik A, Hollis RP, and Kohn DB

Subjects

Anemia, Sickle Cell pathology, Animals, Antigens, CD34 analysis, Base Sequence, Bone Marrow Cells metabolism, Bone Marrow Cells pathology, Cells, Cultured, Endodeoxyribonucleases metabolism, Fetal Blood transplantation, Genetic Loci, Hematopoietic Stem Cell Transplantation, Hematopoietic Stem Cells pathology, Humans, Mice, Mice, Inbred NOD, Mice, SCID, Molecular Sequence Data, Zinc Fingers, Anemia, Sickle Cell genetics, Anemia, Sickle Cell therapy, Genetic Therapy, Hematopoietic Stem Cells metabolism, Mutation, beta-Globins genetics

Abstract

Sickle cell disease (SCD) is characterized by a single point mutation in the seventh codon of the β-globin gene. Site-specific correction of the sickle mutation in hematopoietic stem cells would allow for permanent production of normal red blood cells. Using zinc-finger nucleases (ZFNs) designed to flank the sickle mutation, we demonstrate efficient targeted cleavage at the β-globin locus with minimal off-target modification. By co-delivering a homologous donor template (either an integrase-defective lentiviral vector or a DNA oligonucleotide), high levels of gene modification were achieved in CD34(+) hematopoietic stem and progenitor cells. Modified cells maintained their ability to engraft NOD/SCID/IL2rγ(null) mice and to produce cells from multiple lineages, although with a reduction in the modification levels relative to the in vitro samples. Importantly, ZFN-driven gene correction in CD34(+) cells from the bone marrow of patients with SCD resulted in the production of wild-type hemoglobin tetramers., (© 2015 by The American Society of Hematology.)

Published

2015

7. Simultaneous zinc-finger nuclease editing of the HIV coreceptors ccr5 and cxcr4 protects CD4+ T cells from HIV-1 infection.

Author

Didigu CA, Wilen CB, Wang J, Duong J, Secreto AJ, Danet-Desnoyers GA, Riley JL, Gregory PD, June CH, Holmes MC, and Doms RW

Subjects

Animals, CD4-Positive T-Lymphocytes cytology, Cell Proliferation, Female, HEK293 Cells, HIV Infections prevention & control, HIV Infections therapy, HIV-1, Humans, Male, Mice, Receptors, Chemokine metabolism, CD4-Positive T-Lymphocytes virology, Endodeoxyribonucleases metabolism, HIV Infections immunology, Receptors, CCR5 genetics, Receptors, CXCR4 genetics, Zinc Fingers

Abstract

HIV-1 entry into CD4(+) T cells requires binding of the virus to CD4 followed by engagement of either the C-C chemokine receptor 5 (CCR5) or C-X-C chemokine receptor 4 (CXCR4) coreceptor. Pharmacologic blockade or genetic inactivation of either coreceptor protects cells from infection by viruses that exclusively use the targeted coreceptor. We have used zinc-finger nucleases to drive the simultaneous genetic modification of both ccr5 and cxcr4 in primary human CD4(+) T cells. These gene-modified cells proliferated normally and were resistant to both CCR5- and CXCR4-using HIV-1 in vitro. When introduced into a humanized mouse model of HIV-1 infection, these coreceptor negative cells engraft and traffic normally, and are protected from infection with CCR5- and CXCR4-using HIV-1 strains. These data suggest that simultaneous disruption of the HIV coreceptors may provide a useful approach for the long-term, drug-free treatment of established HIV-1 infections.

Published

2014

8. Robust ZFN-mediated genome editing in adult hemophilic mice.

Author

Anguela XM, Sharma R, Doyon Y, Miller JC, Li H, Haurigot V, Rohde ME, Wong SY, Davidson RJ, Zhou S, Gregory PD, Holmes MC, and High KA

Subjects

Animals, Dependovirus genetics, Disease Models, Animal, Endonucleases metabolism, Factor IX genetics, Factor IX metabolism, Hemophilia B genetics, Hemophilia B pathology, Liver metabolism, Male, Mice, Mice, Transgenic, Protein Multimerization, Endonucleases genetics, Factor IX biosynthesis, Genetic Therapy methods, Genetic Vectors, Genome, Hemophilia B therapy, Zinc Fingers genetics

Abstract

Monogenic diseases, including hemophilia, represent ideal targets for genome-editing approaches aimed at correcting a defective gene. Here we report that systemic adeno-associated virus (AAV) vector delivery of zinc finger nucleases (ZFNs) and corrective donor template to the predominantly quiescent livers of adult mice enables production of high levels of human factor IX in a murine model of hemophilia B. Further, we show that off-target cleavage can be substantially reduced while maintaining robust editing by using obligate heterodimeric ZFNs engineered to minimize unwanted cleavage attributable to homodimerization of the ZFNs. These results broaden the therapeutic potential of AAV/ZFN-mediated genome editing in the liver and could expand this strategy to other nonreplicating cell types.

Published

2013

9. Toward eliminating HLA class I expression to generate universal cells from allogeneic donors.

Author

Torikai H, Reik A, Soldner F, Warren EH, Yuen C, Zhou Y, Crossland DL, Huls H, Littman N, Zhang Z, Tykodi SS, Kebriaei P, Lee DA, Miller JC, Rebar EJ, Holmes MC, Jaenisch R, Champlin RE, Gregory PD, and Cooper LJ

Subjects

Antigens, CD19 metabolism, Base Sequence, Cell Differentiation, Cytotoxicity, Immunologic immunology, Electroporation, Embryonic Stem Cells cytology, Gene Transfer Techniques, HEK293 Cells, Humans, Leukocytes, Mononuclear cytology, Molecular Sequence Data, Protein Engineering, T-Lymphocytes immunology, Zinc Fingers, Deoxyribonucleases genetics, Histocompatibility Antigens Class I metabolism, Stem Cell Transplantation methods, Transplantation, Homologous

Abstract

Long-term engraftment of allogeneic cells necessitates eluding immune-mediated rejection, which is currently achieved by matching for human leukocyte antigen (HLA) expression, immunosuppression, and/or delivery of donor-derived cells to sanctuary sites. Genetic engineering provides an alternative approach to avoid clearance of cells that are recognized as "non-self" by the recipient. To this end, we developed designer zinc finger nucleases and employed a "hit-and-run" approach to genetic editing for selective elimination of HLA expression. Electro-transfer of mRNA species coding for these engineered nucleases completely disrupted expression of HLA-A on human T cells, including CD19-specific T cells. The HLA-A(neg) T-cell pools can be enriched and evade lysis by HLA-restricted cytotoxic T-cell clones. Recognition by natural killer cells of cells that had lost HLA expression was circumvented by enforced expression of nonclassical HLA molecules. Furthermore, we demonstrate that zinc finger nucleases can eliminate HLA-A expression from embryonic stem cells, which broadens the applicability of this strategy beyond infusing HLA-disparate immune cells. These findings establish that clinically appealing cell types derived from donors with disparate HLA expression can be genetically edited to evade an immune response and provide a foundation whereby cells from a single donor can be administered to multiple recipients.

Published

2013

10. 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.

Author

Torikai H, Reik A, Liu PQ, Zhou Y, Zhang L, Maiti S, Huls H, Miller JC, Kebriaei P, Rabinovich B, Lee DA, Champlin RE, Bonini C, Naldini L, Rebar EJ, Gregory PD, Holmes MC, and Cooper LJ

Subjects

Adult, Antigen-Presenting Cells immunology, Antigens, Neoplasm immunology, CD28 Antigens metabolism, CD3 Complex metabolism, Cells, Cultured, Endonucleases metabolism, Gene Knockout Techniques, Humans, K562 Cells, Lymphocyte Activation immunology, Zinc Fingers, Antigens, CD19 immunology, Epitopes immunology, Genetic Engineering, Immunotherapy methods, Receptors, Antigen, T-Cell immunology, Recombinant Proteins immunology, T-Lymphocytes immunology

Abstract

Clinical-grade T cells are genetically modified ex vivo to express a chimeric antigen receptor (CAR) to redirect specificity to a tumor associated antigen (TAA) thereby conferring antitumor activity in vivo. T cells expressing a CD19-specific CAR recognize B-cell malignancies in multiple recipients independent of major histocompatibility complex (MHC) because the specificity domains are cloned from the variable chains of a CD19 monoclonal antibody. We now report a major step toward eliminating the need to generate patient-specific T cells by generating universal allogeneic TAA-specific T cells from one donor that might be administered to multiple recipients. This was achieved by genetically editing CD19-specific CAR(+) T cells to eliminate expression of the endogenous αβ T-cell receptor (TCR) to prevent a graft-versus-host response without compromising CAR-dependent effector functions. Genetically modified T cells were generated using the Sleeping Beauty system to stably introduce the CD19-specific CAR with subsequent permanent deletion of α or β TCR chains with designer zinc finger nucleases. We show that these engineered T cells display the expected property of having redirected specificity for CD19 without responding to TCR stimulation. CAR(+)TCR(neg) T cells of this type may potentially have efficacy as an off-the-shelf therapy for investigational treatment of B-lineage malignancies.

Published

2012