Your search keyword '"Kohn, Donald B."' showing total 65 results

1. Autologous Ex Vivo Lentiviral Gene Therapy for Adenosine Deaminase Deficiency.

Author

Kohn DB, Booth C, Shaw KL, Xu-Bayford J, Garabedian E, Trevisan V, Carbonaro-Sarracino DA, Soni K, Terrazas D, Snell K, Ikeda A, Leon-Rico D, Moore TB, Buckland KF, Shah AJ, Gilmour KC, De Oliveira S, Rivat C, Crooks GM, Izotova N, Tse J, Adams S, Shupien S, Ricketts H, Davila A, Uzowuru C, Icreverzi A, Barman P, Campo Fernandez B, Hollis RP, Coronel M, Yu A, Chun KM, Casas CE, Zhang R, Arduini S, Lynn F, Kudari M, Spezzi A, Zahn M, Heimke R, Labik I, Parrott R, Buckley RH, Reeves L, Cornetta K, Sokolic R, Hershfield M, Schmidt M, Candotti F, Malech HL, Thrasher AJ, and Gaspar HB

Subjects

Adenosine Deaminase deficiency, Adolescent, Child, Child, Preschool, Genetic Therapy adverse effects, Humans, Infant, Lymphocyte Count, Progression-Free Survival, Prospective Studies, Transplantation, Autologous, Agammaglobulinemia therapy, Genetic Therapy methods, Genetic Vectors, Hematopoietic Stem Cell Transplantation, Lentivirus genetics, Severe Combined Immunodeficiency therapy

Abstract

Background: Severe combined immunodeficiency due to adenosine deaminase (ADA) deficiency (ADA-SCID) is a rare and life-threatening primary immunodeficiency., Methods: We treated 50 patients with ADA-SCID (30 in the United States and 20 in the United Kingdom) with an investigational gene therapy composed of autologous CD34+ hematopoietic stem and progenitor cells (HSPCs) transduced ex vivo with a self-inactivating lentiviral vector encoding human ADA . Data from the two U.S. studies (in which fresh and cryopreserved formulations were used) at 24 months of follow-up were analyzed alongside data from the U.K. study (in which a fresh formulation was used) at 36 months of follow-up., Results: Overall survival was 100% in all studies up to 24 and 36 months. Event-free survival (in the absence of reinitiation of enzyme-replacement therapy or rescue allogeneic hematopoietic stem-cell transplantation) was 97% (U.S. studies) and 100% (U.K. study) at 12 months; 97% and 95%, respectively, at 24 months; and 95% (U.K. study) at 36 months. Engraftment of genetically modified HSPCs persisted in 29 of 30 patients in the U.S. studies and in 19 of 20 patients in the U.K. study. Patients had sustained metabolic detoxification and normalization of ADA activity levels. Immune reconstitution was robust, with 90% of the patients in the U.S. studies and 100% of those in the U.K. study discontinuing immunoglobulin-replacement therapy by 24 months and 36 months, respectively. No evidence of monoclonal expansion, leukoproliferative complications, or emergence of replication-competent lentivirus was noted, and no events of autoimmunity or graft-versus-host disease occurred. Most adverse events were of low grade., Conclusions: Treatment of ADA-SCID with ex vivo lentiviral HSPC gene therapy resulted in high overall and event-free survival with sustained ADA expression, metabolic correction, and functional immune reconstitution. (Funded by the National Institutes of Health and others; ClinicalTrials.gov numbers, NCT01852071, NCT02999984, and NCT01380990.)., (Copyright © 2021 Massachusetts Medical Society.)

Published

2021

2. β-Globin Lentiviral Vectors Have Reduced Titers due to Incomplete Vector RNA Genomes and Lowered Virion Production.

Author

Han J, Tam K, Ma F, Tam C, Aleshe B, Wang X, Quintos JP, Morselli M, Pellegrini M, Hollis RP, and Kohn DB

Subjects

Gene Transfer Techniques, Genetic Vectors genetics, HEK293 Cells, Humans, beta-Globins metabolism, tat Gene Products, Human Immunodeficiency Virus genetics, tat Gene Products, Human Immunodeficiency Virus metabolism, Genetic Vectors metabolism, Lentivirus genetics, RNA metabolism, Virion physiology, beta-Globins genetics

Abstract

Lentiviral vectors (LVs) commonly used for the treatment of hemoglobinopathies often have low titers and sub-optimal gene transfer efficiency for human hematopoietic stem and progenitor cells (HSPCs), hindering clinical translation and commercialization for ex vivo gene therapy. We observed that a high percentage of β-globin LV viral genomic RNAs were incomplete toward the 3' end in packaging cells and in released vector particles. The incomplete vector genomes impeded reverse transcription in target cells, limiting stable gene transfer to HSPCs. By combining three modifications to vector design and production (shortening the vector length to 5.3 kb; expressing HIV-1 Tat protein during packaging; and packaging in PKR-/- cells) there was a 30-fold increase in vector titer and a 3-fold increase in vector infectivity in HSPCs. These approaches may improve the manufacturing of β-globin and other complex LVs for enhanced gene delivery and may facilitate clinical applications., (Copyright © 2020 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2021

3. Improved Titer and Gene Transfer by Lentiviral Vectors Using Novel, Small β-Globin Locus Control Region Elements.

Author

Morgan RA, Unti MJ, Aleshe B, Brown D, Osborne KS, Koziol C, Ayoub PG, Smith OB, O'Brien R, Tam C, Miyahira E, Ruiz M, Quintos JP, Senadheera S, Hollis RP, and Kohn DB

Subjects

Animals, Bone Marrow Cells metabolism, Disease Models, Animal, HEK293 Cells, Healthy Volunteers, Hematopoietic Stem Cells metabolism, Humans, Mice, Phenotype, Transfection, Anemia, Sickle Cell therapy, Genetic Therapy methods, Genetic Vectors, Lentivirus genetics, Locus Control Region genetics, Transduction, Genetic methods, beta-Globins genetics

Abstract

β-globin lentiviral vectors (β-LV) have faced challenges in clinical translation for gene therapy of sickle cell disease (SCD) due to low titer and sub-optimal gene transfer to hematopoietic stem and progenitor cells (HSPCs). To overcome the challenge of preserving efficacious expression while increasing vector performance, we used published genomic and epigenomic data available through ENCODE to redefine enhancer element boundaries of the β-globin locus control region (LCR) to construct novel ENCODE core sequences. These novel LCR elements were used to design a β-LV of reduced proviral length, termed CoreGA-AS3-FB, produced at higher titers and possessing superior gene transfer to HSPCs when compared to the full-length parental β-LV at equal MOI. At low vector copy number, vectors containing the ENCODE core sequences were capable of reversing the sickle phenotype in a mouse model of SCD. These studies provide a β-LV that will be beneficial for gene therapy of SCD by significantly reducing the cost of vector production and extending the vector supply., (Copyright © 2019 The American Society of Gene and Cell Therapy. Published by Elsevier Inc. All rights reserved.)

Published

2020

4. Superior lentiviral vectors designed for BSL-0 environment abolish vector mobilization.

Author

Hu P, Bi Y, Ma H, Suwanmanee T, Zeithaml B, Fry NJ, Kohn DB, and Kafri T

Subjects

Animals, Genetic Vectors therapeutic use, Genome, Viral genetics, HIV Infections therapy, HIV Infections virology, HIV-1 genetics, Humans, Mice, RNA, Double-Stranded genetics, RNA, Small Interfering genetics, RNA, Small Interfering therapeutic use, Genetic Vectors genetics, HIV Infections genetics, HIV Long Terminal Repeat genetics, Lentivirus genetics

Abstract

Lentiviral vector mobilization following HIV-1 infection of vector-transduced cells poses biosafety risks to vector-treated patients and their communities. The self-inactivating (SIN) vector design has reduced, however, not abolished mobilization of integrated vector genomes. Furthermore, an earlier study demonstrated the ability of the major product of reverse transcription, a circular SIN HIV-1 vector comprising a single- long terminal repeat (LTR) to support production of high vector titers. Here, we demonstrate that configuring the internal vector expression cassette in opposite orientation to the LTRs abolishes mobilization of SIN vectors. This additional SIN mechanism is in part premised on induction of host PKR response to double-stranded RNAs comprised of mRNAs transcribed from cryptic transcription initiation sites around 3'SIN-LTR's and the vector internal promoter. As anticipated, PKR response following transfection of opposite orientation vectors, negatively affects their titers. Importantly, shRNA-mediated knockdown of PKR rendered titers of SIN HIV-1 vectors comprising opposite orientation expression cassettes comparable to titers of conventional SIN vectors. High-titer vectors carrying an expression cassette in opposite orientation to the LTRs efficiently delivered and maintained high levels of transgene expression in mouse livers. This study establishes opposite orientation expression cassettes as an additional PKR-dependent SIN mechanism that abolishes vector mobilization from integrated and episomal SIN lentiviral vectors.

Published

2018

5. Cytoreductive conditioning intensity predicts clonal diversity in ADA-SCID retroviral gene therapy patients.

Author

Cooper AR, Lill GR, Shaw K, Carbonaro-Sarracino DA, Davila A, Sokolic R, Candotti F, Pellegrini M, and Kohn DB

Subjects

Adaptor Proteins, Signal Transducing genetics, Adenosine Deaminase genetics, Agammaglobulinemia pathology, Child, DNA-Binding Proteins genetics, Genetic Vectors genetics, Humans, LIM Domain Proteins genetics, MDS1 and EVI1 Complex Locus Protein, Proto-Oncogene Proteins genetics, Proto-Oncogenes genetics, Severe Combined Immunodeficiency pathology, T-Lymphocytes cytology, T-Lymphocytes drug effects, T-Lymphocytes metabolism, T-Lymphocytes pathology, Transcription Factors genetics, Adenosine Deaminase deficiency, Agammaglobulinemia genetics, Agammaglobulinemia therapy, Antineoplastic Agents, Alkylating therapeutic use, Busulfan therapeutic use, Gammaretrovirus genetics, Genetic Therapy methods, Genetic Vectors therapeutic use, Severe Combined Immunodeficiency genetics, Severe Combined Immunodeficiency therapy

Abstract

Retroviral gene therapy has proved efficacious for multiple genetic diseases of the hematopoietic system, but roughly half of clinical gene therapy trial protocols using gammaretroviral vectors have reported leukemias in some of the patients treated. In dramatic contrast, 39 adenosine deaminase-deficient severe combined immunodeficiency (ADA-SCID) patients have been treated with 4 distinct gammaretroviral vectors without oncogenic consequence. We investigated clonal dynamics and diversity in a cohort of 15 ADA-SCID children treated with gammaretroviral vectors and found clear evidence of genotoxicity, indicated by numerous common integration sites near proto-oncogenes and by increased abundance of clones with integrations near MECOM and LMO2 These clones showed stable behavior over multiple years and never expanded to the point of dominance or dysplasia. One patient developed a benign clonal dominance that could not be attributed to insertional mutagenesis and instead likely resulted from expansion of a transduced natural killer clone in response to chronic Epstein-Barr virus viremia. Clonal diversity and T-cell repertoire, measured by vector integration site sequencing and T-cell receptor β-chain rearrangement sequencing, correlated significantly with the amount of busulfan preconditioning delivered to patients and to CD34 + cell dose. These data, in combination with results of other ADA-SCID gene therapy trials, suggest that disease background may be a crucial factor in leukemogenic potential of retroviral gene therapy and underscore the importance of cytoreductive conditioning in this type of gene therapy approach.

Published

2017

6. Lentivirus Mediated Correction of Artemis-Deficient Severe Combined Immunodeficiency.

Author

Punwani D, Kawahara M, Yu J, Sanford U, Roy S, Patel K, Carbonaro DA, Karlen AD, Khan S, Cornetta K, Rothe M, Schambach A, Kohn DB, Malech HL, McIvor RS, Puck JM, and Cowan MJ

Subjects

Animals, B-Lymphocytes cytology, B-Lymphocytes metabolism, B-Lymphocytes radiation effects, Cells, Cultured, Combined Modality Therapy, DNA Repair radiation effects, DNA-Binding Proteins, Disease Models, Animal, Endonucleases deficiency, Fibroblasts cytology, Fibroblasts metabolism, Fibroblasts radiation effects, Gamma Rays, Hematopoietic Stem Cell Transplantation, Hematopoietic Stem Cells cytology, Hematopoietic Stem Cells metabolism, Hematopoietic Stem Cells radiation effects, Humans, Mice, Mice, Knockout, Mice, SCID, Nuclear Proteins deficiency, Radiation Tolerance genetics, Severe Combined Immunodeficiency genetics, T-Lymphocytes cytology, T-Lymphocytes metabolism, T-Lymphocytes radiation effects, Endonucleases genetics, Genetic Therapy, Genetic Vectors administration & dosage, Lentivirus genetics, Nuclear Proteins genetics, Severe Combined Immunodeficiency therapy

Abstract

During B and T lymphocyte maturation, V(D)J recombination is initiated by creation of DNA double-strand breaks. Artemis is an exonuclease essential for their subsequent repair by nonhomologous end-joining. Mutations in DCLRE1C, the gene encoding Artemis, cause T - B - NK + severe combined immunodeficiency (ART-SCID) and also confer heightened sensitivity to ionizing radiation and alkylating chemotherapy. Although allogeneic hematopoietic cell transplantation can treat ART-SCID, conditioning regimens are poorly tolerated, leading to early mortality and/or late complications, including short stature, endocrinopathies, and dental aplasia. However, without alkylating chemotherapy as preconditioning, patients usually have graft rejection or limited T cell and no B cell recovery. Thus, addition of normal DCLRE1C cDNA to autologous hematopoietic stem cells is an attractive strategy to treat ART-SCID. We designed a self-inactivating lentivirus vector containing human Artemis cDNA under transcriptional regulation of the human endogenous Artemis promoter (AProArt). Fibroblasts from ART-SCID patients transduced with AProArt lentivirus showed correction of radiosensitivity. Mobilized peripheral blood CD34 + cells from an ART-SCID patient as well as hematopoietic stem cells from Artemis-deficient mice demonstrated restored T and B cell development following AProArt transduction. Murine hematopoietic cells transduced with AProArt exhibited no increase in replating potential in an in vitro immortalization assay, and analysis of AProArt lentivirus insertions showed no predilection for sites that could activate oncogenes. These efficacy and safety findings support institution of a clinical trial of gene addition therapy for ART-SCID., Competing Interests: Author Disclosure No competing financial interests exist.

Published

2017

7. Rescue of splicing-mediated intron loss maximizes expression in lentiviral vectors containing the human ubiquitin C promoter.

Author

Cooper AR, Lill GR, Gschweng EH, and Kohn DB

Subjects

Enhancer Elements, Genetic, Exons, Gene Expression, HEK293 Cells, Humans, K562 Cells, Peptide Elongation Factor 1 genetics, RNA Splicing, Genetic Vectors, Introns, Lentivirus genetics, Promoter Regions, Genetic, Ubiquitin C genetics

Abstract

Lentiviral vectors almost universally use heterologous internal promoters to express transgenes. One of the most commonly used promoter fragments is a 1.2-kb sequence from the human ubiquitin C (UBC) gene, encompassing the promoter, some enhancers, first exon, first intron and a small part of the second exon of UBC. Because splicing can occur after transcription of the vector genome during vector production, we investigated whether the intron within the UBC promoter fragment is faithfully transmitted to target cells. Genetic analysis revealed that more than 80% of proviral forms lack the intron of the UBC promoter. The human elongation factor 1 alpha (EEF1A1) promoter fragment intron was not lost during lentiviral packaging, and this difference between the UBC and EEF1A1 promoter introns was conferred by promoter exonic sequences. UBC promoter intron loss caused a 4-fold reduction in transgene expression. Movement of the expression cassette to the opposite strand prevented intron loss and restored full expression. This increase in expression was mostly due to non-classical enhancer activity within the intron, and movement of putative intronic enhancer sequences to multiple promoter-proximal sites actually repressed expression. Reversal of the UBC promoter also prevented intron loss and restored full expression in bidirectional lentiviral vectors., (© The Author(s) 2014. Published by Oxford University Press on behalf of Nucleic Acids Research.)

Published

2015

8. A modified γ-retrovirus vector for X-linked severe combined immunodeficiency.

Author

Hacein-Bey-Abina S, Pai SY, Gaspar HB, Armant M, Berry CC, Blanche S, Bleesing J, Blondeau J, de Boer H, Buckland KF, Caccavelli L, Cros G, De Oliveira S, Fernández KS, Guo D, Harris CE, Hopkins G, Lehmann LE, Lim A, London WB, van der Loo JC, Malani N, Male F, Malik P, Marinovic MA, McNicol AM, Moshous D, Neven B, Oleastro M, Picard C, Ritz J, Rivat C, Schambach A, Shaw KL, Sherman EA, Silberstein LE, Six E, Touzot F, Tsytsykova A, Xu-Bayford J, Baum C, Bushman FD, Fischer A, Kohn DB, Filipovich AH, Notarangelo LD, Cavazzana M, Williams DA, and Thrasher AJ

Subjects

Animals, Antigens, CD34, DNA, Complementary therapeutic use, Gene Expression, Gene Silencing, Humans, Infant, Interleukin Receptor Common gamma Subunit genetics, Male, Mice, Mutation, T-Lymphocytes immunology, Transduction, Genetic, Transgenes physiology, X-Linked Combined Immunodeficiency Diseases genetics, X-Linked Combined Immunodeficiency Diseases immunology, Gammaretrovirus genetics, Genetic Therapy adverse effects, Genetic Vectors, X-Linked Combined Immunodeficiency Diseases therapy

Abstract

Background: In previous clinical trials involving children with X-linked severe combined immunodeficiency (SCID-X1), a Moloney murine leukemia virus-based γ-retrovirus vector expressing interleukin-2 receptor γ-chain (γc) complementary DNA successfully restored immunity in most patients but resulted in vector-induced leukemia through enhancer-mediated mutagenesis in 25% of patients. We assessed the efficacy and safety of a self-inactivating retrovirus for the treatment of SCID-X1., Methods: We enrolled nine boys with SCID-X1 in parallel trials in Europe and the United States to evaluate treatment with a self-inactivating (SIN) γ-retrovirus vector containing deletions in viral enhancer sequences expressing γc (SIN-γc)., Results: All patients received bone marrow-derived CD34+ cells transduced with the SIN-γc vector, without preparative conditioning. After 12.1 to 38.7 months of follow-up, eight of the nine children were still alive. One patient died from an overwhelming adenoviral infection before reconstitution with genetically modified T cells. Of the remaining eight patients, seven had recovery of peripheral-blood T cells that were functional and led to resolution of infections. The patients remained healthy thereafter. The kinetics of CD3+ T-cell recovery was not significantly different from that observed in previous trials. Assessment of insertion sites in peripheral blood from patients in the current trial as compared with those in previous trials revealed significantly less clustering of insertion sites within LMO2, MECOM, and other lymphoid proto-oncogenes in our patients., Conclusions: This modified γ-retrovirus vector was found to retain efficacy in the treatment of SCID-X1. The long-term effect of this therapy on leukemogenesis remains unknown. (Funded by the National Institutes of Health and others; ClinicalTrials.gov numbers, NCT01410019, NCT01175239, and NCT01129544.).

Published

2014

9. Effects of vector backbone and pseudotype on lentiviral vector-mediated gene transfer: studies in infant ADA-deficient mice and rhesus monkeys.

Author

Carbonaro Sarracino D, Tarantal AF, Lee CC, Martinez M, Jin X, Wang X, Hardee CL, Geiger S, Kahl CA, and Kohn DB

Subjects

Adenosine Deaminase deficiency, Adenosine Deaminase genetics, Animals, Disease Models, Animal, Female, Gene Expression, Gene Order, Genetic Vectors administration & dosage, Genetic Vectors pharmacokinetics, Humans, Macaca mulatta, Mice, Mice, Knockout, Retroviridae genetics, Severe Combined Immunodeficiency genetics, Severe Combined Immunodeficiency therapy, Tissue Distribution, Transgenes, Gene Transfer Techniques, Genetic Vectors genetics, Lentivirus genetics, Transduction, Genetic

Abstract

Systemic delivery of a lentiviral vector carrying a therapeutic gene represents a new treatment for monogenic disease. Previously, we have shown that transfer of the adenosine deaminase (ADA) cDNA in vivo rescues the lethal phenotype and reconstitutes immune function in ADA-deficient mice. In order to translate this approach to ADA-deficient severe combined immune deficiency patients, neonatal ADA-deficient mice and newborn rhesus monkeys were treated with species-matched and mismatched vectors and pseudotypes. We compared gene delivery by the HIV-1-based vector to murine γ-retroviral vectors pseudotyped with vesicular stomatitis virus-glycoprotein or murine retroviral envelopes in ADA-deficient mice. The vesicular stomatitis virus-glycoprotein pseudotyped lentiviral vectors had the highest titer and resulted in the highest vector copy number in multiple tissues, particularly liver and lung. In monkeys, HIV-1 or simian immunodeficiency virus vectors resulted in similar biodistribution in most tissues including bone marrow, spleen, liver, and lung. Simian immunodeficiency virus pseudotyped with the gibbon ape leukemia virus envelope produced 10- to 30-fold lower titers than the vesicular stomatitis virus-glycoprotein pseudotype, but had a similar tissue biodistribution and similar copy number in blood cells. The relative copy numbers achieved in mice and monkeys were similar when adjusted to the administered dose per kg. These results suggest that this approach can be scaled-up to clinical levels for treatment of ADA-deficient severe combined immune deficiency subjects with suboptimal hematopoietic stem cell transplantation options.

Published

2014

10. Envelope, please. And the award goes to….

Author

Kohn DB and Hollis RP

Subjects

Animals, Humans, Betaretrovirus genetics, Genetic Therapy methods, Genetic Vectors genetics, Hematopoietic Stem Cells, Lentivirus genetics, Transduction, Genetic, Viral Envelope Proteins genetics

Published

2014

11. Dissecting the mechanism of histone deacetylase inhibitors to enhance the activity of zinc finger nucleases delivered by integrase-defective lentiviral vectors.

Author

Joglekar AV, Stein L, Ho M, Hoban MD, Hollis RP, and Kohn DB

Subjects

Humans, K562 Cells, Zinc Fingers, Deoxyribonucleases biosynthesis, Deoxyribonucleases genetics, Genetic Vectors, Histone Deacetylase Inhibitors pharmacology, Integrases, Lentivirus, Transduction, Genetic, Viral Proteins

Abstract

Integrase-defective lentiviral vectors (IDLVs) have been of limited success in the delivery of zinc finger nucleases (ZFNs) to human cells, due to low expression. A reason for reduced gene expression has been proposed to involve the epigenetic silencing of vector genomes, carried out primarily by histone deacetylases (HDACs). In this study, we tested valproic acid (VPA), a known HDAC inhibitor (HDACi), for its ability to increase transgene expression from IDLVs, especially in the context of ZFN delivery. Using ZFNs targeting the human adenosine deaminase (ADA) gene in K562 cells, we demonstrated that treatment with VPA enhanced ZFN expression by up to 3-fold, resulting in improved allelic disruption at the ADA locus. Furthermore, three other U.S. Food and Drug Administration-approved HDACis (vorinostat, givinostat, and trichostatin-A) exhibited a similar effect on the activity of ZFN-IDLVs in K562 cells. In primary human CD34(+) cells, VPA- and vorinostat-treated cells showed higher levels of expression of both green fluorescent protein (GFP) as well as ZFNs from IDLVs. A major mechanism for the effects of HDAC inhibitors on improving expression was from their modulation of the cell cycle, and the influence of heterochromatinization was determined to be a lesser contributing factor.

Published

2014

12. Preclinical demonstration of lentiviral vector-mediated correction of immunological and metabolic abnormalities in models of adenosine deaminase deficiency.

Author

Carbonaro DA, Zhang L, Jin X, Montiel-Equihua C, Geiger S, Carmo M, Cooper A, Fairbanks L, Kaufman ML, Sebire NJ, Hollis RP, Blundell MP, Senadheera S, Fu PY, Sahaghian A, Chan RY, Wang X, Cornetta K, Thrasher AJ, Kohn DB, and Gaspar HB

Subjects

Adenosine Deaminase immunology, Adenosine Deaminase metabolism, Agammaglobulinemia genetics, Agammaglobulinemia pathology, Animals, B-Lymphocytes immunology, Cells, Cultured, Disease Models, Animal, Female, HEK293 Cells, HT29 Cells, Humans, Male, Mice, Mice, Inbred C57BL, Promoter Regions, Genetic, Severe Combined Immunodeficiency genetics, Severe Combined Immunodeficiency pathology, T-Lymphocytes immunology, Transduction, Genetic, Virus Integration, Adenosine Deaminase deficiency, Adenosine Deaminase genetics, Agammaglobulinemia immunology, Agammaglobulinemia therapy, Genetic Vectors adverse effects, Lentivirus genetics, Peptide Elongation Factor 1 genetics, Severe Combined Immunodeficiency immunology, Severe Combined Immunodeficiency therapy

Abstract

Gene transfer into autologous hematopoietic stem cells by γ-retroviral vectors (gRV) is an effective treatment for adenosine deaminase (ADA)-deficient severe combined immunodeficiency (SCID). However, current gRV have significant potential for insertional mutagenesis as reported in clinical trials for other primary immunodeficiencies. To improve the efficacy and safety of ADA-SCID gene therapy (GT), we generated a self-inactivating lentiviral vector (LV) with a codon-optimized human cADA gene under the control of the short form elongation factor-1α promoter (LV EFS ADA). In ADA(-/-) mice, LV EFS ADA displayed high-efficiency gene transfer and sufficient ADA expression to rescue ADA(-/-) mice from their lethal phenotype with good thymic and peripheral T- and B-cell reconstitution. Human ADA-deficient CD34(+) cells transduced with 1-5 × 10(7) TU/ml had 1-3 vector copies/cell and expressed 1-2x of normal endogenous levels of ADA, as assayed in vitro and by transplantation into immune-deficient mice. Importantly, in vitro immortalization assays demonstrated that LV EFS ADA had significantly less transformation potential compared to gRV vectors, and vector integration-site analysis by nrLAM-PCR of transduced human cells grown in immune-deficient mice showed no evidence of clonal skewing. These data demonstrated that the LV EFS ADA vector can effectively transfer the human ADA cDNA and promote immune and metabolic recovery, while reducing the potential for vector-mediated insertional mutagenesis.

Published

2014

13. Integrase-defective lentiviral vectors as a delivery platform for targeted modification of adenosine deaminase locus.

Author

Joglekar AV, Hollis RP, Kuftinec G, Senadheera S, Chan R, and Kohn DB

Subjects

Endonucleases genetics, Genetic Loci, Humans, K562 Cells, Lentivirus metabolism, Zinc Fingers, Adenosine Deaminase genetics, Endonucleases metabolism, Genetic Vectors, Integrases genetics, Lentivirus genetics, Transduction, Genetic, Virus Integration

Abstract

We investigated the use of integrase-defective lentiviral vectors (IDLVs) for transient delivery of zinc finger nucleases (ZFNs) and donor templates for site-specific modification of the human adenosine deaminase (hADA) gene. Initially, we constructed IDLVs carrying ZFN monomers (Single-IDLVs) and found them to be able to deliver their gene-editing payload to K562 cells successfully upon cotransduction, with minimal cytotoxicity. To simplify delivery, we designed an IDLV construct to deliver both ZFN monomers from the same vector (Double-IDLV). However, this construct in its original state was prone to rearrangements of the vector genome, resulting in greatly reduced functionality; this was due to recombination between highly similar ZFN monomers arranged in tandem. We modified the Double-IDLV constructs to reduce recombination and restored simultaneous delivery of both ZFNs. We also tested an IDLV construct for delivery of donor templates and demonstrated its efficacy for gene modification. In summary, we highlighted the importance of modifying vector design for co-delivery of highly similar sequences inherent to genome-editing nucleases, and demonstrated significant improvement in the use of IDLVs for delivery of ZFNs and donor templates for genome modification.

Published

2013

14. Gene therapy for adenosine deaminase-deficient severe combined immune deficiency: clinical comparison of retroviral vectors and treatment plans.

Author

Candotti F, Shaw KL, Muul L, Carbonaro D, Sokolic R, Choi C, Schurman SH, Garabedian E, Kesserwan C, Jagadeesh GJ, Fu PY, Gschweng E, Cooper A, Tisdale JF, Weinberg KI, Crooks GM, Kapoor N, Shah A, Abdel-Azim H, Yu XJ, Smogorzewska M, Wayne AS, Rosenblatt HM, Davis CM, Hanson C, Rishi RG, Wang X, Gjertson D, Yang OO, Balamurugan A, Bauer G, Ireland JA, Engel BC, Podsakoff GM, Hershfield MS, Blaese RM, Parkman R, and Kohn DB

Subjects

Adenosine Deaminase deficiency, Adolescent, Antigens, CD34 metabolism, Child, Child, Preschool, Female, Humans, Infant, Male, Retroviridae genetics, Transduction, Genetic, Transplantation Conditioning, Young Adult, Agammaglobulinemia therapy, Bone Marrow Transplantation methods, Genetic Therapy methods, Genetic Vectors, Hematopoietic Stem Cell Transplantation methods, Severe Combined Immunodeficiency therapy

Abstract

We conducted a gene therapy trial in 10 patients with adenosine deaminase (ADA)-deficient severe combined immunodeficiency using 2 slightly different retroviral vectors for the transduction of patients' bone marrow CD34(+) cells. Four subjects were treated without pretransplantation cytoreduction and remained on ADA enzyme-replacement therapy (ERT) throughout the procedure. Only transient (months), low-level (< 0.01%) gene marking was observed in PBMCs of 2 older subjects (15 and 20 years of age), whereas some gene marking of PBMC has persisted for the past 9 years in 2 younger subjects (4 and 6 years). Six additional subjects were treated using the same gene transfer protocol, but after withdrawal of ERT and administration of low-dose busulfan (65-90 mg/m(2)). Three of these remain well, off ERT (5, 4, and 3 years postprocedure), with gene marking in PBMC of 1%-10%, and ADA enzyme expression in PBMC near or in the normal range. Two subjects were restarted on ERT because of poor gene marking and immune recovery, and one had a subsequent allogeneic hematopoietic stem cell transplantation. These studies directly demonstrate the importance of providing nonmyeloablative pretransplantation conditioning to achieve therapeutic benefits with gene therapy for ADA-deficient severe combined immunodeficiency.

Published

2012

15. Challenges in vector and trial design using retroviral vectors for long-term gene correction in hematopoietic stem cell gene therapy.

Author

Corrigan-Curay J, Cohen-Haguenauer O, O'Reilly M, Ross SR, Fan H, Rosenberg N, Somia N, King N, Friedmann T, Dunbar C, Aiuti A, Naldini L, Baum C, von Kalle C, Kiem HP, Montini E, Bushman F, Sorrentino BP, Carrondo M, Malech H, Gahrton G, Shapiro R, Wolff L, Rosenthal E, Jambou R, Zaia J, and Kohn DB

Subjects

Gene Transfer Techniques, Humans, Research Design, Genetic Therapy adverse effects, Genetic Therapy ethics, Genetic Therapy legislation & jurisprudence, Genetic Vectors adverse effects, Genetic Vectors genetics, Hematopoietic Stem Cell Transplantation, Retroviridae genetics

Published

2012

16. Highly efficient large-scale lentiviral vector concentration by tandem tangential flow filtration.

Author

Cooper AR, Patel S, Senadheera S, Plath K, Kohn DB, and Hollis RP

Subjects

Animals, Antigens, CD34 metabolism, Cell Culture Techniques, Cell Line, Tumor, Fibroblasts metabolism, HT29 Cells, Hematopoietic Stem Cells metabolism, Humans, Induced Pluripotent Stem Cells metabolism, Lentivirus genetics, Mice, Transduction, Genetic, Centrifugation, Filtration methods, Genetic Vectors isolation & purification, Lentivirus isolation & purification

Abstract

Large-scale lentiviral vector (LV) concentration can be inefficient and time consuming, often involving multiple rounds of filtration and centrifugation. This report describes a simpler method using two tangential flow filtration (TFF) steps to concentrate liter-scale volumes of LV supernatant, achieving in excess of 2000-fold concentration in less than 3h with very high recovery (>97%). Large volumes of LV supernatant can be produced easily through the use of multi-layer flasks, each having 1720 cm(2) surface area and producing ∼560 mL of supernatant per flask. Combining the use of such flasks and TFF greatly simplifies large-scale production of LV. As a demonstration, the method is used to produce a very high titer LV (>10(10)TU/mL) and transduce primary human CD34+ hematopoietic stem/progenitor cells at high final vector concentrations with no overt toxicity. A complex LV (STEMCCA) for induced pluripotent stem cell (iPSC) generation is also concentrated from low initial titer and used to transduce and reprogram primary human fibroblasts with no overt toxicity. Additionally, a generalized and simple multiplexed real-time PCR assay is described for lentiviral vector titer and copy number determination., (Copyright © 2011 Elsevier B.V. All rights reserved.)

Published

2011

17. Preloading potential of retroviral vectors is packaging cell clone dependent and centrifugation onto CH-296 ensures highest transduction efficiency.

Author

Sondergaard CS, Haldrup C, Beer C, Andersen B, Kohn DB, and Pedersen L

Subjects

Animals, Cell Line, Centrifugation, Chromatography, Affinity, Clone Cells, Humans, Mice, Time Factors, Tissue Culture Techniques, Virion isolation & purification, Fibronectins metabolism, Genetic Vectors genetics, Retroviridae genetics, Transduction, Genetic, Virus Assembly

Abstract

Retroviral vector-mediated gene transfer has been used successfully in clinical gene therapy. Cells of the hematopoietic lineages, however, remain difficult to transduce, although precoating of culture vessels with the fibronectin fragment CH-296 may improve transduction efficiency. Alternatively, low-speed centrifugation of vector-containing supernatant onto culture vessels may improve transduction efficiency in the absence of CH-296 preloading. Using the NIH/3T3-derived Moloney murine leukemia virus-based packaging cell lines PG13, PA317, and PT67, we here show that preloading by low-speed centrifugation improves transduction efficiency in a packaging cell subclone-dependent manner. Preloading by centrifugation, however, cannot generally replace CH-296 and we obtained the overall highest transduction levels when combining centrifugation and CH-296 precoating. We found, moreover, that the factor responsible for high susceptibility to preloading in our PG13-derived vector supernatant was transferable to a PA317-derived vector supernatant with low susceptibility to preloading. Furthermore, our PA317, PG13, and PT67 subclones shed into their supernatants variable amounts of fibronectin. This soluble fibronectin formed aggregates of various sizes and generated complexes with vector particles. The fibronectin-vector complexes readily sedimented onto culture vessels and copurified after fibronectin-specific affinity purification of vector-containing supernatants. Finally, vector supernatant from 293T cells, which barely produce fibronectin, was not susceptible to preloading. The susceptibility to preloading by centrifugation thus appears to be dependent both on the specific packaging cell line and on the association of vector particles and packaging cell-produced fibronectin. Rigorous screening of individual vector-containing supernatants is therefore required to identify optimal transduction conditions for retroviral gene transfer.

Published

2009

18. In vivo biosafety model to assess the risk of adverse events from retroviral and lentiviral vectors.

Author

Bauer G, Dao MA, Case SS, Meyerrose T, Wirthlin L, Zhou P, Wang X, Herrbrich P, Arevalo J, Csik S, Skelton DC, Walker J, Pepper K, Kohn DB, and Nolta JA

Subjects

Animals, Biological Assay, Cells, Cultured, Hematopoietic Stem Cell Transplantation, Hematopoietic Stem Cells virology, Mesenchymal Stem Cell Transplantation, Mesenchymal Stem Cells virology, Mice, Mice, Inbred Strains, Models, Animal, Risk, Genetic Therapy adverse effects, Genetic Vectors adverse effects, Lentivirus, Moloney murine leukemia virus, Retroviridae, Transduction, Genetic

Abstract

Serious adverse events in some human gene therapy clinical trials have raised safety concerns when retroviral or lentiviral vectors are used for gene transfer. We evaluated the potential for generating replication-competent retrovirus (RCR) and assessed the risk of occurrence of adverse events in an in vivo system. Human hematopoietic stem and progenitor cells (HSCs) and mesenchymal stem cells (MSCs) transduced with two different Moloney murine leukemia virus (MoMuLV)-based vectors were cotransplanted into a total of 481 immune-deficient mice (that are unable to reject cells that become transformed), and the animals were monitored for 18 months. Animals with any signs of illness were immediately killed, autopsied, and subjected to a range of biosafety studies. There was no detectable evidence of insertional mutagenesis leading to human leukemias or solid tumors in the 18 months during which the animals were studied. In 117 serum samples analyzed by vector rescue assay there was no detectable RCR. An additional 149 mice received HSCs transduced with lentiviral vectors, and were followed for 2-6 months. No vector-associated adverse events were observed, and none of the mice had detectable human immunodeficiency virus (HIV) p24 antigen in their sera. Our in vivo system, therefore, helps to provide an assessment of the risks involved when retroviral or lentiviral vectors are considered for use in clinical gene therapy applications.

Published

2008

19. Foamy virus vectors expressing anti-HIV transgenes efficiently block HIV-1 replication.

Author

Taylor JA, Vojtech L, Bahner I, Kohn DB, Laer DV, Russell DW, and Richard RE

Subjects

Cell Line, Cells, Cultured, Gene Products, rev biosynthesis, Gene Products, rev genetics, Gene Transfer Techniques, Genetic Therapy, HIV Envelope Protein gp41 biosynthesis, HIV Envelope Protein gp41 genetics, HIV Infections genetics, HIV Infections virology, Humans, Anti-HIV Agents chemical synthesis, Gene Expression Regulation, Viral, Genetic Vectors therapeutic use, HIV Infections prevention & control, HIV-1 genetics, Spumavirus genetics, Transgenes, Virus Replication genetics

Abstract

Gene therapy has the potential to control human immunodeficiency virus (HIV) in patients who do not respond to traditional antiviral therapy. In this study, we tested foamy virus (FV) vectors expressing three anti-HIV transgenes, both individually and in a combination vector. The transgenes tested in this study are RevM10, a dominant negative version of the viral rev protein, Sh1, a short hairpin RNA directed against a conserved overlapping sequence of tat and rev, and membrane-associated C46 (maC46), a membrane-attached peptide that blocks HIV cell entry. FV vectors efficiently transduce hematopoietic stem cells and, unlike lentivirus (LV) vectors, do not share viral proteins with HIV. The titers of the FV vectors described in this study were not affected by anti-HIV transgenes. On a direct comparison of FV vectors expressing the individual transgenes, entry inhibition using the maC46 transgene was found to be the most effective at blocking HIV replication. A clinically relevant FV vector expressing three anti-HIV transgenes effectively blocked HIV infection in primary macrophages derived from transduced, peripheral blood CD34-selected cells and in a cell line used for propagating HIV, CEMx174. These results suggest that there are potential benefits of using FV vectors in HIV gene therapy.

Published

2008

20. Lentiviral vectors ready for prime-time.

Author

Kohn DB

Subjects

Adult, Gene Transfer Techniques, HIV-1 genetics, HIV-1 immunology, HIV-1 metabolism, Humans, Middle Aged, Viral Envelope Proteins genetics, Viral Envelope Proteins metabolism, Genetic Vectors genetics, Lentivirus physiology, Transfection methods, Virus Replication genetics

Published

2007

21. In vivo transduction by intravenous injection of a lentiviral vector expressing human ADA into neonatal ADA gene knockout mice: a novel form of enzyme replacement therapy for ADA deficiency.

Author

Carbonaro DA, Jin X, Petersen D, Wang X, Dorey F, Kil KS, Aldrich M, Blackburn MR, Kellems RE, and Kohn DB

Subjects

Adenosine Deaminase metabolism, Animals, Animals, Newborn, Disease Models, Animal, Female, Genetic Therapy methods, Genetic Vectors pharmacokinetics, Germ Cells physiology, Humans, Injections, Intravenous, Male, Mice, Mice, Knockout, Severe Combined Immunodeficiency immunology, Tissue Distribution, Transduction, Genetic, Adenosine Deaminase deficiency, Adenosine Deaminase genetics, Genetic Vectors administration & dosage, HIV-1 genetics, Severe Combined Immunodeficiency therapy

Abstract

Using a mouse model of adenosine deaminase-deficient severe combined immune deficiency syndrome (ADA-deficient SCID), we have developed a noninvasive method of gene transfer for the sustained systemic expression of human ADA as enzyme replacement therapy. The method of delivery is a human immunodeficiency virus 1-based lentiviral vector given systemically by intravenous injection on day 1 to 2 of life. In this article we characterize the biodistribution of the integrated vector, the expression levels of ADA enzyme activity in various tissues, as well as the efficacy of systemic ADA expression to correct the ADA-deficient phenotype in this mouse model. The long-term expression of enzymatically active ADA achieved by this method, primarily from transduction of liver and lung, restored immunologic function and significantly extended survival. These studies illustrate the potential for sustained in vivo production of enzymatically active ADA, as an alternative to therapy by frequent injection of exogenous ADA protein.

Published

2006

22. Transient gene expression by nonintegrating lentiviral vectors.

Author

Nightingale SJ, Hollis RP, Pepper KA, Petersen D, Yu XJ, Yang C, Bahner I, and Kohn DB

Subjects

Antigens, CD34 metabolism, Base Sequence, Cells, Cultured, Drug Resistance, Genetic Therapy methods, Green Fluorescent Proteins genetics, HIV-1 genetics, HT29 Cells, Hematopoietic Stem Cells metabolism, Humans, Jurkat Cells, Kanamycin Kinase genetics, Molecular Sequence Data, Neomycin pharmacology, Gene Expression Regulation, Genetic Vectors genetics, Lentivirus genetics, Virus Integration

Abstract

Nonintegrating lentiviral (NIL) vectors were produced from HIV-1-based lentiviral vectors by introducing combinations of mutations made to disable the integrase protein itself and to alter the integrase recognition sequences (att) in the viral LTR. NIL vectors with these novel combinations of mutations were used to transduce the human T lymphoid cell line Jurkat and primary human CD34(+) hematopoietic progenitor cells to assess their efficacy measured through transient expression of the enhanced green fluorescent protein (eGFP) reporter gene. The most disabled NIL vectors resulted in initial high levels of eGFP expression (approximately 90% of cells), but expression was transient, diminishing toward background (<0.5%) within less than 1 month. Southern blot analyses of transduced Jurkat cells confirmed the loss of detectable NIL vector sequence (linear form and one- and two-LTR circles) by 1 month. There were low residual levels of integration by NIL vectors (reduced approximately 10(4)-fold compared to wild-type vectors), despite any combination of the engineered changes. Based upon analysis of the sequences of the DNA from the junctions of the vector LTR and cellular chromosomes, these rare integrated NIL vector sequences were not mediated by an integrase-driven mechanism due to reversion of the engineered mutations, but more likely were produced by background recombination events. The development of NIL vectors provides a novel tool for efficient transient gene expression in primary stem cells and hematopoietic and lymphoid cells.

Published

2006

23. Effects of busulfan dose escalation on engraftment of infant rhesus monkey hematopoietic stem cells after gene marking by a lentiviral vector.

Author

Kahl CA, Tarantal AF, Lee CI, Jimenez DF, Choi C, Pepper K, Petersen D, Fletcher MD, Leapley AC, Fisher J, Burns TS, Ultsch MN, Dorey FJ, and Kohn DB

Subjects

Animals, Area Under Curve, Base Sequence, Busulfan pharmacokinetics, Cell Line, DNA Primers, Dose-Response Relationship, Drug, Humans, Macaca mulatta, Busulfan pharmacology, Genetic Markers, Genetic Vectors, Lentivirus genetics

Abstract

Objective: Non-myeloablative cytoreduction is used in clinical hematopoietic stem cell gene therapy trials to increase engraftment of gene-modified cells. We utilized an infant rhesus monkey model to identify an optimal dosage of busulfan that results in efficient long-term gene marking with minimal toxicities., Methods: Bone marrow (BM) was harvested, followed by a single 2-hour intravenous infusion of busulfan at escalating dosages of 0 to 160 mg/m(2). CD34(+) cells were immunoselected from BM, transduced overnight with a simian immunodeficiency virus-based lentiviral vector carrying a non-expressed marker gene, and injected intravenously 48 hours post-busulfan administration. Pharmacokinetics were assessed, as well as adverse effects and peripheral blood and BM gene marking., Results: Increasing dosages of busulfan resulted in increased area-under-the-curve (AUC) with some variability at each dosage level, suggesting interindividual variation in clearance. Blood chemistries were normal and no adverse effects were observed as a result of busulfan infusion. At 120 and 160 mg/m(2), transient neutropenia and thrombocytopenia were noted but not lymphopenia. Over the 6 months of study posttransplantation, a busulfan dosage-related increase in gene marking was observed ranging from undetectable (no busulfan) up to 0.1% gene-containing cells in animals achieving the highest busulfan AUC. This corresponds to a more than 100-fold increase in gene marking over the busulfan dosage range studied., Conclusions: These data indicate that increased gene marking of hematopoietic stem cells can be achieved by escalating busulfan dosages from 40 to 160 mg/m(2) without significant toxicity in infant nonhuman primates.

Published

2006

24. Specific and stable gene transfer to human embryonic stem cells using pseudotyped lentiviral vectors.

Author

Jang JE, Shaw K, Yu XJ, Petersen D, Pepper K, Lutzko C, and Kohn DB

Subjects

Amino Acid Transport System ASC genetics, Animals, Cell Line, Glycoproteins genetics, Green Fluorescent Proteins metabolism, Humans, Mice, Minor Histocompatibility Antigens, Cell Differentiation genetics, Gene Transfer Techniques, Genetic Vectors, Hematopoietic Stem Cells metabolism, Lentivirus genetics

Abstract

Genetic modification of human embryonic stem cells (hESCs) is an important tool for understanding and influencing their biologic properties. At the present time, lentiviral vectors pseudotyped with the vesicular stomatitis virus G protein (VSV-G) have been most effective for stable gene transfer to hESCs. However, they also efficiently transduce murine embryonic fibroblasts (MEF), used to support the undifferentiated state of many commonly used hESC lines. Transduction of both the MEF as well as hESCs complicates analyses of gene transfer and expression. We made lentiviral vectors pseudotyped with envelope glycoproteins from retroviruses that have been shown to have more restricted transduction ranges and evaluated their specificity. Lentiviral vectors pseudotyped by the envelopes from either the gibbon ape leukemia virus (GALV) or the RD114 feline endogenous virus (RD114) specifically transduced hESCs to similar extents as VSV-G pseudotyped vectors, but did not transduce MEF. In addition, gene modfication by these pseudotyped lentiviral vectors was stably maintained throughout differentiation of hESCs in vitro. These pseudotyped lentiviral vectors may be valuable tools for efficient, specific and stable gene modification of hESCs.

Published

2006

25. Neonatal gene therapy of MPS I mice by intravenous injection of a lentiviral vector.

Author

Kobayashi H, Carbonaro D, Pepper K, Petersen D, Ge S, Jackson H, Shimada H, Moats R, and Kohn DB

Subjects

Aging physiology, Animals, Animals, Newborn, Bone and Bones abnormalities, Bone and Bones metabolism, Cell Line, Tumor, Central Nervous System metabolism, DNA, Complementary genetics, Gene Expression, Genetic Vectors administration & dosage, Glycosaminoglycans chemistry, Glycosaminoglycans metabolism, Humans, Iduronidase deficiency, Iduronidase genetics, Iduronidase metabolism, Injections, Intravenous, Lysosomes genetics, Lysosomes metabolism, Mice, Mice, Knockout, Mucopolysaccharidosis I enzymology, Neurons metabolism, Sulfur chemistry, Survival Rate, Genetic Therapy, Genetic Vectors genetics, Lentivirus genetics, Mucopolysaccharidosis I genetics, Mucopolysaccharidosis I therapy

Abstract

Mucopolysaccharidosis type I (MPS I) is a lysosomal glycosaminoglycan (GAG) storage disorder caused by deficiency of alpha-l-iduronidase (IDUA). In this study, we evaluated the potential to perform gene therapy for MPS I by direct in vivo injection of a lentiviral vector, using an IDUA gene knockout murine model. We compared the efficacy in newborn versus young adult MPS I mice of a single intravenous injection of the lentiviral vector. The extent of transduction was dose-dependent, with the liver receiving the highest level of vector, but other somatic organs reaching almost the same level. The phenotypic manifestations of disease were partially improved in the mice treated as young adults, but were nearly normalized at every end-point measured in the mice treated as neonates. In the neonatally treated mice, the expressed IDUA activity resulted in decreased GAG storage, prevention of skeletal abnormalities, a more normal gross appearance, and improved survival. Most strikingly, significant levels of IDUA enzyme were produced in the brain of mice treated as neonates, with transduction of neurons at high levels. The sustained expression of enzymatically active IDUA in multiple organs had a significant beneficial effect on the phenotypic abnormalities of MPS I, which may be translated to clinical gene therapy of patients with Hurler disease.

Published

2005

26. Factors influencing the titer and infectivity of lentiviral vectors.

Author

Logan AC, Nightingale SJ, Haas DL, Cho GJ, Pepper KA, and Kohn DB

Subjects

Antigens, CD34 biosynthesis, Cell Line, Gene Products, gag metabolism, Green Fluorescent Proteins metabolism, HIV-1 metabolism, Humans, Immunoassay, Membrane Glycoproteins chemistry, Models, Genetic, Plasmids metabolism, Promoter Regions, Genetic, Stem Cells cytology, Time Factors, Transfection, Transgenes, Ultracentrifugation, Viral Envelope Proteins chemistry, Gene Transfer Techniques, Genetic Vectors, Lentivirus genetics

Abstract

Lentiviral vectors have undergone several generations of design improvement to enhance their biosafety and expression characteristics, and have been approved for use in human clinical studies. Most preclinical studies with these vectors have employed easily assayed marker genes for the purpose of determining vector titers and transduction efficiencies. Naturally, the adaptation of these vector systems to clinical use will increasingly involve the transfer of genes whose products may not be easily measured, meaning that the determination of vector titer will be more complicated. One method for determining vector titer that can be universally employed on all human immunodeficiency virus type 1-based lentiviral vector supernatants involves the measurement of Gag (p24) protein concentration in vector supernatants by immunoassay. We have studied the effects that manipulation of several variables involved in vector design and production by transient transfection have on vector titer and infectivity. We have determined that manipulation of the amount of transfer vector, packaging, and envelope plasmids used to transfect the packaging cells does not alter vector infectivity, but does influence vector titer. We also found that modifications to the transfer vector construct, such as replacing the internal promoter or transgene, do not generally alter vector infectivity, whereas inclusion of the central polypurine tract in the transfer vector increases vector infectivity on HEK293 cells and human umbilical cord blood CD34+ hematopoietic progenitor cells (HPCs). The infectivities of vector supernatants can also be increased by harvesting at early time points after the initiation of vector production, collection in serum-free medium, and concentration by ultracentrifugation. For the transduction of CD34+ HPCs, we found that the simplest method of increasing vector infectivity is to pseudotype vector particles with the RD114 envelope instead of vesicular stomatitis virus G glycoprotein (VSV-G).

Published

2004

27. Integrated self-inactivating lentiviral vectors produce full-length genomic transcripts competent for encapsidation and integration.

Author

Logan AC, Haas DL, Kafri T, and Kohn DB

Subjects

Base Sequence, Cell Line, HIV-1 genetics, Humans, Molecular Sequence Data, Promoter Regions, Genetic, Transduction, Genetic, Virus Assembly, Genetic Vectors, Genome, Viral, HIV Long Terminal Repeat genetics, HIV-1 metabolism, Transcription, Genetic, Virus Integration

Abstract

To make human immunodeficiency virus type 1 (HIV-1)-based vectors safer for use in the research and clinical setting, a significant modification to the HIV-1 genome has been the deletion of promoter and enhancer elements from the U3 region of the long terminal repeat (LTR). Vectors containing this deletion are thought to have no LTR-directed transcription and are called self-inactivating (SIN) lentivectors. Using four distinct approaches, we show that SIN lentivectors continue to have promoter activity near the 5' LTR, which is responsible for the production of full-length vector transcripts. To verify that transcripts derived from the LTR in SIN lentivectors are competent for encapsidation and integration, we transduced a lentiviral packaging cell line with a SIN lentivector and then observed the production of viable vector particles containing full-length SIN lentivector genomes. We have also attempted to identify sequences in the SIN lentivector which are responsible for transcriptional activation at the 5' LTR. Using different segments of the vector LTR and leader region in a promoter assay, we have determined that the residual promoter activity is contained entirely within the leader region and that, although this element is downstream of the transcription initiation site, it is capable of initiating transcription from the 5' end of R in the LTR. Mutation of leader region binding sites for the transcriptional activators downstream binding factor 1 (DBF1) and SP1 reduces transcription from the SIN LTR by up to 80%. Knowledge of the potential for mobilization of HIV-1-derived SIN lentivectors will be important for the design of future gene therapy trials with such vectors.

Published

2004

28. Use of lentiviral vectors to induce long-term tolerance to gal(+) heart grafts.

Author

Kearns-Jonker M, Fischer-Lougheed J, Shulkin I, Kleihauer A, Mitsuhashi N, Kohn DB, Weinberg K, D'Apice AJ, Starnes VA, and Cramer DV

Subjects

Animals, Antibodies analysis, Antibodies, Heterophile analysis, B-Lymphocytes immunology, Bone Marrow metabolism, Bone Marrow Transplantation, Disaccharides metabolism, Graft Rejection, Graft Survival, Mice, Mice, Inbred C57BL, Mice, Knockout, Recombinant Fusion Proteins metabolism, Spleen immunology, Spleen pathology, Swine, Transplantation Chimera immunology, Transplantation, Heterotopic, Galactosyltransferases genetics, Genetic Vectors, Heart Transplantation immunology, Lentivirus genetics, Transduction, Genetic, Transplantation Tolerance

Abstract

Background: Tolerance to organ grafts has been achieved by establishing a state of stable mixed-cell chimerism after bone marrow transplantation. Gene therapy has been applied to establish chimerism for cells expressing galactose alpha 1,3 galactose in alpha 1,3 galactosyltransferase deficient (gal knockout) mice using retroviral vectors. Limitations to the success of this methodology include short-term expression of the introduced gene and rejection of gal hearts transplanted into these animals within a month., Methods: Autologous bone marrow from gal knockout mice was transduced with a lentiviral vector expressing porcine alpha 1,3 galactosyltransferase and transplanted into lethally irradiated gal knockout mice. Chimerism was monitored by flow cytometry. Hearts from wild type mice (gal/) were transplanted into these animals and palpated daily. Xenoantibodies directed at the gal carbohydrate or porcine xenoantigens were detected by enzyme-linked immunosorbent assay., Results: Hearts from wild-type gal/ donors were permanently accepted in all mice receiving autologous, transduced bone marrow before heart transplantation. Control mice rejected gal hearts within 12 to 14 days. Histologic analysis demonstrated classical signs of rejection in controls and normal myocardium with no evidence of rejection in mice chimeric for the gal carbohydrate. Anti-gal xenoantibodies were not produced in gal chimeras, but normal antibody responses to other xenoantigens were detected. Specific tolerance for the gal carbohydrate was achieved by this procedure., Conclusions: These experiments report the first demonstration of permanent survival of gal hearts after transplantation with autologous, transduced bone marrow. Transduction with lentiviral vectors results in long-term, stable chimerism at levels sufficient to induce long-term tolerance to heart grafts in mice.

Published

2004

29. Morphological analysis and lentiviral transduction of fetal monkey bone marrow-derived mesenchymal stem cells.

Author

Lee CI, Kohn DB, Ekert JE, and Tarantal AF

Subjects

Animals, Bone Marrow Cells cytology, Cell Cycle, Cell Division, Fetus cytology, Flow Cytometry, Gene Expression, Green Fluorescent Proteins, HIV-1 genetics, Immunochemistry, Luminescent Proteins genetics, Luminescent Proteins metabolism, Mesenchymal Stem Cells metabolism, Mesenchymal Stem Cells ultrastructure, Osteogenesis, Promoter Regions, Genetic, Vimentin genetics, Vimentin metabolism, Genetic Vectors, Lentivirus genetics, Macaca mulatta embryology, Mesenchymal Stem Cells cytology, Transduction, Genetic

Abstract

We explored the transduction kinetics of HIV-1-derived lentiviral vectors containing the CMV, EF1alpha, or PGK promoter expressing EGFP in fetal rhesus monkey bone marrow-derived mesenchymal stem cells (rhMSC). Studies included the effects of transduction (MOI 0-100) on growth, cell cycle, and differentiation toward an osteogenic lineage. Flow cytometric analysis indicated an approximate 8- to 10-fold greater quantity of EGFP-expressing rhMSC when cells were transduced with the CMV or EF1alpha promoter compared to PGK, although quantitative PCR revealed no differences at the DNA level. The CMV promoter initially expressed 10- to 100-fold higher levels of EGFP compared to EF1alpha or PGK, respectively, at increasing MOI, although a significant decline in transgene expression was observed posttransduction and with advancing passage (P < 0.01), whereas a significant increase in the level of expression was observed over time with the EF1alpha promoter. At an MOI of 100, a transient arrest at the S phase of the cell cycle was observed for both vector constructs. Transduced rhMSC differentiated toward an osteogenic lineage comparable to untransduced rhMSC and showed equivalent levels of alkaline phosphatase activity. These findings suggest that the SIN HIV-1-derived lentiviral vectors used in these studies can efficiently transduce rhMSC in vitro (CMV > EF1alpha > PGK) without inhibiting differentiation potential, although the cell cycle was transiently altered at high MOI

Published

2004

30. Scaffold attachment region-containing retrovirus vectors improve long-term proviral expression after transplantation of GFP-modified CD34+ baboon repopulating cells.

Author

Kurre P, Morris J, Thomasson B, Kohn DB, and Kiem HP

Subjects

Animals, Gene Expression, Graft Survival, Green Fluorescent Proteins, Hematopoietic Stem Cells cytology, Hematopoietic Stem Cells metabolism, Kinetics, Luminescent Proteins genetics, Papio, Proviruses genetics, Proviruses growth & development, Retroviridae genetics, Time Factors, Transduction, Genetic standards, Genetic Vectors, Hematopoietic Stem Cell Transplantation, Matrix Attachment Regions genetics, Proviruses metabolism, Transduction, Genetic methods

Abstract

Sustained high-level proviral expression is important for clinical applications of gene therapy. Genetic elements including the beta-interferon scaffold attachment region (SAR) have been shown to improve transgene expression in hematopoietic cells. We hypothesized that SAR elements might improve expression and allow the preselection of successfully transduced cells. Thus, we transplanted green fluorescent protein (GFP)-selected cells, half of which had been transduced with either SAR or non-SAR-containing retrovirus vectors, into 3 animals. All animals showed delayed engraftment compared with historic controls (28 vs 15.5 days). GFP marking was seen at levels up to 8% but declined over the first 6 weeks. Importantly, fluorescence intensity was 2- to 9-fold increased in progeny of SAR versus non-SAR vector-modified cells in all hematopoietic lineages for the duration of follow-up (6-12 months). In conclusion, the use of SAR-containing vectors improved transgene expression in hematopoietic repopulating cells, which may obviate the need for multicopy integration to achieve high-level expression and reduce the risk for insertional mutagenesis.

Published

2003

31. Lentivirus vectors incorporating the immunoglobulin heavy chain enhancer and matrix attachment regions provide position-independent expression in B lymphocytes.

Author

Lutzko C, Senadheera D, Skelton D, Petersen D, and Kohn DB

Subjects

Animals, B-Lymphocytes cytology, Base Sequence, Cell Differentiation, Cell Line, Cytomegalovirus genetics, DNA Primers, Flow Cytometry, Green Fluorescent Proteins, Humans, Luminescent Proteins genetics, Mice, Promoter Regions, Genetic, Transgenes, B-Lymphocytes metabolism, Enhancer Elements, Genetic, Genetic Vectors, Immunoglobulin Heavy Chains genetics, Lentivirus genetics, Matrix Attachment Region Binding Proteins genetics

Abstract

In the present studies we developed lentivirus vectors with regulated, consistent transgene expression in B lymphocytes by incorporating the immunoglobulin heavy chain enhancer (E micro ) with and without associated matrix attachment regions (E micro MAR) into lentivirus vectors. Incorporation of these fragments upstream of phosphoglycerate kinase (PGK) or cytomegalovirus promoters resulted in a two- to threefold increase in enhanced green fluorescent protein (EGFP) mean fluorescence intensity (MFI) in B-lymphoid but not T-lymphoid, myeloid, fibroblast, or carcinoma cell lines. A 1-log increase in EGFP expression was observed in B-lymphoid cells (but not myeloid cells) differentiated from human CD34(+) progenitors in vitro transduced with E micro - and E micro MAR-containing lentivectors. Lastly, we evaluated the expression from the E micro MAR element in mice 2 to 24 weeks posttransplant with transduced hematopoietic stem cells. In mice receiving vectors with the E micro and E micro MAR elements upstream of the PGK promoter, there was a 2- to 10-fold increase in EGFP expression in B cells (but not other cell types). Evaluation of the coefficient of variation of expression among different cell types demonstrated that consistent, position-independent transgene expression was observed exclusively in B cells transduced with the E micro MAR-containing vector and not other cells types or vectors. Proviral genomes with the E micro MAR element had increased chromatin accessibility, which likely contributed to the position independence of expression in B lymphocytes. In summary, incorporation of the E micro MAR element in lentivirus vectors resulted in enhanced, position-independent expression in primary B lymphocytes. These vectors provide a useful tool for the study of B-lymphocyte biology and the development of gene therapy for disorders affecting B lymphocytes, such as immune deficiencies.

Published

2003

32. Expression from second-generation feline immunodeficiency virus vectors is impaired in human hematopoietic cells.

Author

Price MA, Case SS, Carbonaro DA, Yu XJ, Petersen D, Sabo KM, Curran MA, Engel BC, Margarian H, Abkowitz JL, Nolan GP, Kohn DB, and Crooks GM

Subjects

Antigens, CD34 biosynthesis, Blotting, Northern, Bone Marrow Cells cytology, Cytomegalovirus genetics, Fetal Blood metabolism, Genetic Therapy methods, Green Fluorescent Proteins, HIV-1 genetics, Humans, Lentivirus genetics, Luminescent Proteins metabolism, Phosphoglycerate Kinase genetics, RNA metabolism, Time Factors, Transgenes, Gene Transfer Techniques, Genetic Vectors, Hematopoietic Stem Cells metabolism, Immunodeficiency Virus, Feline genetics

Abstract

Vectors based on the feline immunodeficiency virus (FIV) have been developed as an alternative to those based on another lentivirus, human immunodeficiency virus-1 (HIV-1), because of theoretical safety advantages. We compared the efficiency of gene transfer and expression in human and feline hematopoietic progenitors using second-generation HIV-1 and FIV-based vectors. Vector pairs were tested using either human cytomegalovirus or murine phospho-glycerate kinase (PGK) internal promoters and were pseudotyped with the vesicular stomatitis virus G protein (VSV-G). Vector proviral copy numbers were similar in human and feline hematopoietic primary cells and cell lines transduced by HIV-1 or FIV vectors, demonstrating that both vectors are able to transfer genes efficiently to these cell types. HIV-1 vectors were well expressed in human primary hematopoietic cells and cell lines. However, transgene expression from FIV vectors was almost undetectable in human hematopoietic cells. In contrast, the FIV vector was expressed well in primary hematopoietic feline cells and human non-hematopoietic cells, demonstrating that low transgene expression from the FIV vector is a phenomenon specific to human hematopoietic cells. Northern blot analysis demonstrated decreased vector transcript levels in human CEM cells transduced with FIV relative to cells transduced with HIV-1, despite high vector copy numbers. No evidence of vector transcript instability was seen in studies of transduced CEM cells treated with actinomycin D. We conclude that FIV vectors can transfer genes into human hematopoietic cells as effectively as HIV-1 vectors, but that unknown elements in the current FIV backbone inhibit expression from FIV vectors in human hematopoietic cells.

Published

2002

33. Advances in lentiviral vector design for gene-modification of hematopoietic stem cells.

Author

Logan AC, Lutzko C, and Kohn DB

Subjects

Animals, Cell Cycle genetics, DNA, Recombinant genetics, DNA, Recombinant therapeutic use, Genetic Therapy methods, Genetic Vectors isolation & purification, Genetic Vectors therapeutic use, Hematopoietic Stem Cells virology, Humans, Mice, Recombination, Genetic, Safety, Gene Expression Regulation, Viral, Genetic Vectors genetics, Genome, Viral, Hematopoietic Stem Cells physiology, Lentivirus genetics, Transduction, Genetic methods

Abstract

Lentiviral vectors are more efficient at transducing quiescent hematopoietic stem cells than murine retroviral vectors. This characteristic is due to multiple karyophilic components of the lentiviral vector pre-integration complex. Lentiviral vectors are also able to carry more complex payloads than murine retroviral vectors, making it possible to deliver expression cassettes that direct either constitutive or targeted expression in various hematopoietic stem cell progeny.

Published

2002

34. Kinetics of fluorescence expression in nonhuman primates transplanted with GFP retrovirus-modified CD34 cells.

Author

Kurre P, Morris J, Andrews RG, Kohn DB, and Kiem HP

Subjects

Animals, Flow Cytometry, Green Fluorescent Proteins, Kinetics, Moloney murine leukemia virus genetics, Papio, Promoter Regions, Genetic, Gene Expression, Genetic Vectors, Luminescent Proteins metabolism, Retroviridae genetics

Abstract

Downregulation and loss of proviral expression have been demonstrated to occur in a variety of in vitro studies and in mouse models. Here we evaluated the kinetics of proviral expression after transplantation in a competitive repopulating model in the baboon. Transgene persistence and green fluorescent protein (GFP) expression in peripheral blood leukocytes (PBL) were analyzed in four animals by semiquantitative PCR and flow cytometry for up to 80 weeks (range 17-80). All animals were transplanted with cells transduced with EGFP or EYFP reporters driven by Moloney murine leukemia virus (MoMuLV) or a modified promoter/enhancer, (MND) respectively. Simultaneous dual-color analysis of fluorescence levels in granulocyte and lymphocyte subsets following hematopoietic reconstitution demonstrated progressive loss of fluorescence intensity occurring predominantly early after transplant in cells transduced with both retrovirus backbones and at serial time points. In addition, we carried out PCR analysis of DNA extracted from sorted EGFP(-)/EYFP(-) cells and confirmed the presence of cells genetically marked by either vector in this population, indicating the persistence of cells that have downregulated or lost retroviral gene expression. In comparison to mouse studies, however, we did not detect substantial differences between MND and MoMuLV backbones.

Published

2002

35. Supramolecular nanosubstrate–mediated delivery system enables CRISPR-Cas9 knockin of hemoglobin beta gene for hemoglobinopathies

Author

Yang, Peng, Chou, Shih-Jie, Li, Jindian, Hui, Wenqiao, Liu, Wenfei, Sun, Na, Zhang, Ryan Y, Zhu, Yazhen, Tsai, Ming-Long, Lai, Henkie I, Smalley, Matthew, Zhang, Xinyue, Chen, Jiayuan, Romero, Zulema, Liu, Dahai, Ke, Zunfu, Zou, Chang, Lee, Chin-Fa, Jonas, Steven J, Ban, Qian, Weiss, Paul S, Kohn, Donald B, Chen, Kai, Chiou, Shih-Hwa, and Tseng, Hsian-Rong

Subjects

Medical Biotechnology, Biomedical and Clinical Sciences, Biotechnology, Genetics, Gene Therapy, Rare Diseases, 5.2 Cellular and gene therapies, Aetiology, Development of treatments and therapeutic interventions, 2.1 Biological and endogenous factors, Animals, CRISPR-Cas Systems, Gene Editing, Genetic Vectors, Hemoglobinopathies, Hemoglobins, Mice

Abstract

Leveraging the endogenous homology-directed repair (HDR) pathway, the CRISPR-Cas9 gene-editing system can be applied to knock in a therapeutic gene at a designated site in the genome, offering a general therapeutic solution for treating genetic diseases such as hemoglobinopathies. Here, a combined supramolecular nanoparticle (SMNP)/supramolecular nanosubstrate-mediated delivery (SNSMD) strategy is used to facilitate CRISPR-Cas9 knockin of the hemoglobin beta (HBB) gene into the adeno-associated virus integration site 1 (AAVS1) safe-harbor site of an engineered K562 3.21 cell line harboring the sickle cell disease mutation. Through stepwise treatments of the two SMNP vectors encapsulating a Cas9•single-guide RNA (sgRNA) complex and an HBB/green fluorescent protein (GFP)-encoding plasmid, CRISPR-Cas9 knockin was successfully achieved via HDR. Last, the HBB/GFP-knockin K562 3.21 cells were introduced into mice via intraperitoneal injection to show their in vivo proliferative potential. This proof-of-concept demonstration paves the way for general gene therapeutic solutions for treating hemoglobinopathies.

Published

2020

36. Lentiviral gene therapy for X-linked chronic granulomatous disease.

Author

Kohn, Donald B, Booth, Claire, Kang, Elizabeth M, Pai, Sung-Yun, Shaw, Kit L, Santilli, Giorgia, Armant, Myriam, Buckland, Karen F, Choi, Uimook, De Ravin, Suk See, Dorsey, Morna J, Kuo, Caroline Y, Leon-Rico, Diego, Rivat, Christine, Izotova, Natalia, Gilmour, Kimberly, Snell, Katie, Dip, Jinhua Xu-Bayford, Darwish, Jinan, Morris, Emma C, Terrazas, Dayna, Wang, Leo D, Bauser, Christopher A, Paprotka, Tobias, Kuhns, Douglas B, Gregg, John, Raymond, Hayley E, Everett, John K, Honnet, Geraldine, Biasco, Luca, Newburger, Peter E, Bushman, Frederic D, Grez, Manuel, Gaspar, H Bobby, Williams, David A, Malech, Harry L, Galy, Anne, Thrasher, Adrian J, and Net4CGD consortium

Subjects

Net4CGD consortium, Neutrophils, Hematopoietic Stem Cells, Chromosomes, Human, X, Humans, Lentivirus, Granulomatous Disease, Chronic, Antigens, CD34, Treatment Outcome, Transplantation Conditioning, Comorbidity, Gene Silencing, Genes, Regulator, Genetic Vectors, Adolescent, Child, Child, Preschool, United States, Male, Promoter Regions, Genetic, Young Adult, Patient Safety, Genetic Therapy, United Kingdom, NADPH Oxidases, Genetics, Hematology, Regenerative Medicine, Stem Cell Research, Stem Cell Research - Nonembryonic - Human, Gene Therapy, Clinical Trials and Supportive Activities, Infectious Diseases, Clinical Research, 5.2 Cellular and gene therapies, Development of treatments and therapeutic interventions, Inflammatory and immune system, Infection, Medical and Health Sciences, Immunology

Abstract

Chronic granulomatous disease (CGD) is a rare inherited disorder of phagocytic cells1,2. We report the initial results of nine severely affected X-linked CGD (X-CGD) patients who received ex vivo autologous CD34+ hematopoietic stem and progenitor cell-based lentiviral gene therapy following myeloablative conditioning in first-in-human studies (trial registry nos. NCT02234934 and NCT01855685). The primary objectives were to assess the safety and evaluate the efficacy and stability of biochemical and functional reconstitution in the progeny of engrafted cells at 12 months. The secondary objectives included the evaluation of augmented immunity against bacterial and fungal infection, as well as assessment of hematopoietic stem cell transduction and engraftment. Two enrolled patients died within 3 months of treatment from pre-existing comorbidities. At 12 months, six of the seven surviving patients demonstrated stable vector copy numbers (0.4-1.8 copies per neutrophil) and the persistence of 16-46% oxidase-positive neutrophils. There was no molecular evidence of either clonal dysregulation or transgene silencing. Surviving patients have had no new CGD-related infections, and six have been able to discontinue CGD-related antibiotic prophylaxis. The primary objective was met in six of the nine patients at 12 months follow-up, suggesting that autologous gene therapy is a promising approach for CGD patients.

Published

2020

37. Editing the Sickle Cell Disease Mutation in Human Hematopoietic Stem Cells: Comparison of Endonucleases and Homologous Donor Templates

Author

Romero, Zulema, Lomova, Anastasia, Said, Suzanne, Miggelbrink, Alexandra, Kuo, Caroline Y, Campo-Fernandez, Beatriz, Hoban, Megan D, Masiuk, Katelyn E, Clark, Danielle N, Long, Joseph, Sanchez, Julie M, Velez, Miriam, Miyahira, Eric, Zhang, Ruixue, Brown, Devin, Wang, Xiaoyan, Kurmangaliyev, Yerbol Z, Hollis, Roger P, and Kohn, Donald B

Subjects

Medical Biotechnology, Biomedical and Clinical Sciences, Cardiovascular Medicine and Haematology, Rare Diseases, Hematology, Gene Therapy, Regenerative Medicine, Genetics, Stem Cell Research - Nonembryonic - Human, Biotechnology, Stem Cell Research, Sickle Cell Disease, Transplantation, 5.2 Cellular and gene therapies, Development of treatments and therapeutic interventions, Anemia, Sickle Cell, CRISPR-Cas Systems, Dependovirus, Endonucleases, Gene Editing, Gene Expression, Gene Targeting, Genetic Therapy, Genetic Vectors, Hematopoietic Stem Cells, Humans, Mutation, Parvovirinae, Tissue Donors, Transduction, Genetic, Zinc Finger Nucleases, beta-Globins, CRISPR/Cas9, adeno-associated virus 6, gene editing, hematopoietic stem cells, homologous recombination, non-homologous end joining, sickle cell disease, zinc finger nuclease, Biological Sciences, Technology, Medical and Health Sciences, Clinical sciences, Medical biotechnology

Abstract

Site-specific correction of a point mutation causing a monogenic disease in autologous hematopoietic stem and progenitor cells (HSPCs) can be used as a treatment of inherited disorders of the blood cells. Sickle cell disease (SCD) is an ideal model to investigate the potential use of gene editing to transvert a single point mutation at the β-globin locus (HBB). We compared the activity of zinc-finger nucleases (ZFNs) and CRISPR/Cas9 for editing, and homologous donor templates delivered as single-stranded oligodeoxynucleotides (ssODNs), adeno-associated virus serotype 6 (AAV6), integrase-deficient lentiviral vectors (IDLVs), and adenovirus 5/35 serotype (Ad5/35) to transvert the base pair responsible for SCD in HBB in primary human CD34+ HSPCs. We found that the ZFNs and Cas9 directed similar frequencies of nuclease activity. In vitro, AAV6 led to the highest frequencies of homology-directed repair (HDR), but levels of base pair transversions were significantly reduced when analyzing cells in vivo in immunodeficient mouse xenografts, with similar frequencies achieved with either AAV6 or ssODNs. AAV6 also caused significant impairment of colony-forming progenitors and human cell engraftment. Gene correction in engrafting hematopoietic stem cells may be limited by the capacity of the cells to mediate HDR, suggesting additional manipulations may be needed for high-efficiency gene correction in HSPCs.

Published

2019

38. Hematopoietic Stem Cell Gene Therapy: Progress and Lessons Learned

Author

Morgan, Richard A, Gray, David, Lomova, Anastasia, and Kohn, Donald B

Subjects

Medical Biotechnology, Biomedical and Clinical Sciences, Transplantation, Biotechnology, Genetics, Stem Cell Research - Nonembryonic - Human, Stem Cell Research, Gene Therapy, Regenerative Medicine, Stem Cell Research - Nonembryonic - Non-Human, 5.2 Cellular and gene therapies, Development of treatments and therapeutic interventions, Blood, Clinical Trials as Topic, Gene Editing, Gene Transfer Techniques, Genetic Therapy, Genetic Vectors, Hematopoietic Stem Cell Transplantation, Hematopoietic Stem Cells, Humans, Biological Sciences, Medical and Health Sciences, Developmental Biology, Biological sciences, Biomedical and clinical sciences

Abstract

The use of allogeneic hematopoietic stem cells (HSCs) to treat genetic blood cell diseases has become a clinical standard but is limited by the availability of suitable matched donors and potential immunologic complications. Gene therapy using autologous HSCs should avoid these limitations and thus may be safer. Progressive improvements in techniques for genetic correction of HSCs, by either vector gene addition or gene editing, are facilitating successful treatments for an increasing number of diseases. We highlight the progress, successes, and remaining challenges toward the development of HSC gene therapies and discuss lessons they provide for the development of future clinical stem cell therapies.

Published

2017

39. Differentiation of RPE cells from integration-free iPS cells and their cell biological characterization.

Author

Hazim, Roni A, Karumbayaram, Saravanan, Jiang, Mei, Dimashkie, Anupama, Lopes, Vanda S, Li, Douran, Burgess, Barry L, Vijayaraj, Preethi, Alva-Ornelas, Jackelyn A, Zack, Jerome A, Kohn, Donald B, Gomperts, Brigitte N, Pyle, April D, Lowry, William E, and Williams, David S

Subjects

Fibroblasts, Epithelial Cells, Skin, Animals, Mice, Inbred BALB C, Mice, Knockout, Humans, Mice, Encephalitis Virus, Venezuelan Equine, Retinal Degeneration, Disease Models, Animal, Intercellular Signaling Peptides and Proteins, Cell Differentiation, Cell Polarity, Genetic Vectors, Retinal Pigment Epithelium, Injections, Intraocular, Induced Pluripotent Stem Cells, Primary Cell Culture, Cellular Reprogramming, Induced pluripotent stem cells, Live-cell imaging, Phagocytosis, RPE cytoskeleton, Retinal pigment epithelium, Inbred BALB C, Knockout, Encephalitis Virus, Venezuelan Equine, Disease Models, Animal, Injections, Intraocular, Biological Sciences, Technology, Medical and Health Sciences

Abstract

BackgroundDysfunction of the retinal pigment epithelium (RPE) is implicated in numerous forms of retinal degeneration. The readily accessible environment of the eye makes it particularly suitable for the transplantation of RPE cells, which can now be derived from autologous induced pluripotent stem cells (iPSCs), to treat retinal degeneration. For RPE transplantation to become feasible in the clinic, patient-specific somatic cells should be reprogrammed to iPSCs without the introduction of reprogramming genes into the genome of the host cell, and then subsequently differentiated into RPE cells that are well characterized for safety and functionality prior to transplantation.MethodsWe have reprogrammed human dermal fibroblasts to iPSCs using nonintegrating RNA, and differentiated the iPSCs toward an RPE fate (iPSC-RPE), under Good Manufacturing Practice (GMP)-compatible conditions.ResultsUsing highly sensitive assays for cell polarity, structure, organelle trafficking, and function, we found that iPSC-RPE cells in culture exhibited key characteristics of native RPE. Importantly, we demonstrate for the first time with any stem cell-derived RPE cell that live cells are able to support dynamic organelle transport. This highly sensitive test is critical for RPE cells intended for transplantation, since defects in intracellular motility have been shown to promote RPE pathogenesis akin to that found in macular degeneration. To test their capabilities for in-vivo transplantation, we injected the iPSC-RPE cells into the subretinal space of a mouse model of retinal degeneration, and demonstrated that the transplanted cells are capable of rescuing lost RPE function.ConclusionsThis report documents the successful generation, under GMP-compatible conditions, of human iPSC-RPE cells that possess specific characteristics of healthy RPE. The report adds to a growing literature on the utility of human iPSC-RPE cells for cell culture investigations on pathogenicity and for therapeutic transplantation, by corroborating findings of others, and providing important new information on essential RPE cell biological properties.

Published

2017

40. Improving Gene Therapy Efficiency through the Enrichment of Human Hematopoietic Stem Cells

Author

Masiuk, Katelyn E, Brown, Devin, Laborada, Jennifer, Hollis, Roger P, Urbinati, Fabrizia, and Kohn, Donald B

Subjects

Medical Biotechnology, Biomedical and Clinical Sciences, Cardiovascular Medicine and Haematology, Immunology, Stem Cell Research, Stem Cell Research - Nonembryonic - Non-Human, Clinical Research, Gene Therapy, Stem Cell Research - Nonembryonic - Human, Regenerative Medicine, Biotechnology, Genetics, Hematology, Transplantation, Development of treatments and therapeutic interventions, 5.2 Cellular and gene therapies, ADP-ribosyl Cyclase 1, Animals, Antigens, CD34, Gene Expression, Gene Transfer Techniques, Genes, Reporter, Genetic Therapy, Genetic Vectors, Graft Survival, Hematopoietic Stem Cell Transplantation, Hematopoietic Stem Cells, Humans, Immunomagnetic Separation, Immunophenotyping, Lentivirus, Mice, Transduction, Genetic, Transgenes, gene therapy, hematopoietic stem cells, lentiviral vectors, Biological Sciences, Technology, Medical and Health Sciences, Clinical sciences, Medical biotechnology

Abstract

Lentiviral vector (LV)-based hematopoietic stem cell (HSC) gene therapy is becoming a promising clinical strategy for the treatment of genetic blood diseases. However, the current approach of modifying 1 × 108 to 1 × 109 CD34+ cells per patient requires large amounts of LV, which is expensive and technically challenging to produce at clinical scale. Modification of bulk CD34+ cells uses LV inefficiently, because the majority of CD34+ cells are short-term progenitors with a limited post-transplant lifespan. Here, we utilized a clinically relevant, immunomagnetic bead (IB)-based method to purify CD34+CD38- cells from human bone marrow (BM) and mobilized peripheral blood (mPB). IB purification of CD34+CD38- cells enriched severe combined immune deficiency (SCID) repopulating cell (SRC) frequency an additional 12-fold beyond standard CD34+ purification and did not affect gene marking of long-term HSCs. Transplant of purified CD34+CD38- cells led to delayed myeloid reconstitution, which could be rescued by the addition of non-transduced CD38+ cells. Importantly, LV modification and transplantation of IB-purified CD34+CD38- cells/non-modified CD38+ cells into immune-deficient mice achieved long-term gene-marked engraftment comparable with modification of bulk CD34+ cells, while utilizing ∼7-fold less LV. Thus, we demonstrate a translatable method to improve the clinical and commercial viability of gene therapy for genetic blood cell diseases.

Published

2017

41. Potentially therapeutic levels of anti-sickling globin gene expression following lentivirus-mediated gene transfer in sickle cell disease bone marrow CD34+ cells

Author

Urbinati, Fabrizia, Hargrove, Phillip W, Geiger, Sabine, Romero, Zulema, Wherley, Jennifer, Kaufman, Michael L, Hollis, Roger P, Chambers, Christopher B, Persons, Derek A, Kohn, Donald B, and Wilber, Andrew

Subjects

Medical Biotechnology, Biomedical and Clinical Sciences, Cardiovascular Medicine and Haematology, Clinical Research, Biotechnology, Regenerative Medicine, Genetics, Transplantation, Hematology, Stem Cell Research - Nonembryonic - Non-Human, Sickle Cell Disease, Stem Cell Research, Gene Therapy, Rare Diseases, Orphan Drug, Pain Research, Stem Cell Research - Nonembryonic - Human, Development of treatments and therapeutic interventions, 5.2 Cellular and gene therapies, Blood, Anemia, Sickle Cell, Antigens, CD34, Bone Marrow Cells, Fetal Hemoglobin, Flow Cytometry, Gene Expression, Gene Transfer Techniques, Genetic Therapy, Genetic Vectors, Hemoglobins, Humans, Lentivirus, Reverse Transcriptase Polymerase Chain Reaction, beta-Globins, gamma-Globins, Cardiorespiratory Medicine and Haematology, Immunology, Cardiovascular medicine and haematology

Abstract

Sickle cell disease (SCD) can be cured by allogeneic hematopoietic stem cell transplant. However, this is only possible when a matched donor is available, making the development of gene therapy using autologous hematopoietic stem cells a highly desirable alternative. We used a culture model of human erythropoiesis to directly compare two insulated, self-inactivating, and erythroid-specific lentiviral vectors, encoding for γ-globin (V5m3-400) or a modified β-globin (βAS3-FB) for production of antisickling hemoglobin (Hb) and correction of red cell deformability after deoxygenation. Bone marrow CD34+ cells from three SCD patients were transduced using V5m3-400 or βAS3-FB and compared with mock-transduced SCD or healthy donor CD34+ cells. Lentiviral transduction did not impair cell growth or differentiation, as gauged by proliferation and acquisition of erythroid markers. Vector copy number averaged approximately one copy per cell, and corrective globin mRNA levels were increased more than sevenfold over mock-transduced controls. Erythroblasts derived from healthy donor and mock-transduced SCD cells produced a low level of fetal Hb that was increased to 23.6 ± 4.1% per vector copy for cells transduced with V5m3-400. Equivalent levels of modified normal adult Hb of 17.6 ± 3.8% per vector copy were detected for SCD cells transduced with βAS3-FB. These levels of antisickling Hb production were sufficient to reduce sickling of terminal-stage red blood cells upon deoxygenation. We concluded that the achieved levels of fetal Hb and modified normal adult Hb would likely prove therapeutic to SCD patients who lack matched donors.

Published

2015

42. Enrichment of human hematopoietic stem/progenitor cells facilitates transduction for stem cell gene therapy.

Author

Baldwin, Kismet, Urbinati, Fabrizia, Romero, Zulema, Campo-Fernandez, Beatriz, Kaufman, Michael L, Cooper, Aaron R, Masiuk, Katelyn, Hollis, Roger P, and Kohn, Donald B

Subjects

Hematopoietic Stem Cells, Cell Line, Erythroid Cells, Animals, Mice, Inbred NOD, Humans, Lentivirus, Receptors, LDL, Antigens, CD34, Hematopoietic Stem Cell Transplantation, Cell Separation, Transduction, Genetic, Cell Differentiation, Cell Proliferation, Genetic Vectors, Antigens, CD38, Genetic Therapy, Gene therapy, Hematopoietic stem cells, Lentiviral vector, Stem cell enrichment, ADP-ribosyl Cyclase 1, Immunology, Biological Sciences, Technology, Medical and Health Sciences

Abstract

Autologous hematopoietic stem cell (HSC) gene therapy for sickle cell disease has the potential to treat this illness without the major immunological complications associated with allogeneic transplantation. However, transduction efficiency by β-globin lentiviral vectors using CD34-enriched cell populations is suboptimal and large vector production batches may be needed for clinical trials. Transducing a cell population more enriched for HSC could greatly reduce vector needs and, potentially, increase transduction efficiency. CD34(+) /CD38(-) cells, comprising ∼1%-3% of all CD34(+) cells, were isolated from healthy cord blood CD34(+) cells by fluorescence-activated cell sorting and transduced with a lentiviral vector expressing an antisickling form of beta-globin (CCL-β(AS3) -FB). Isolated CD34(+) /CD38(-) cells were able to generate progeny over an extended period of long-term culture (LTC) compared to the CD34(+) cells and required up to 40-fold less vector for transduction compared to bulk CD34(+) preparations containing an equivalent number of CD34(+) /CD38(-) cells. Transduction of isolated CD34(+) /CD38(-) cells was comparable to CD34(+) cells measured by quantitative PCR at day 14 with reduced vector needs, and average vector copy/cell remained higher over time for LTC initiated from CD34(+) /38(-) cells. Following in vitro erythroid differentiation, HBBAS3 mRNA expression was similar in cultures derived from CD34(+) /CD38(-) cells or unfractionated CD34(+) cells. In vivo studies showed equivalent engraftment of transduced CD34(+) /CD38(-) cells when transplanted in competition with 100-fold more CD34(+) /CD38(+) cells. This work provides initial evidence for the beneficial effects from isolating human CD34(+) /CD38(-) cells to use significantly less vector and potentially improve transduction for HSC gene therapy.

Published

2015

43. Effects of Vector Backbone and Pseudotype on Lentiviral Vector-mediated Gene Transfer: Studies in Infant ADA-Deficient Mice and Rhesus Monkeys

Author

Sarracino, Denise Carbonaro, Tarantal, Alice F, Lee, C Chang I, Martinez, Michele, Jin, Xiangyang, Wang, Xiaoyan, Hardee, Cinnamon L, Geiger, Sabine, Kahl, Christoph A, and Kohn, Donald B

Subjects

Medical Biotechnology, Medical Microbiology, Biomedical and Clinical Sciences, Gene Therapy, Regenerative Medicine, Genetics, Pediatric, Hematology, Biotechnology, Transplantation, Development of treatments and therapeutic interventions, 5.2 Cellular and gene therapies, Good Health and Well Being, Adenosine Deaminase, Animals, Disease Models, Animal, Female, Gene Expression, Gene Order, Gene Transfer Techniques, Genetic Vectors, Humans, Lentivirus, Macaca mulatta, Mice, Mice, Knockout, Retroviridae, Severe Combined Immunodeficiency, Tissue Distribution, Transduction, Genetic, Transgenes, Biological Sciences, Technology, Medical and Health Sciences, Clinical sciences, Medical biotechnology

Abstract

Systemic delivery of a lentiviral vector carrying a therapeutic gene represents a new treatment for monogenic disease. Previously, we have shown that transfer of the adenosine deaminase (ADA) cDNA in vivo rescues the lethal phenotype and reconstitutes immune function in ADA-deficient mice. In order to translate this approach to ADA-deficient severe combined immune deficiency patients, neonatal ADA-deficient mice and newborn rhesus monkeys were treated with species-matched and mismatched vectors and pseudotypes. We compared gene delivery by the HIV-1-based vector to murine γ-retroviral vectors pseudotyped with vesicular stomatitis virus-glycoprotein or murine retroviral envelopes in ADA-deficient mice. The vesicular stomatitis virus-glycoprotein pseudotyped lentiviral vectors had the highest titer and resulted in the highest vector copy number in multiple tissues, particularly liver and lung. In monkeys, HIV-1 or simian immunodeficiency virus vectors resulted in similar biodistribution in most tissues including bone marrow, spleen, liver, and lung. Simian immunodeficiency virus pseudotyped with the gibbon ape leukemia virus envelope produced 10- to 30-fold lower titers than the vesicular stomatitis virus-glycoprotein pseudotype, but had a similar tissue biodistribution and similar copy number in blood cells. The relative copy numbers achieved in mice and monkeys were similar when adjusted to the administered dose per kg. These results suggest that this approach can be scaled-up to clinical levels for treatment of ADA-deficient severe combined immune deficiency subjects with suboptimal hematopoietic stem cell transplantation options.

Published

2014

44. HSV-sr39TK Positron Emission Tomography and Suicide Gene Elimination of Human Hematopoietic Stem Cells and Their Progeny in Humanized Mice

Author

Gschweng, Eric H, McCracken, Melissa N, Kaufman, Michael L, Ho, Michelle, Hollis, Roger P, Wang, Xiaoyan, Saini, Navdeep, Koya, Richard C, Chodon, Thinle, Ribas, Antoni, Witte, Owen N, and Kohn, Donald B

Subjects

Medical Biotechnology, Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Stem Cell Research, Genetics, Vaccine Related, Biotechnology, Gene Therapy, Clinical Research, Regenerative Medicine, Stem Cell Research - Nonembryonic - Human, Immunization, Cancer, Development of treatments and therapeutic interventions, 5.2 Cellular and gene therapies, Animals, Antigens, CD34, Antigens, Neoplasm, Disease Models, Animal, Genes, Transgenic, Suicide, Genetic Therapy, Genetic Vectors, Hematopoietic Stem Cells, Herpesvirus 1, Human, Humans, Immunotherapy, Membrane Proteins, Mice, Positron-Emission Tomography, Receptors, Antigen, T-Cell, T-Lymphocytes, Transduction, Genetic, Oncology & Carcinogenesis, Biochemistry and cell biology, Oncology and carcinogenesis

Abstract

Engineering immunity against cancer by the adoptive transfer of hematopoietic stem cells (HSC) modified to express antigen-specific T-cell receptors (TCR) or chimeric antigen receptors generates a continual supply of effector T cells, potentially providing superior anticancer efficacy compared with the infusion of terminally differentiated T cells. Here, we demonstrate the in vivo generation of functional effector T cells from CD34-enriched human peripheral blood stem cells modified with a lentiviral vector designed for clinical use encoding a TCR recognizing the cancer/testes antigen NY-ESO-1, coexpressing the PET/suicide gene sr39TK. Ex vivo analysis of T cells showed antigen- and HLA-restricted effector function against melanoma. Robust engraftment of gene-modified human cells was demonstrated with PET reporter imaging in hematopoietic niches such as femurs, humeri, vertebrae, and the thymus. Safety was demonstrated by the in vivo ablation of PET signal, NY-ESO-1-TCR-bearing cells, and integrated lentiviral vector genomes upon treatment with ganciclovir, but not with vehicle control. Our study provides support for the efficacy and safety of gene-modified HSCs as a therapeutic modality for engineered cancer immunotherapy. Cancer Res; 74(18); 5173-83. ©2014 AACR.

Published

2014

45. Gene therapy: charting a future course--summary of a National Institutes of Health Workshop, April 12, 2013.

Author

O'Reilly, Marina, Federoff, Howard J, Fong, Yuman, Kohn, Donald B, Patterson, Amy P, Ahmed, Nabil, Asokan, Aravind, Boye, Shannon E, Crystal, Ronald G, De Oliveira, Satiro, Gargiulo, Linda, Harper, Scott Q, Ikeda, Yasuhiro, Jambou, Robert, Montgomery, Maureen, Prograis, Lawrence, Rosenthal, Eugene, Sterman, Daniel H, Vandenberghe, Luk H, Zoloth, Laurie, Abedi, Mehrdad, Adair, Jennifer, Adusumilli, Prasad S, Goins, William F, Gray, Jhanelle, Monahan, Paul, Popplewell, Leslie, Sena-Esteves, Miguel, Tannous, Bakhos, Weber, Thomas, Wierda, William, Gopal-Srivastava, Rashmi, McDonald, Cheryl L, Rosenblum, Daniel, and Corrigan-Curay, Jacqueline

Subjects

Animals, Education, Continuing, Genetic Research, Genetic Therapy: economics, ethics, legislation & jurisprudence, Genetic Vectors, Humans, National Institutes of Health (U.S.), Stem Cell Research, Stem Cell Transplantation, Transduction, Genetic, United States

Abstract

Recently, the gene therapy field has begun to experience clinical successes in a number of different diseases using various approaches and vectors. The workshop Gene Therapy: Charting a Future Course, sponsored by the National Institutes of Health (NIH) Office of Biotechnology Activities, brought together early and mid-career researchers to discuss the key scientific challenges and opportunities, ethical and communication issues, and NIH and foundation resources available to facilitate further clinical advances.

Published

2014

46. Stable Transduction of Quiescent CD34 + CD38 - Human Hematopoietic Cells by HIV-1-Based Lentiviral Vectors

Author

Case, Scott S., Price, Mary A., Jordan, Craig T., Yu, Xiao Jin, Wang, Lijun, Bauer, Gerhard, Haas, Dennis L., Xu, Dakun, Stripecke, Renata, Naldini, Luigi, Kohn, Donald B., and Crooks, Gay M.

Published

1999

47. Consistent, Persistent Expression from Modified Retroviral Vectors in Murine Hematopoietic Stem Cells

Author

Robbins, Paul B., Skelton, Dianne C., Yu, Xiao-Jin, Halene, Stephanie, Leonard, Earl H., and Kohn, Donald B.

Published

1998

48. Transduction of Pluripotent Human Hematopoietic Stem Cells Demonstrated by Clonal Analysis after Engraftment in Immune-Deficient Mice

Author

Nolta, Jan A., Dao, Mo A., Wells, Susie, Smogorzewska, E. Monika, and Kohn, Donald B.

Published

1996

49. Correction of Adenosine Deaminase Deficiency in Cultured Human T and B Cells by Retrovirus-Mediated Gene Transfer

Author

Kantoff, Philip W., Kohn, Donald B., Mitsuya, Hiroaki, Armentano, Donna, Sieberg, Miri, Zwiebel, James A., Eglitis, Martin A., McLachlin, Jeanne R., Wiginton, Dan A., Hutton, John J., Horowitz, Sheldon D., Gilboa, Eli, Blaese, R. Michael, and Anderson, W. French

Published

1986

50. Lack of Expression from a Retroviral Vector After Transduction of Murine Hematopoietic Stem Cells is Associated with Methylation in vivo

Author

Challita, Pia-Maria and Kohn, Donald B.

Published

1994