论文信息 - Genotoxicity of retroviral integration in hematopoietic cells.

Genotoxicity of retroviral integration in hematopoietic cells.

The experience of the past 3 years, since the first case of leukemia was reported in a child cured of X-linked severe combined immunodeficiency (X-SCID) by gene therapy, indicates that the potential genotoxicity of retroviral integration in hematopoietic cells will remain a consideration in evaluating the relative risks versus benefits of gene therapy for specific blood disorders. Although many unique variables may have contributed to an increased risk in X-SCID patients, clonal dominance or frank neoplasia in animal models, clonal dominance in humans with chronic granulomatous disease, and the ability of retroviral integration to immortalize normal bone marrow cells or convert factor-dependent cells to factor independence suggest that transduction of cells with an integrating retrovirus has the potential for altering their subsequent biologic behavior. The selective pressure imposed during in vitro culture or after engraftment may uncover a growth or survival advantage for cells in which an integration event has affected gene expression. Such cells then carry the risk that subsequent mutations may lead to neoplastic evolution of individual clones. Balancing that risk is that the vast majority of integration events seem to be neutral and that optimizing vector design may diminish the probability of altering gene expression by an integrated vector genome. Several cell culture systems and animal models designed to empirically evaluate the safety of vector systems are being developed and should provide useful data for weighing the relative risks and benefits for specific diseases and patient populations. Gene therapy interventions continue to have enormous potential for the treatment of disorders of the hematopoietic system. The future of such efforts seems bright as we continue to evolve and improve various strategies to make such interventions both effective and as safe as possible.

[1] F. Bushman,et al. Retroviral DNA Integration: ASLV, HIV, and MLV Show Distinct Target Site Preferences , 2004, PLoS biology.

[2] C. von Kalle,et al. Recurrent retroviral vector integration at the Mds1/Evi1 locus in nonhuman primate hematopoietic cells. , 2005, Blood.

[3] J. Abkowitz,et al. Improved transduction of human sheep repopulating cells by retrovirus vectors pseudotyped with feline leukemia virus type C or RD114 envelopes. , 2005, Blood.

[4] J. Gebert,et al. Double suicide gene (cytosine deaminase and herpes simplex virus thymidine kinase) but not single gene transfer allows reliable elimination of tumor cells in vivo. , 1998, Human gene therapy.

[5] M. Roncarolo,et al. IL-3 or IL-7 increases ex vivo gene transfer efficiency in ADA-SCID BM CD34+ cells while maintaining in vivo lymphoid potential. , 2004, Molecular therapy : the journal of the American Society of Gene Therapy.

[6] D. Bartel,et al. MicroRNAs Modulate Hematopoietic Lineage Differentiation , 2004, Science.

[7] C. Croce,et al. MicroRNA profiling reveals distinct signatures in B cell chronic lymphocytic leukemias. , 2004, Proceedings of the National Academy of Sciences of the United States of America.

[8] K. Mitani,et al. Molecular mechanisms of leukemogenesis by AML1/EVI-1 , 2004, Oncogene.

[9] M. L. Beau,et al. Ex vivo culture of Fancc-/- stem/progenitor cells predisposes cells to undergo apoptosis, and surviving stem/progenitor cells display cytogenetic abnormalities and an increased risk of malignancy. , 2005, Blood.

[10] C. Dunbar,et al. Persistence and expression of the adenosine deaminase gene for 12 years and immune reaction to gene transfer components: long-term results of the first clinical gene therapy trial. , 2003, Blood.

[11] Timothy B. Stockwell,et al. The Sequence of the Human Genome , 2001, Science.

[12] Licheng Zeng,et al. Successful correction of the human beta-thalassemia major phenotype using a lentiviral vector. , 2004, Blood.

[13] C. Farrell,et al. Prospects and implications of using chromatin insulators in gene therapy and transgenesis. , 2004, BioEssays : news and reviews in molecular, cellular and developmental biology.

[14] J. Stephenson,et al. Isolation from BALB/c mouse cells of a structural polypeptide of a third endogenous type C virus. , 1974, Cell.

[15] Phillip D. Zamore,et al. Ribo-gnome: The Big World of Small RNAs , 2005, Science.

[16] F. Bushman,et al. Target-sequence preferences of HIV-1 integration complexes in vitro. , 1996, Virology.

[17] C. von Kalle,et al. Long-term clinical and molecular follow-up of large animals receiving retrovirally transduced stem and progenitor cells: no progression to clonal hematopoiesis or leukemia. , 2004, Molecular therapy : the journal of the American Society of Gene Therapy.

[18] David A. Williams,et al. Introduction of new genetic material into pluripotent haematopoietic stem cells of the mouse , 1984, Nature.

[19] A. Mortellaro,et al. Correction of ADA-SCID by Stem Cell Gene Therapy Combined with Nonmyeloablative Conditioning , 2002, Science.

[20] W. Leonard,et al. Restoration of lymphoid populations in a murine model of X-linked severe combined immunodeficiency by a gene-therapy approach. , 1999, Blood.

[21] M. Schweder,et al. Human A1, a Bcl-2-related gene, is induced in leukemic cells by cytokines as well as differentiating factors , 1997, Leukemia.

[22] K. Weinberg,et al. T lymphocytes with a normal ADA gene accumulate after transplantation of transduced autologous umbilical cord blood CD34+ cells in ADA-deficient SCID neonates , 1998, Nature Medicine.

[23] T. Rabbitts,et al. The oncogenic LIM protein Rbtn2 causes thymic developmental aberrations that precede malignancy in transgenic mice. , 1995, Oncogene.

[24] S. Burgess,et al. Weak Palindromic Consensus Sequences Are a Common Feature Found at the Integration Target Sites of Many Retroviruses , 2005, Journal of Virology.

[25] R. Gelber,et al. Improved outcome for children with acute lymphoblastic leukemia: results of Dana-Farber Consortium Protocol 91-01. , 2001, Blood.

[26] K. Keyvanfar,et al. Efficient gene transfer into rhesus repopulating hematopoietic stem cells using a simian immunodeficiency virus-based lentiviral vector system. , 2004, Blood.

[27] B. Sorrentino,et al. Transduction of murine bone marrow cells with an MDR1 vector enables ex vivo stem cell expansion, but these expanded grafts cause a myeloproliferative syndrome in transplanted mice. , 1998, Blood.

[28] G. Vassilopoulos,et al. Gene transfer with foamy virus vectors. , 2002, Methods in enzymology.

[29] J. Rehg,et al. Ectopic expression of rhombotin-2 causes selective expansion of CD4-CD8- lymphocytes in the thymus and T-cell tumors in transgenic mice. , 1995, Blood.

[30] Takeshi Suzuki,et al. New genes involved in cancer identified by retroviral tagging , 2002, Nature Genetics.

[31] A. Schambach,et al. Tumor cells escape suicide gene therapy by genetic and epigenetic instability. , 2004, Blood.

[32] I. Shah. Severe combined immunodeficiency. , 2005, Indian pediatrics.

[33] K. Sugamura,et al. gamma-c gene transfer into SCID X1 patients' B-cell lines restores normal high-affinity interleukin-2 receptor expression and function. , 1996, Blood.

[34] C. Croce,et al. Human microRNA genes are frequently located at fragile sites and genomic regions involved in cancers. , 2004, Proceedings of the National Academy of Sciences of the United States of America.

[35] A. Fischer,et al. Long-term survival and transplantation of haemopoietic stem cells for immunodeficiencies: report of the European experience 1968–99 , 2003, The Lancet.

[36] A. Fischer,et al. Stable and functional lymphoid reconstitution of common cytokine receptor gamma chain deficient mice by retroviral-mediated gene transfer. , 2000, Blood.

[37] Shawn M. Burgess,et al. Transcription Start Regions in the Human Genome Are Favored Targets for MLV Integration , 2003, Science.

[38] Hans-Peter Kiem,et al. Foamy virus vector integration sites in normal human cells , 2006, Proceedings of the National Academy of Sciences of the United States of America.

[39] Félix Recillas-Targa,et al. Position-effect protection and enhancer blocking by the chicken β-globin insulator are separable activities , 2002, Proceedings of the National Academy of Sciences of the United States of America.

[40] T. Hawley,et al. Performance- and safety-enhanced lentiviral vectors containing the human interferon-β scaffold attachment region and the chicken β-globin insulator , 2003 .

[41] Paul Shinn,et al. HIV-1 Integration in the Human Genome Favors Active Genes and Local Hotspots , 2002, Cell.

[42] J. Nolta,et al. Immune-deficient mouse models for analysis of human stem cells. , 2003, BioTechniques.

[43] J. V. Moran,et al. Initial sequencing and analysis of the human genome. , 2001, Nature.

[44] A. Fischer,et al. Sustained correction of X-linked severe combined immunodeficiency by ex vivo gene therapy. , 2002, The New England journal of medicine.

[45] D. Baltimore,et al. Construction of a retrovirus packaging mutant and its use to produce helper-free defective retrovirus , 1983, Cell.

[46] M. Sadelain. Insertional oncogenesis in gene therapy: how much of a risk? , 2004, Gene Therapy.

[47] L. Arthur,et al. Simian Immunodeficiency Virus Integration Preference Is Similar to That of Human Immunodeficiency Virus Type 1 , 2005, Journal of Virology.

[48] S. Holland,et al. Prolonged production of NADPH oxidase-corrected granulocytes after gene therapy of chronic granulomatous disease. , 1997, Proceedings of the National Academy of Sciences of the United States of America.

[49] E. Medico,et al. Promoter trapping reveals significant differences in integration site selection between MLV and HIV vectors in primary hematopoietic cells. , 2005, Blood.

[50] Y. Ikeda,et al. Gene transfer to repopulating human CD34+ cells using amphotropic-, GALV-, or RD114-pseudotyped HIV-1-based vectors from stable producer cells. , 2005, Molecular therapy : the journal of the American Society of Gene Therapy.

[51] S. Sandmeyer,et al. Integration by design , 2003, Proceedings of the National Academy of Sciences of the United States of America.

[52] Hannah Hoag. Gene therapy rising? , 2005, Nature.

[53] C. von Kalle,et al. Murine Leukemia Induced by Retroviral Gene Marking , 2002, Science.

[54] Y. Hamel,et al. Optimization of retroviral gene transfer protocol to maintain the lymphoid potential of progenitor cells. , 2001, Human gene therapy.

[55] Cameron S. Osborne,et al. LMO2-Associated Clonal T Cell Proliferation in Two Patients after Gene Therapy for SCID-X1 , 2003, Science.

[56] C. von Kalle,et al. Leukemias following retroviral transfer of multidrug resistance 1 (MDR1) are driven by combinatorial insertional mutagenesis. , 2005, Blood.

[57] S. Rosenberg,et al. T Lymphocyte-Directed Gene Therapy for ADA− SCID: Initial Trial Results After 4 Years , 1995, Science.

[58] R. Nagel,et al. High-level β-globin expression and preferred intragenic integration after lentiviral transduction of human cord blood stem cells , 2004 .

[59] P. Jolicoeur,et al. Mapping the viral sequences conferring leukemogenicity and disease specificity in Moloney and amphotropic murine leukemia viruses , 1984, Journal of virology.

[60] E. Barklis,et al. Characterization of the Moloney murine leukemia virus stem cell-specific repressor binding site. , 1993, Virology.

[61] R. Ghirlando,et al. Chromatin boundaries and chromatin domains. , 2004, Cold Spring Harbor symposia on quantitative biology.

[62] T. Lu,et al. Transient in vivo selection of transduced peripheral blood cells using antifolate drug selection in rhesus macaques that received transplants with hematopoietic stem cells expressing dihydrofolate reductase vectors. , 2004, Blood.

[63] D. M. Spencer. Developments in suicide genes for preclinical and clinical applications. , 2000, Current opinion in molecular therapeutics.

[64] Christof von Kalle,et al. A serious adverse event after successful gene therapy for X-linked severe combined immunodeficiency. , 2003, The New England journal of medicine.

[65] D. Trono,et al. Self-Inactivating Lentivirus Vector for Safe and Efficient In Vivo Gene Delivery , 1998, Journal of Virology.

[66] D. Bartel. MicroRNAs Genomics, Biogenesis, Mechanism, and Function , 2004, Cell.

[67] Christof von Kalle,et al. Side effects of retroviral gene transfer into hematopoietic stem cells. , 2003, Blood.

[68] C. Croce,et al. Frequent deletions and down-regulation of micro- RNA genes miR15 and miR16 at 13q14 in chronic lymphocytic leukemia , 2002, Proceedings of the National Academy of Sciences of the United States of America.

[69] R. Schreiber,et al. The immunobiology of cancer immunosurveillance and immunoediting. , 2004, Immunity.

[70] V. Corces,et al. The gypsy retrotransposon of Drosophila melanogaster: mechanisms of mutagenesis and interaction with the suppressor of Hairy-wing locus. , 1989, Developmental genetics.

[71] T. Rabbitts,et al. Activation of the T-cell oncogene LMO2 after gene therapy for X-linked severe combined immunodeficiency. , 2004, The New England journal of medicine.

[72] Sridhar Hannenhalli,et al. Genome-wide analysis of retroviral DNA integration , 2005, Nature Reviews Microbiology.

[73] A. West,et al. Insulators: many functions, many mechanisms. , 2002, Genes & development.

[74] Christof von Kalle,et al. Distinct Genomic Integration of MLV and SIV Vectors in Primate Hematopoietic Stem and Progenitor Cells , 2004, PLoS biology.

[75] Kathryn L. Parsley,et al. Failure of SCID-X1 gene therapy in older patients. , 2005, Blood.

[76] A. Fischer,et al. Severe combined immunodeficiency. A model disease for molecular immunology and therapy , 2005, Immunological reviews.

[77] A. Hotz-Wagenblatt,et al. Insertion of retroviral vectors in NOD/SCID repopulating human peripheral blood progenitor cells occurs preferentially in the vicinity of transcription start regions and in introns. , 2004, Molecular therapy : the journal of the American Society of Gene Therapy.

[78] W. Ludwig,et al. TTG-2, a new gene encoding a cysteine-rich protein with the LIM motif, is overexpressed in acute T-cell leukaemia with the t(11;14)(p13;q11). , 1991, Oncogene.

[79] Christine Kinnon,et al. Mutations in TNFRSF13B Encoding TACI Are Associated With Common Variable Immunodeficiency in Humans , 2006, Pediatrics.

[80] Lung-Ji Chang,et al. RNA 3′ Readthrough of Oncoretrovirus and Lentivirus: Implications for Vector Safety and Efficacy , 2002, Journal of Virology.

[81] B. Fehse,et al. Clonal Dominance of Hematopoietic Stem Cells Triggered by Retroviral Gene Marking , 2005, Science.

[82] J. Claverie. Fewer Genes, More Noncoding RNA , 2005, Science.

[83] R. Mulligan,et al. Effects of retroviral vector design on expression of human adenosine deaminase in murine bone marrow transplant recipients engrafted with genetically modified cells. , 1995, Proceedings of the National Academy of Sciences of the United States of America.

[84] F. Pedersen,et al. Alleviation of murine leukemia virus repression in embryonic carcinoma cells by genetically engineered primer binding sites and artificial tRNA primers. , 2000, Virology.

[85] E. Golemis,et al. Disease specificity of nondefective Friend and Moloney murine leukemia viruses is controlled by a small number of nucleotides , 1987, Journal of virology.

[86] Jody A. Vandergriff,et al. Prolonged multilineage clonal hematopoiesis in a rhesus recipient of CD34 positive cells marked with a RD114 pseudotyped oncoretroviral vector. , 2003, Blood cells, molecules & diseases.

[87] C. Bordignon,et al. Retroviral vector integration deregulates gene expression but has no consequence on the biology and function of transplanted T cells , 2006, Proceedings of the National Academy of Sciences of the United States of America.

[88] Cheng Cheng,et al. Improved outcome for children with acute lymphoblastic leukemia: results of Total Therapy Study XIIIB at St Jude Children's Research Hospital. , 2004, Blood.

[89] C. Bordignon,et al. Suicide-Gene-Transduced Donor T-Cells for Controlled Graft-versus-Host Disease and Graft-Versus-Tumor , 2002, International journal of hematology.

[90] C. von Kalle,et al. Polyclonal long-term repopulating stem cell clones in a primate model. , 2002, Blood.

[91] N. Copeland,et al. Gene Therapy Insertional Mutagenesis Insights , 2004, Science.

[92] M. Sadelain,et al. Occurrence of leukaemia following gene therapy of X-linked SCID , 2003, Nature Reviews Cancer.

[93] C. von Kalle,et al. Stem cell clonality and genotoxicity in hematopoietic cells: gene activation side effects should be avoidable. , 2004, Seminars in hematology.

[94] C. von Kalle,et al. Acute myeloid leukemia is associated with retroviral gene transfer to hematopoietic progenitor cells in a rhesus macaque. , 2006, Blood.

[95] D. H. Randle,et al. Tumor spectrum in ARF-deficient mice. , 1999, Cancer research.

[96] T. Rabbitts,et al. The effect of chromosomal translocations in acute leukemias: the LMO2 paradigm in transcription and development. , 1999, Cancer research.

[97] F. Bushman. Targeting Survival Integration Site Selection by Retroviruses and LTR-Retrotransposons , 2003, Cell.

[98] C. von Kalle,et al. Lentiviral vector transduction of NOD/SCID repopulating cells results in multiple vector integrations per transduced cell: risk of insertional mutagenesis. , 2003, Blood.

[99] M. Breindl,et al. Transcriptionally active genome regions are preferred targets for retrovirus integration , 1990, Journal of virology.

[100] M. Cavazzana‐Calvo,et al. The future of gene therapy , 2004, Nature.

[101] J. Kaiser,et al. As Gelsinger Case Ends, Gene Therapy Suffers Another Blow , 2005, Science.

[102] H. Varmus,et al. Retroviral integration into minichromosomes in vitro. , 1992, The EMBO journal.

[103] David A. Williams,et al. Chance or necessity? Insertional mutagenesis in gene therapy and its consequences. , 2003, Molecular therapy : the journal of the American Society of Gene Therapy.

[104] P. Kantoff,et al. Self-inactivating retroviral vectors designed for transfer of whole genes into mammalian cells. , 1986, Proceedings of the National Academy of Sciences of the United States of America.

[105] C. von Kalle,et al. Clonal evidence for the transduction of CD34+ cells with lymphomyeloid differentiation potential and self-renewal capacity in the SCID-X1 gene therapy trial. , 2005, Blood.

[106] J. Roberts,et al. Hematopoietic stem-cell transplantation for the treatment of severe combined immunodeficiency. , 1999, The New England journal of medicine.

[107] G. Stamatoyannopoulos,et al. Development of virus vectors for gene therapy of beta chain hemoglobinopathies: flanking with a chromatin insulator reduces gamma-globin gene silencing in vivo. , 2002, Blood.

[108] F. Deist,et al. Gene therapy of human severe combined immunodeficiency (SCID)-X1 disease. , 2000, Science.

[109] F. Bushman,et al. Human immunodeficiency virus integrase directs integration to sites of severe DNA distortion within the nucleosome core. , 1994, Proceedings of the National Academy of Sciences of the United States of America.

[110] M. Relling,et al. High incidence of secondary brain tumours after radiotherapy and antimetabolites , 1999, The Lancet.

[111] U. Choi,et al. Progress toward effective gene therapy for chronic granulomatous disease. , 2004, Japanese journal of infectious diseases.

[112] F. Behm,et al. Granulocyte colony-stimulating factor and the risk of secondary myeloid malignancy after etoposide treatment. , 2003, Blood.

[113] Bob Löwenberg,et al. High EVI1 expression predicts poor survival in acute myeloid leukemia: a study of 319 de novo AML patients. , 2003, Blood.

[114] N. Copeland,et al. Insertional mutagenesis identifies genes that promote the immortalization of primary bone marrow progenitor cells. , 2005, Blood.

[115] B. Fehse,et al. Pois(s)on – It's a Question of Dose… , 2004, Gene Therapy.

[116] G. Nucifora,et al. EVI1 induces myelodysplastic syndrome in mice. , 2004, The Journal of clinical investigation.

[117] H. Lodish,et al. MicroRNAs as regulators of mammalian hematopoiesis. , 2005, Seminars in immunology.

[118] J. Puck,et al. Lymphoid development and function in X-linked severe combined immunodeficiency mice after stem cell gene therapy. , 2000, Molecular therapy : the journal of the American Society of Gene Therapy.

[119] A. Hagenbeek,et al. Safety of retroviral gene marking with a truncated NGF receptor , 2003, Nature Medicine.

[120] M. Ogawa,et al. Reversible expression of CD34 by adult human bone marrow long-term engrafting hematopoietic stem cells. , 2003, Experimental hematology.

[121] H L Robinson,et al. Acceptor sites for retroviral integrations map near DNase I-hypersensitive sites in chromatin , 1986, Journal of virology.

[122] D. Pinkel. Treatment of childhood acute lymphocytic leukemia. , 1970, The Journal of pediatrics.

[123] P. Brown,et al. Correct integration of retroviral DNA in vitro , 1987, Cell.

[124] K. Cornetta,et al. American Society of Gene Therapy (ASGT) ad hoc subcommittee on retroviral-mediated gene transfer to hematopoietic stem cells. , 2003, Molecular therapy : the journal of the American Society of Gene Therapy.

[125] Adam Bagg,et al. Fatal systemic inflammatory response syndrome in a ornithine transcarbamylase deficient patient following adenoviral gene transfer. , 2003, Molecular genetics and metabolism.

[126] F. Sigaux,et al. Genomic alterations of the p19ARF encoding exons in T-cell acute lymphoblastic leukemia. , 1998, Blood.

[127] R. Frederickson. Report from the 2nd Stem Cell Clonality and Genotoxicity Retreat: St. Louis, MO, June 1, 2005. , 2005, Molecular therapy : the journal of the American Society of Gene Therapy.