Lentiviral Gene Therapy Combined with Low-Dose Busulfan in Infants with SCID-X1

Ewelina Mamcarz(St. Jude Children's Research Hospital), Sheng Zhou(St. Jude Children's Research Hospital), Timothy Lockey(St. Jude Children's Research Hospital), Hossam A. Abdelsamed(St. Jude Children's Research Hospital), Shane J. Cross(St. Jude Children's Research Hospital), Guolian Kang(St. Jude Children's Research Hospital), Zhijun Ma(St. Jude Children's Research Hospital), Jose Condori(St. Jude Children's Research Hospital), Jola Dowdy(St. Jude Children's Research Hospital), Brandon M. Triplett(St. Jude Children's Research Hospital), Chen Li(St. Jude Children's Research Hospital), Gabriela Marón(St. Jude Children's Research Hospital), Juan Carlos Aldave Becerra(Hospital Nacional Cayetano Heredia), Joseph A. Church(Children's Hospital of Los Angeles), Elif Dokmeci(University of New Mexico), James T. Love(University of Oklahoma Health Sciences Center), Ana Carolina da Matta Ain(Universidade de Taubaté), Hedi van der Watt(Right to Care), Xing Tang(St. Jude Children's Research Hospital), William E. Janssen(St. Jude Children's Research Hospital), Byoung Y. Ryu(St. Jude Children's Research Hospital), Suk See De Ravin(National Institutes of Health), Mitchell J. Weiss(St. Jude Children's Research Hospital), Ben Youngblood(St. Jude Children's Research Hospital), Janel Long-Boyle(UCSF Benioff Children's Hospital), Stephen Gottschalk(St. Jude Children's Research Hospital), Michael M. Meagher(St. Jude Children's Research Hospital), Harry L. Malech(National Institutes of Health), Jennifer M. Puck(UCSF Benioff Children's Hospital), Morton J. Cowan(UCSF Benioff Children's Hospital), Brian P. Sorrentino(St. Jude Children's Research Hospital)
New England Journal of Medicine
April 17, 2019
10.1056/nejmoa1815408
Cited by 263Open Access
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Abstract

BACKGROUND: Allogeneic hematopoietic stem-cell transplantation for X-linked severe combined immunodeficiency (SCID-X1) often fails to reconstitute immunity associated with T cells, B cells, and natural killer (NK) cells when matched sibling donors are unavailable unless high-dose chemotherapy is given. In previous studies, autologous gene therapy with γ-retroviral vectors failed to reconstitute B-cell and NK-cell immunity and was complicated by vector-related leukemia. METHODS: complementary DNA to bone marrow stem cells after low-exposure, targeted busulfan conditioning in eight infants with newly diagnosed SCID-X1. RESULTS: Eight infants with SCID-X1 were followed for a median of 16.4 months. Bone marrow harvest, busulfan conditioning, and cell infusion had no unexpected side effects. In seven infants, the numbers of CD3+, CD4+, and naive CD4+ T cells and NK cells normalized by 3 to 4 months after infusion and were accompanied by vector marking in T cells, B cells, NK cells, myeloid cells, and bone marrow progenitors. The eighth infant had an insufficient T-cell count initially, but T cells developed in this infant after a boost of gene-corrected cells without busulfan conditioning. Previous infections cleared in all infants, and all continued to grow normally. IgM levels normalized in seven of the eight infants, of whom four discontinued intravenous immune globulin supplementation; three of these four infants had a response to vaccines. Vector insertion-site analysis was performed in seven infants and showed polyclonal patterns without clonal dominance in all seven. CONCLUSIONS: Lentiviral vector gene therapy combined with low-exposure, targeted busulfan conditioning in infants with newly diagnosed SCID-X1 had low-grade acute toxic effects and resulted in multilineage engraftment of transduced cells, reconstitution of functional T cells and B cells, and normalization of NK-cell counts during a median follow-up of 16 months. (Funded by the American Lebanese Syrian Associated Charities and others; LVXSCID-ND ClinicalTrials.gov number, NCT01512888.).

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