| Literature DB >> 27099176 |
Suk See De Ravin1, Xiaolin Wu2, Susan Moir3, Sandra Anaya-O'Brien4, Nana Kwatemaa4, Patricia Littel4, Narda Theobald4, Uimook Choi4, Ling Su2, Martha Marquesen4, Dianne Hilligoss4, Janet Lee4, Clarissa M Buckner3, Kol A Zarember4, Geraldine O'Connor5, Daniel McVicar5, Douglas Kuhns2, Robert E Throm6, Sheng Zhou6, Luigi D Notarangelo7, I Celine Hanson8, Mort J Cowan9, Elizabeth Kang4, Coleen Hadigan3, Michael Meagher6, John T Gray10, Brian P Sorrentino6, Harry L Malech1.
Abstract
X-linked severe combined immunodeficiency (SCID-X1) is a profound deficiency of T, B, and natural killer (NK) cell immunity caused by mutations inIL2RGencoding the common chain (γc) of several interleukin receptors. Gamma-retroviral (γRV) gene therapy of SCID-X1 infants without conditioning restores T cell immunity without B or NK cell correction, but similar treatment fails in older SCID-X1 children. We used a lentiviral gene therapy approach to treat five SCID-X1 patients with persistent immune dysfunction despite haploidentical hematopoietic stem cell (HSC) transplant in infancy. Follow-up data from two older patients demonstrate that lentiviral vector γc transduced autologous HSC gene therapy after nonmyeloablative busulfan conditioning achieves selective expansion of gene-marked T, NK, and B cells, which is associated with sustained restoration of humoral responses to immunization and clinical improvement at 2 to 3 years after treatment. Similar gene marking levels have been achieved in three younger patients, albeit with only 6 to 9 months of follow-up. Lentiviral gene therapy with reduced-intensity conditioning appears safe and can restore humoral immune function to posthaploidentical transplant older patients with SCID-X1.Entities:
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Year: 2016 PMID: 27099176 PMCID: PMC5557273 DOI: 10.1126/scitranslmed.aad8856
Source DB: PubMed Journal: Sci Transl Med ISSN: 1946-6234 Impact factor: 17.956