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Outcome of Hematopoietic Stem Cell Gene Therapy for Wiskott-Aldrich Syndrome

Authors :
Myriam Armant
Luigi D. Notarangelo
Safa Baris
Wendy B. London
Emily Morris
Akihiko Saitoh
Jet van der Spek
Roxane Labrosse
Vy Do Uyen Vu
Alejandra King
Stephanie Koo
Lisa R. Forbes
Lyanna R. Kessler
Jenny M. Despotovic
Julia Chu
Alexandra Miggelbrink
Sung-Yun Pai
Ahmet Ozen
Brenda Mackinnon
David A. Williams
Frederic D. Bushman
Anne Galy
John K. Everett
Johnson Fong
Colleen Dansereau
Thi Mai Anh Thi Nguyen
Hayley Raymond
Takayuki Takachi
Labrosse, Roxane
Chu, Julia
Armant, Myriam
van der Spek, Jet
Miggelbrink, Alexandra
Fong, Johnson
Everett, John K.
Raymond, Hayley
Kessler, Lyanna
Dansereau, Colleen
Mackinnon, Brenda
Koo, Stephanie
Morris, Emily
London, Wendy B.
Ozen, Ahmet
Baris, Safa
Despotovic, Jenny M.
Forbes, Lisa
Saitoh, Akihiko
Takachi, Takayuki
King, Alejandra
Thi Mai Anh Thi Nguyen
Vy Do Uyen Vu
Bushman, Frederic D.
Galy, Anne
Notarangelo, Luigi
Williams, David A.
Pai, Sung-Yun
Source :
Blood. 134:4629-4629
Publication Year :
2019
Publisher :
American Society of Hematology, 2019.

Abstract

Background Wiskott-Aldrich syndrome (WAS) is a rare X-linked disorder characterized by combined immunodeficiency, eczema, microthrombocytopenia, infections, autoimmunity and lymphoma. Gene therapy (GT) using autologous CD34+ cells is an emerging alternative treatment with advantages over standard allogeneic hematopoietic stem cell transplant for patients who lack well matched donors, avoiding graft-versus-host-disease. An initial experience with gene therapy using a γ-retroviral vector showed correction of hematological defects in 9/10 patients, but was aggravated by development of leukemia in 7 of them. We report the outcomes of a phase I/II clinical trial in which 5 WAS patients underwent GT using a self-inactivating lentiviral (SIN-LV) vector expressing the human WAS cDNA under the control of a 1.6kB fragment of the human WAS promoter. Subjects and Methods Five patients with severe WAS (clinical score 3-5) were enrolled at a median age of 1.8 years (1.4 - 8 years) at a single pediatric tertiary care center. WAS protein (WASP) was absent or markedly decreased in 2 and 3 subjects, respectively. Purified CD34+ cells from mobilized peripheral blood (n = 4) or both mobilized peripheral blood and bone marrow (n = 1) were transduced ex-vivo with the SIN-LV vector and re-infused after conditioning with busulfan (target AUC of 70-80 mg*h/L) and fludarabine (120mg/m2). The median dose of CD34+ cells infused was 9.8 x 106 cells/kg (6.3 - 24.9 x 106 cells/kg) with a mean vector copy number (VCN) of 1.7 copies/cell in CD34+ cells (0.54 - 3.37). In addition to eczema, thrombocytopenia and WAS-related infections in all patients, two subjects also had autoimmunity pre-GT, manifested as skin vasculitis and autoimmune cytopenias. Results All 5 subjects were alive and well at median follow-up of 4.8 years (2.5 - 5.9 years). Multi-lineage vector gene marking was sustained over time. All subjects had improvement or resolution of eczema and none have had any intercurrent severe infectious events. WASP expression measured by flow cytometry in T cells was increased over baseline in all patients, but remained below normal levels and correlated with VCN and cell dose received. Proliferation of T cells in response to anti-CD3, which was initially defective in 4/5 patients, improved post-GT. Humoral immune deficiency was also ameliorated, as evidenced by independence from Ig replacement and vaccine responses in those tested. All subjects remained platelet transfusion-free and none have had severe bleeding events. Platelet levels increased to >50 x 103 cells/uL in two patients with a VCN ≥2 in transduced stem cells and myeloid VCN ~1 copy/cell in neutrophils; the other 3 subjects sustained platelet counts No severe GT-related adverse events have occurred to date. Replication-competent lentivirus was not detected. Analysis of integration site distributions in five subjects showed reconstitution to be highly polyclonal, with no clones expanded to >20% of the transgene-marked cell population. To date, there have been no malignancies reported, either related to GT or WAS itself. Conclusion In summary, our data confirm and extend the safety and efficacy of GT in correcting disease manifestations associated with WAS, as seen in other studies using SIN-LV. Higher VCN in the drug product and in transduced stem cells correlated with better reconstitution of platelets and myeloid function. In contrast to other groups, we found in our study that patients with poor lymphocyte reconstitution post-GT may be at risk of ongoing autoimmunity despite high-level gene marking. Disclosures London: ArQule, Inc: Consultancy; United Therapeutics: Consultancy. Despotovic:Novartis: Research Funding; Amgen: Research Funding; Dova: Honoraria. Forbes:Takeda: Consultancy. Galy:Genethon: Employment. Williams:Novartis: Membership on an entity's Board of Directors or advisory committees; bluebird bio: Other: License of certain IP relevant to hemoglobinopathies. Potential for future royalty/milestone income. Received payment in past through BCH institutional licensing agreement., Research Funding; Orchard Therapeutics: Membership on an entity's Board of Directors or advisory committees, Other: Co-founder, potential for future royalty/milestone income, Research Funding; Alerion Biosciences: Membership on an entity's Board of Directors or advisory committees, Other: Co-founder. OffLabel Disclosure: CliniMACS technology for CD34+ cell selection

Details

ISSN :
15280020 and 00064971
Volume :
134
Database :
OpenAIRE
Journal :
Blood
Accession number :
edsair.doi.dedup.....7cead8c8d1684b78314fb9119c0d7f0a