IMPORTANCE: Wiskott-Aldrich syndrome is a rare primary immunodeficiency associated with severe microthrombocytopenia. Partially HLA antigen-matched allogeneic hematopoietic stem cell (HSC) transplantation is often curative but is associated with significant comorbidity. OBJECTIVE: To assess the outcomes and safety of autologous HSC gene therapy in Wiskott-Aldrich syndrome. DESIGN, SETTING, AND PARTICIPANTS: Gene-corrected autologous HSCs were infused in 7 consecutive patients with severe Wiskott-Aldrich syndrome lacking HLA antigen-matched related or unrelated HSC donors (age range, 0.8-15.5 years; mean, 7 years) following myeloablative conditioning. Patients were enrolled in France and England and treated between December 2010 and January 2014. Follow-up of patients in this intermediate analysis ranged from 9 to 42 months. INTERVENTION: A single infusion of gene-modified CD34+ cells with an advanced lentiviral vector. MAIN OUTCOMES AND MEASURES: Primary outcomes were improvement at 24 months in eczema, frequency and severity of infections, bleeding tendency, and autoimmunity and reduction in disease-related days of hospitalization. Secondary outcomes were improvement in immunological and hematological characteristics and evidence of safety through vector integration analysis. RESULTS: Six of the 7 patients were alive at the time of last follow-up (mean and median follow-up, 28 months and 27 months, respectively) and showed sustained clinical benefit. One patient died 7 months after treatment of preexisting drug-resistant herpes virus infection. Eczema and susceptibility to infections resolved in all 6 patients. Autoimmunity improved in 5 of 5 patients. No severe bleeding episodes were recorded after treatment, and at last follow-up, all 6 surviving patients were free of blood product support and thrombopoietic agonists. Hospitalization days were reduced from a median of 25 days during the 2 years before treatment to a median of 0 days during the 2 years after treatment. All 6 surviving patients exhibited high-level, stable engraftment of functionally corrected lymphoid cells. The degree of myeloid cell engraftment and of platelet reconstitution correlated with the dose of gene-corrected cells administered. No evidence of vector-related toxicity was observed clinically or by molecular analysis. CONCLUSIONS AND RELEVANCE: This study demonstrated the feasibility of the use of gene therapy in patients with Wiskott-Aldrich syndrome. Controlled trials with larger numbers of patients are necessary to assess long-term outcomes and safety.

Outcomes following gene therapy in patients with severe Wiskott-Aldrich syndrome / Hacein-Bey Abina, S.; Gaspar, H. B.; Blondeau, J.; Caccavelli, L.; Charrier, S.; Buckland, K.; Picard, C.; Six, E.; Himoudi, N.; Gilmour, K.; Mcnicol, A. -M.; Hara, H.; Xu-Bayford, J.; Rivat, C.; Touzot, F.; Mavilio, F.; Lim, A.; Treluyer, J. -M.; Heritier, S.; Lefrere, F.; Magalon, J.; Pengue-Koyi, I.; Honnet, G.; Blanche, S.; Sherman, E. A.; Male, F.; Berry, C.; Malani, N.; Bushman, F. D.; Fischer, A.; Thrasher, A. J.; Galy, A.; Cavazzana, M.. - In: JAMA. - ISSN 0098-7484. - 313:15(2015), pp. 1550-1563. [10.1001/jama.2015.3253]

Outcomes following gene therapy in patients with severe Wiskott-Aldrich syndrome

Mavilio F.;
2015

Abstract

IMPORTANCE: Wiskott-Aldrich syndrome is a rare primary immunodeficiency associated with severe microthrombocytopenia. Partially HLA antigen-matched allogeneic hematopoietic stem cell (HSC) transplantation is often curative but is associated with significant comorbidity. OBJECTIVE: To assess the outcomes and safety of autologous HSC gene therapy in Wiskott-Aldrich syndrome. DESIGN, SETTING, AND PARTICIPANTS: Gene-corrected autologous HSCs were infused in 7 consecutive patients with severe Wiskott-Aldrich syndrome lacking HLA antigen-matched related or unrelated HSC donors (age range, 0.8-15.5 years; mean, 7 years) following myeloablative conditioning. Patients were enrolled in France and England and treated between December 2010 and January 2014. Follow-up of patients in this intermediate analysis ranged from 9 to 42 months. INTERVENTION: A single infusion of gene-modified CD34+ cells with an advanced lentiviral vector. MAIN OUTCOMES AND MEASURES: Primary outcomes were improvement at 24 months in eczema, frequency and severity of infections, bleeding tendency, and autoimmunity and reduction in disease-related days of hospitalization. Secondary outcomes were improvement in immunological and hematological characteristics and evidence of safety through vector integration analysis. RESULTS: Six of the 7 patients were alive at the time of last follow-up (mean and median follow-up, 28 months and 27 months, respectively) and showed sustained clinical benefit. One patient died 7 months after treatment of preexisting drug-resistant herpes virus infection. Eczema and susceptibility to infections resolved in all 6 patients. Autoimmunity improved in 5 of 5 patients. No severe bleeding episodes were recorded after treatment, and at last follow-up, all 6 surviving patients were free of blood product support and thrombopoietic agonists. Hospitalization days were reduced from a median of 25 days during the 2 years before treatment to a median of 0 days during the 2 years after treatment. All 6 surviving patients exhibited high-level, stable engraftment of functionally corrected lymphoid cells. The degree of myeloid cell engraftment and of platelet reconstitution correlated with the dose of gene-corrected cells administered. No evidence of vector-related toxicity was observed clinically or by molecular analysis. CONCLUSIONS AND RELEVANCE: This study demonstrated the feasibility of the use of gene therapy in patients with Wiskott-Aldrich syndrome. Controlled trials with larger numbers of patients are necessary to assess long-term outcomes and safety.
2015
JAMA
313
15
1550
1563
WOS:000353198700020
2-s2.0-84928389399
25898053
Outcomes following gene therapy in patients with severe Wiskott-Aldrich syndrome / Hacein-Bey Abina, S.; Gaspar, H. B.; Blondeau, J.; Caccavelli, L.; Charrier, S.; Buckland, K.; Picard, C.; Six, E.; Himoudi, N.; Gilmour, K.; Mcnicol, A. -M.; Hara, H.; Xu-Bayford, J.; Rivat, C.; Touzot, F.; Mavilio, F.; Lim, A.; Treluyer, J. -M.; Heritier, S.; Lefrere, F.; Magalon, J.; Pengue-Koyi, I.; Honnet, G.; Blanche, S.; Sherman, E. A.; Male, F.; Berry, C.; Malani, N.; Bushman, F. D.; Fischer, A.; Thrasher, A. J.; Galy, A.; Cavazzana, M.. - In: JAMA. - ISSN 0098-7484. - 313:15(2015), pp. 1550-1563. [10.1001/jama.2015.3253]
Hacein-Bey Abina, S.; Gaspar, H. B.; Blondeau, J.; Caccavelli, L.; Charrier, S.; Buckland, K.; Picard, C.; Six, E.; Himoudi, N.; Gilmour, K.; Mcnicol, A. -M.; Hara, H.; Xu-Bayford, J.; Rivat, C.; Touzot, F.; Mavilio, F.; Lim, A.; Treluyer, J. -M.; Heritier, S.; Lefrere, F.; Magalon, J.; Pengue-Koyi, I.; Honnet, G.; Blanche, S.; Sherman, E. A.; Male, F.; Berry, C.; Malani, N.; Bushman, F. D.; Fischer, A.; Thrasher, A. J.; Galy, A.; Cavazzana, M.
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