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Adenosine deaminase (ADA) enzyme deficiency results in severe combined immunodeficiency (SCID), a fatal autosomal recessive inherited immune disorder. Strimvelis (or GSK2696273) is a gene therapy intended for patients with ADA-SCID and for whom no suitable human leukocyte antigen (HLA) matched related stem cell donor is available. This therapy aims to restore ADA function in hematopoietic cell lineages, and in doing so prevents the pathology caused by purine metabolites (i.e., impaired immune function). This registry evaluates the long term safety and effectiveness outcomes of subjects who have received Strimvelis and is conducted as a post approval safety study associated with EMA marketing authorisation of Strimvelis™. In this study will be also included patients for whom the gene therapy medicinal product has been prepared starting from mobilized peripheral blood (mPB)-derived CD34+ cells (mPB-GT).
This is a prospective and retrospective, non-interventional follow-up registry of patients with ADA-SCID treated with Strimvelis™. The registry does not have a comparator group and the product will have been given on a single occasion prior to entering this registry. Safety and effectiveness will be assessed for a target number of 50 patients who will have received Strimvelis™ or GSK2696273 or mPB-GT. The end of enrollment will be after the recruitment of the 50th patient and the registry will close when the 50th patient finishes the 15- year follow-up.
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| Label | Type | Description | Intervention Names |
|---|---|---|---|
| ADA-SCID subjects treated with Strimvelis | Subjects with ADA-SCID who have received Strimvelis (previously GSK2696273) gene therapy, comprising patients treated prior to marketing authorisation (i.e. clinical studies and compassionate use programs) and those treated after marketing authorisation. In this study will be also included patients for whom the gene therapy medicinal product has been prepared starting from mobilized peripheral blood (mPB)-derived CD34+ cells, treated under hospital exemption (HE) frame, according to the Italian Decree of the Ministry of Health, January 16th 2015, "Provisions on advanced therapy drugs prepared on a non-repetitive basis". |
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| Name | Type | Description | Arm Group Labels | Other Names |
|---|---|---|---|---|
| Strimvelis | Genetic | Strimvelis is a CD34+ cell enriched dispersion of human autologous bone marrow derived hematopoietic stem/progenitor cells transduced with a retroviral vector containing the human ADA gene. It will be administered as an intravenous infusion once only. In this study will be also included patients for whom the gene therapy medicinal product has been prepared starting from mobilized peripheral blood (mPB)-derived CD34+ cells, treated under hospital exemption (HE) frame, according to the Italian Decree of the Ministry of Health, January 16th 2015, "Provisions on advanced therapy drugs prepared on a non-repetitive basis". |
| Measure | Description | Time Frame |
|---|---|---|
| Frequency of adverse events of special interest | The following adverse events of interest will be evaluated:
The number (%) of patients experiencing AESIs in each of these categories along with the number of events will be summarized by System Organ Class (SOC) and Preferred Term (PT). | Up to 15 years |
| Frequency of reported AEs and SAEs/ADRs | The number (%) of patients experiencing AEs along with the number of events will be summarized by System Organ Class (SOC) and Preferred Term (PT).
| Up to 15 years |
| Actual values of laboratory blood test results (i.e. biochemistry, haematology) at each annual visits. | The baseline evaluation for each parameter will be the final evaluation prior to treatment with Strimvelis™. For each parameter, the actual value will be summarized at each annual visit using descriptive statistics. Laboratory evaluations will be flagged against the normal range as low/normal/high. For each parameter, the number (%) of subjects with evaluations that were low/normal/high relative to the normal range will be summarized by annual visit. Out of range values will be assessed for their clinical significance. For each parameter, the number (%) of subjects with clinically significant evaluations will be summarized by annual visit and at any time post-treatment. | At each annual visit up to 15 years |
| Measure | Description | Time Frame |
|---|---|---|
| Overall Survival | Number and cause of deaths and time to onset of fatal events will be summarised. Starting time will be the date of therapy administration. | Up to 15 years |
| Event (Intervention) free survival |
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Inclusion Criteria
There are no formal exclusion criteria for participation as this registry will follow all patients who have received Strimvelis™ or GSK2696273, or mPB-GT prior to enrollment, subject to informed consent.
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This registry will include all subjects who have received Strimvelis (or GSK2696273) or mPB-GT and consented to participate in the registry. A target number of 50 subjects will be enrolled in the registry.
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| Name | Affiliation | Role |
|---|---|---|
| Fondazione Telethon | Fondazione Telethon | Study Director |
| Facility | Status | City | State | ZIP | Country | Contacts |
|---|---|---|---|---|---|---|
| Ospedale San Raffaele | Milan | Lombardy | 20132 | Italy |
| PubMed Identifier | Type | Citation | Retractions |
|---|---|---|---|
| 38355973 | Derived | Migliavacca M, Barzaghi F, Fossati C, Rancoita PMV, Gabaldo M, Dionisio F, Giannelli S, Salerio FA, Ferrua F, Tucci F, Calbi V, Gallo V, Recupero S, Consiglieri G, Pajno R, Sambuco M, Priolo A, Ferri C, Garella V, Monti I, Silvani P, Darin S, Casiraghi M, Corti A, Zancan S, Levi M, Cesana D, Carlucci F, Pituch-Noworolska A, AbdElaziz D, Baumann U, Finocchi A, Cancrini C, Ladogana S, Meinhardt A, Meyts I, Montin D, Notarangelo LD, Porta F, Pasquet M, Speckmann C, Stepensky P, Tommasini A, Rabusin M, Karakas Z, Galicchio M, Leonardi L, Duse M, Guner SN, Di Serio C, Ciceri F, Bernardo ME, Aiuti A, Cicalese MP. Long-term and real-world safety and efficacy of retroviral gene therapy for adenosine deaminase deficiency. Nat Med. 2024 Feb;30(2):488-497. doi: 10.1038/s41591-023-02789-4. Epub 2024 Feb 14. |
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| ID | Term |
|---|---|
| D007153 | Immunologic Deficiency Syndromes |
| C531816 | Severe combined immunodeficiency due to adenosine deaminase deficiency |
| ID | Term |
|---|---|
| D007154 | Immune System Diseases |
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| Number (%) of subjects with fertility and positive pregnancy outcomes | Fertility and pregnancy related outcomes will be listed and/or summarised as appropriate. Number (%) of subjects with fertility and pregnancy outcome will be reported. If the registry remains open after an individual patient has been followed for 15 years post treatment, fertility and pregnancy related events and outcomes will continue to be solicited or spontaneously reported, every 2 years until the registry closes. | Up to 15 years |
| The number (%) of subjects with an abnormal retroviral insertion site (RIS) analysis. | Data from RIS will be collected only if an HCP has performed these tests (e.g. following suspected malignancy or after a diagnosis of malignancy). The number (%) of subjects with an abnormal result will be summarized. | Up to 15 years. |
Event (Intervention) free survival will be evaluated using the time in years from treatment with Strimvelis to either the first intervention (Hematopoietic Stem Cell Transplant or >3 months of Enzyme Replacement Therapy). Summary statistics, proportions and rates will be provided.
| Up to 15 years. |
| The number (%) of subjects requiring use of treatments of interest | The medications/treatments of interest in this study are ERT, HSCT, Immunoglobulins, radiotherapy and cytotoxic agents. Categorical responses for whether subjects have received these treatments are captured per annual visit. The number (%) of subjects requiring each of these treatments and any of these treatments will be summarized at each annual visit throughout the follow-up period and overall. For ERT, the duration of treatment and number of patients requiring more than three months of continuous treatment will be summarized. | Up to 15 years. |
| Immune reconstitution | Peripheral lymphocytes and T cell function from response to mitogens will be evaluated. Actual counts and the change from baseline will be summarized at each annual visit using summary statistics (n, mean, 95% CI, SD, geometric mean, (gCV), minimum, median, maximum). | Baseline and annually up to 15 years. |
| Growth | Growth (i.e. height and weight) percentiles will be calculated and compared to World Health Organisation (WHO) standard growth charts. | Up to 15 years. |
| Systemic metabolite detoxification | Systemic metabolite detoxification will be assessed using dAXP levels in RBCs and ADA activity in plasma, RBCs and lymphocytes. Actual values and the change from baseline will be summarized at each annual visit using summary statistics (n, mean, 95% CI, SD, geometric mean, gCV, minimum, median, maximum). The geometric mean and 95% CI will be plotted over time. In addition, individual plots over time will be produced. Adequate ADA activity is defined as a level of >= 210 nmol/h/mg, adequate dAXP in RBC is defined as < 100 nmol/mL. The number (%) of patients with adequate levels of ADA activity and dAXP will be summarized. | Baseline and annually up to 15 years. |
| Vector copy number, measured in PBMCs (peripheral blood mononuclear cells) and subpopulations. | Vector copy number (VCN) will be measured in PBMCs and and subpopulations CD3+, CD4+, CD8+, CD19+, CD15+ and CD56+ cells and summarized. VCN will be summarized by visit using summary statistics (n, mean, 95% CI, SD, geometric mean, gCV, minimum, median, maximum). | Up to 15 years. |
| Number and proportion of patients with severe infections, and associated length of stay | Severe infections, defined as infections requiring hospitalization or prolonging hospitalization, will be identified from the adverse event data. The rate of infection will be calculated as number of severe infections divided by the person-years of observation after treatment with Strimvelis™. The cumulative number (%) of patients with severe infections and the cumulative rate of severe infections will be presented at each year post treatment along their 95% CI. | Up to 15 years. |
| The number (%) of subjects falling into each category for pediatric development and quality of life assessments | Pediatric development assessments will include:
| Up to 15 years. |
| Patient (or proxy) reported Peds-QL | Data from patient (or proxy) reported outcome measures and development questionnaires [e.g. Peds-QL] where they are used routinely as part of a physician's standard of care or where permitted by local authorities as non-interventional assessments, will also be summarised. Absolute scores will be calculated. | Up to 15 years. |
| Response to childhood vaccinations | Response to vaccinations against tetanus toxoid, diphtheria, pertussis, hepatitis B, hemophilius influenzae B (HIB), pneumococcus and measles, mumps and rubella (MMR) will be assessed. The number of subjects receiving each vaccination and any vaccination will be summarized along with the number (%) of those subjects with a positive response. The exact binomial 95% confidence interval will be provided for each response category of each vaccination type. | Up to 15 years. |