Gene Transfer for Severe Combined Immunodeficiency, X-linked (SCID-X1) Using a Self-inactivating (SIN) Gammaretroviral Vector
| Status: | Active, not recruiting |
|---|---|
| Conditions: | Infectious Disease, HIV / AIDS |
| Therapuetic Areas: | Immunology / Infectious Diseases |
| Healthy: | No |
| Age Range: | Any |
| Updated: | 5/30/2018 |
| Start Date: | April 2010 |
| End Date: | March 2033 |
Multi-institutional Phase I/II Trial Evaluating the Treatment of SCID-X1 Patients With Retrovirus-mediated Gene Transfer
Researchers are working on ways to treat SCID patients who don't have a matched brother or
sister. One of the goals is to avoid the problems that happen with stem cell transplant from
parents and unrelated people, such as repeat transplants, incomplete cure of the immune
system, exposure to chemotherapy, and graft versus host disease.
The idea behind gene transfer is to replace the broken gene by putting a piece of genetic
material (DNA) that has the normal gene into the child's cells. Gene transfer can only be
done if we know which gene is missing or broken in the patient. For SCID-X1, gene transfer
has been done in the laboratory and in two previous clinical trials by inserting the normal
gene into stem cells from bone marrow. The bone marrow is the "factory" inside the bones that
creates blood and immune cells. So fixing the gene in the bone marrow stem cells should fix
the immune problem, without giving chemotherapy and without risk of graft versus host
disease, because the child's own cells are used, rather than another person's. Out of the 20
subjects enrolled in the two previous trials, 18 are alive with better immune systems after
gene transfer. Two of the surviving subjects received gene corrected cells over 10 years ago.
Gene transfer is still research for two reasons. One is that not enough children have been
studied to tell if the procedure is consistently successful. Of the 20 children enrolled in
the previous two trials, one child did not have correction of the immune system, and died of
complications after undergoing stem cell transplant. The second important reason why gene
transfer is research is that we are still learning about the side effects of gene transfer
and how to do gene transfer safely. In the last two trials, 5 children have experienced a
serious side effect. These children developed leukemia related to the gene transfer itself.
Leukemia is a cancer of the white blood cells, a condition where a few white blood cells grow
out of control. Of these children, 4 of the 5 have received chemotherapy (medication to treat
cancer) and are currently in remission (no leukemia can be found by sensitive testing),
whereas one died of gene transfer-related leukemia.
sister. One of the goals is to avoid the problems that happen with stem cell transplant from
parents and unrelated people, such as repeat transplants, incomplete cure of the immune
system, exposure to chemotherapy, and graft versus host disease.
The idea behind gene transfer is to replace the broken gene by putting a piece of genetic
material (DNA) that has the normal gene into the child's cells. Gene transfer can only be
done if we know which gene is missing or broken in the patient. For SCID-X1, gene transfer
has been done in the laboratory and in two previous clinical trials by inserting the normal
gene into stem cells from bone marrow. The bone marrow is the "factory" inside the bones that
creates blood and immune cells. So fixing the gene in the bone marrow stem cells should fix
the immune problem, without giving chemotherapy and without risk of graft versus host
disease, because the child's own cells are used, rather than another person's. Out of the 20
subjects enrolled in the two previous trials, 18 are alive with better immune systems after
gene transfer. Two of the surviving subjects received gene corrected cells over 10 years ago.
Gene transfer is still research for two reasons. One is that not enough children have been
studied to tell if the procedure is consistently successful. Of the 20 children enrolled in
the previous two trials, one child did not have correction of the immune system, and died of
complications after undergoing stem cell transplant. The second important reason why gene
transfer is research is that we are still learning about the side effects of gene transfer
and how to do gene transfer safely. In the last two trials, 5 children have experienced a
serious side effect. These children developed leukemia related to the gene transfer itself.
Leukemia is a cancer of the white blood cells, a condition where a few white blood cells grow
out of control. Of these children, 4 of the 5 have received chemotherapy (medication to treat
cancer) and are currently in remission (no leukemia can be found by sensitive testing),
whereas one died of gene transfer-related leukemia.
Severe combined immunodeficiencies (SCID) are a heterogeneous group of inherited disorders
characterized by a profound reduction or absence of T lymphocyte function. They arise from a
variety of molecular defects which affect lymphocyte development and function. The most
common form of SCID is an X-linked form (SCID-X1) which accounts for 40-50% of all cases.
SCID-X1 is caused by defects in the common cytokine receptor chain, which was originally
identified as a component of the high affinity interleukin-2 receptor (IL-2RG), but is now
known to be an essential component of the IL-4, -7, -9 -15, and -21 cytokine receptor
complexes. Classic SCID-X1 has an extremely poor prognosis without treatment. Death usually
occurs in the first year of life from infectious complications unless definitive treatment
can be administered. Until the recent advent of somatic gene therapy, hematopoietic stem cell
transplantation (HSCT) offered the only curative option for patients with any form of SCID.
If a genotypically matched sibling donor is available, HSCT is a highly successful procedure.
However a genotypically matched family donor is only available for approximately 30% of
patients. For the remaining individuals, alternative donor transplants, principally from
matched unrelated or haploidentical parental donors have been performed. These approaches are
still problematic with toxicity from ablative therapy, graft-versus-host disease and
incomplete lymphoid reconstitution. Recent gene transfer trials have documented the efficacy
of gene transfer in this disease, albeit with toxicity related to insertional mutagenesis. A
new generation of self-inactivating (SIN) vectors has been developed which lack all
enhancer-promoter elements of the LTR U3 region and are also devoid of all gammaretroviral
coding regions. A SIN vector expressing the IL-2RG gene, pSRS11.EFS.IL2RG.pre* has been
developed and has shown a reduction in mutagenic potential compared to LTR configuration in
non-clinical studies. The current study is a phase I/II trial of somatic gene therapy for
patients with SCID-X1.
characterized by a profound reduction or absence of T lymphocyte function. They arise from a
variety of molecular defects which affect lymphocyte development and function. The most
common form of SCID is an X-linked form (SCID-X1) which accounts for 40-50% of all cases.
SCID-X1 is caused by defects in the common cytokine receptor chain, which was originally
identified as a component of the high affinity interleukin-2 receptor (IL-2RG), but is now
known to be an essential component of the IL-4, -7, -9 -15, and -21 cytokine receptor
complexes. Classic SCID-X1 has an extremely poor prognosis without treatment. Death usually
occurs in the first year of life from infectious complications unless definitive treatment
can be administered. Until the recent advent of somatic gene therapy, hematopoietic stem cell
transplantation (HSCT) offered the only curative option for patients with any form of SCID.
If a genotypically matched sibling donor is available, HSCT is a highly successful procedure.
However a genotypically matched family donor is only available for approximately 30% of
patients. For the remaining individuals, alternative donor transplants, principally from
matched unrelated or haploidentical parental donors have been performed. These approaches are
still problematic with toxicity from ablative therapy, graft-versus-host disease and
incomplete lymphoid reconstitution. Recent gene transfer trials have documented the efficacy
of gene transfer in this disease, albeit with toxicity related to insertional mutagenesis. A
new generation of self-inactivating (SIN) vectors has been developed which lack all
enhancer-promoter elements of the LTR U3 region and are also devoid of all gammaretroviral
coding regions. A SIN vector expressing the IL-2RG gene, pSRS11.EFS.IL2RG.pre* has been
developed and has shown a reduction in mutagenic potential compared to LTR configuration in
non-clinical studies. The current study is a phase I/II trial of somatic gene therapy for
patients with SCID-X1.
Inclusion Criteria:
1. Diagnosis of SCID-X1 based on immunophenotype (<200 CD3+ autologous T cells, and
confirmed by DNA sequencing)
AND
2. Lack an HLA identical (A, B, C, DR, DQ) related donor
AND either one of the following:
1. Patients in good clinical condition who do not have a readily available HLA identical
(A,B,C,DR,DQ) unrelated donor (readily available defined as: a donor confirmed within 6
weeks of searching, with ability to transplant within 3 months of diagnosis).
2. Patients with an active, therapy-resistant infection or other medical conditions that
significantly increase the risk of allogeneic transplant. Examples of "therapy-resistant
infections that significantly increase the risk of allogeneic transplant" include but are
not limited to:
1. interstitial pneumonia due to adenovirus or parainfluenzae virus.
2. protracted diarrhea requiring total parenteral nutrition.
3. disseminated BCG infection.
4. virus-induced lymphoproliferative disease.
5. any active opportunistic infection (eg, due to Pneumocystis jiroveci,
cytomegalovirus,cryptosporidium) that does not improve on medical management.
6. active and progressive pulmonary disease requiring mechanic ventilation. Inclusion of
patients with disease-related organ dysfunction is justified by the known poor outcome
with standard treatment and the potential life-saving nature of the treatment
proposed. Patients who are on high-dose steroids or other immunosuppressive agents
will also be considered eligible, because use of these drugs is common in patients
with SCID and maternal T cell engraftment or who present with severe interstitial lung
disease. Use of immunosuppressive drugs does not affect efficacy of hematopoietic cell
transplantation, and therefore should not affect efficacy of gene transfer.
Exclusion Criteria:
1. No available molecular diagnosis confirming SCID-X1.
2. Patients who have an available HLA-identical related donor.
3. Diagnosis of active malignant disease other than EBV-associated lymphoproliferative
disease
4. Patients with evidence of infection with HIV-1
5. Previous gene transfer
6. Major (life-threatening) congenital anomalies. Examples of "major (life-threatening)
congenital anomalies" include, but are not limited to: unrepaired cyanotic heart
disease, hypoplastic lungs, anencephaly or other major CNS malformations, other severe
non-repairable malformations of the gastrointestinal or genitourinary tracts that
significantly impair organ function.
7. Other conditions which in the opinion of the P.I. or co-investigators, contra-indicate
collection and/or infusion of transduced cells or indicate patient's inability to
follow the protocol. These may include for example clinical ineligibility to receive
anesthesia, severe deterioration of clinical condition of the patient after collection
of bone marrow but before infusion of transduced cells, or documented refusal or
inability of the family to return for scheduled visits. There may be other unforeseen
rare circumstances that would result in exclusion of the patient, such as sudden loss
of legal guardianship.
Although the presentation of the disease may be variable in type, the severity of the
immunodeficiency is uniform. The gene transfer protocol will be instituted in the place of
haploidentical transplant for those patients who do not have a matched family donor or in
whom an unrelated donor transplant is not indicated for the reasons specified above. Apart
from the gene transfer protocol, the patients will not undergo additional procedures that
would not form part of an equivalent haploidentical transplantation regimen, and will not
receive conditioning chemotherapy.
We found this trial at
3
sites
Cincinnati, Ohio 45267
Principal Investigator: Rebecca Marsh, MD
Phone: 513-803-1139
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Boston, Massachusetts 02115
Principal Investigator: Sung-Yun Pai, MD
Phone: 617-919-2508
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Los Angeles, California 90095
Principal Investigator: Donald B Kohn, MD
Phone: 310-794-1964
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