Overview
Biochemical Response to Interferon-Gamma in Subjects With Specific Gene Mutation in Chronic Granulomatous Disease
Status:
Terminated
Terminated
Trial end date:
2014-11-14
2014-11-14
Target enrollment:
0
0
Participant gender:
All
All
Summary
Background: - Chronic granulomatous disease (CGD) is an immunodeficiency disease in which white blood cells are unable to kill certain bacteria and fungi. People with CGD are more likely to develop recurrent life-threatening infections. Certain changes or mutations in genes contribute to the severity of CGD, and also appear to affect the success of treatment with interferon-gamma, a substance that is used to improve the immune system s ability to fight infection. Researchers are interested in studying changes in the immune system caused by interferon-gamma treatment of CGD in individuals with different mutations that cause CGD. Objectives: - To compare changes in the immune system caused by interferon-gamma treatment for CGD in individuals with different mutations that cause CGD. Eligibility: - Individuals of any age who have been diagnosed with CGD and have specific types of mutations that cause CGD (to be determined after testing). Design: - Participants will be screened with a medical history, physical examination, and blood and urine tests. Participants must weigh more than 11 kilograms (~24 pounds) to participate in the study. - Participants will receive injections of interferon-gamma once weekly for 4 weeks, twice weekly for 4 weeks, and then three times weekly for 4 weeks (a total of 24 injections). - Blood will be drawn periodically during treatment and for 8 weeks after the treatment, for a total of 21 weeks on the study. Participants will regularly provide information on their symptoms and responses to treatment to the study researchers.Phase:
Phase 4Accepts Healthy Volunteers?
NoDetails
Lead Sponsor:
National Institute of Allergy and Infectious Diseases (NIAID)Treatments:
Interferon-gamma
Interferons
Criteria
- INCLUSION CRITERIA:Subjects may be enrolled if they are:
1. Already are enrolled on an existing CGD protocol at the Clinical Center (and will
remain enrolled on their existing protocol);
2. Are included in one of the study cohorts listed below;
3. Male or female;
4. Able to comply with self-administration of a subcutaneous injection; and
5. Willing to have their blood samples stored for the duration of this study and for
future research.
Study Groups/Cohorts:
X-linked CGD Nonsense/Frameshift/RNA Processing/Deletion Mutations Cohort: Subjects in this
cohort must have X-linked CGD resulting from a documented nonsense, frameshift, RNA
processing, or deletion gene mutation. Subjects with other gene defects or for whom the
specific genetic defect has not been determined are not eligible for inclusion in this
cohort.
X-linked CGD Missense Mutation with Low Baseline Superoxide Production (less than or equal
to 2.5 nmol/10(6) cells/hr) Cohort: Subjects in this cohort must have X-linked CGD
resulting from a documented missense gene and superoxide production by cytochrome c
reduction assay at baseline of less than or equal to 2.5 nmol/10(6) cells/hr. Subjects with
other gene defects or for whom the specific genetic defect has not been determined are not
eligible for inclusion in this cohort.
X-linked CGD Missense Mutation with Higher Baseline Superoxide Production (greater than 2.5
nmol/10(6) cells/hr) Cohort: Subjects in this cohort must have X-linked CGD resulting from
a documented missense gene and superoxide production by cytochrome c reduction assay at
baseline of greater than 2.5 nmol/10(6) cells/hr. Subjects with other gene defects or for
whom the specific genetic defect has not been determined are not eligible for inclusion in
this cohort.
Autosomal Recessive p47phox CGD Cohort: Subjects in this cohort must have autosomal
recessive CGD resulting from a documented p47phox gene mutation. Subjects with other gene
defects or for whom the specific genetic defect has not been determined are not eligible
for inclusion in this cohort.
Autosomal Recessive p67phox CGD Cohort: Subjects in this cohort must have autosomal
recessive CGD resulting from a documented p67phox gene mutation. Subjects with other gene
defects or for whom the specific genetic defect has not been determined are not eligible
for inclusion in this cohort.
EXCLUSION CRITERIA:
Subjects are excluded from the study who:
1. Have undergone successful bone marrow transplantation;
2. Had a serious adverse reaction to IFN gamma in the past;
3. Are pregnant or breast feeding;
4. Weigh less than 11 kg;
5. Are currently on therapy with INF gamma;
6. Have any of the following medical conditions:
- Coronary artery disease;
- Hepatic disease and/or liver enzymes elevated above 3 times normal;
- Seizure disorder, or
- Severe myelosuppression (absolute neutrophil count less than1000 cells/mm(3)).
Participation of Minors: minor patients will be invited to participant in this study.
Participation of Women: Exposure to IFN gamma by the developing human fetus may be
detrimental. For this reason, women of childbearing-age will have a pregnancy test prior to
undergoing study procedures. Should a woman become pregnant or suspect that she is pregnant
while participating in this study, she should immediately inform study staff and her
primary care physician.
Pregnancy and Lactation: The effects of IFN gamma therapy on the developing fetus and
newborn infant have not been studied. Therefore, it is not recommended that subjects who
are pregnant or breast-feeding receive IFN gamma and they will be excluded from this study.