DiGeorge Anomaly, Complete DiGeorge Anomaly, Complete Atypical DiGeorge Anomaly, Complete DiGeorge Syndrome, Complete Atypical DiGeorge Syndrome
Conditions
Keywords
DiGeorge Anomaly, Thymus Transplantation, DiGeorge Syndrome, Athymia, Parathyroid Transplantation, Hypocalcemia, Hypoparathyroidism, Low T cell numbers, Immunoreconstitution, Immunodeficiency, Complete DiGeorge Anomaly, Complete Atypical DiGeorge Anomaly, Complete DiGeorge Syndrome, Complete Atypical DiGeorge Syndrome, Cultured Thymus Tissue Implantation (CTTI)
Brief summary
The study purpose is to determine if cultured thymus tissue implantation (CTTI) (previously described as transplantation) with tailored immunosuppression based on the recipient's pre-implantation T cell population is a safe and effective treatment for complete DiGeorge anomaly. This study will also evaluate whether cultured thymus tissue implantation and parathyroid transplantation with immunosuppression is a safe and effective treatment for complete DiGeorge anomaly and hypoparathyroidism.
Detailed description
Complete DiGeorge anomaly is a congenital disorder characterized by athymia. Without successful treatment, children remain immunodeficient and usually die by age 2 years. In infants with complete DiGeorge anomaly and no T cells, cultured thymus tissue implantation (CTTI) without immunosuppression resulted in diverse T cell development and good T cell function. Some infants with no thymus have some T cells that presumably developed extrathymically; these T cells can reject a thymus graft. The purpose of this study is to tailor immunosuppression use for complete DiGeorge anomaly subjects who have some T cells and different T cell function levels. This protocol includes tailored immunosuppression regimens to allow subjects with different T cell function levels to be suppressed adequately. Patients with complete DiGeorge often have hypoparathyroidism, a life threatening condition. Successful CTTI does not result in improvement of the hypoparathyroidism. The patients must go to the clinic for frequent calcium levels and to the hospital for calcium infusions. These infants are at risk for seizures from low calcium. This study had a parental parathyroid transplant arm for subjects with hypoparathyroidism who require calcium replacement. Whether or not a subject was enrolled in the parathyroid arm, the immunosuppression regimen the subject received was dependent on the immune findings as stated in the clinical protocol.
Interventions
Potential thymus recipient subjects are screened for eligibility. Thymus donor (unrelated donor), and thymus donor's birth mother are screened for safety. CTTI is done under general anesthesia in the operating room. Cultured thymus tissue is implanted into the subject's quadriceps. Two to three months post CTTI, if medically stable, the subject undergoes allograft biopsy. At the time of implantation and biopsy, a skin biopsy is done. Immunosuppression is weaned as per protocol.
OTHERCultured Thymus Tissue Implantation and Parental Parathyroid Transplantation
For subjects w/ hypoparathyroidism, the subject may receive CTTI and parathyroid transplant. For parathyroid transplant, parental parathyroid donors are screened. Parathyroid is harvested from the parent who shares the most Human Leukocyte Antigens (HLA) alleles with the thymus donor. Parathyroid gland is minced and placed in quadriceps muscle; there is no dose. Parathyroid donors are monitored as outpatients until recipients' discharge. Recipients' calcium and PTH levels are monitored indefinitely. Potential thymus recipient subjects are screened for eligibility. Thymus donor (unrelated donor), and thymus donor's birth mother are screened for safety. CTTI is done under general anesthesia in the operating room. Cultured thymus tissue is implanted into the subject's quadriceps. Two to three months post CTTI, if medically stable, the subject undergoes allograft biopsy. At the time of CTTI and biopsy, a skin biopsy is done. Immunosuppression is weaned as per protocol.
PROCEDUREBlood Draw
Birth mothers of Thymus Recipients are asked to participate in the study and undergo phlebotomy to allow testing of T cell identity in the Complete DiGeorge subjects. If blood is not obtainable then a buccal swab may be done.
Three doses of 2 mg/kg IV (through a central venous catheter) prior to CTTI. Each dose of Rabbit anti-thymocyte globulin (RATGAM) is given over 12 hours. RATGAM is usually given on days-5, -4, and -3 prior to CTTI or CTTI and parathyroid transplantation. Medications (diphenhydramine, steroids, and acetaminophen) are given with rabbit anti-thymocyte globulin.
DRUGCyclosporine
In addition to RATGAM, subjects with typical cDGA with PHA responses \>50,000 cpm, or atypical cDGA with PHA response \<75,000cpm (when not on immunosuppression) or \<40,000 cpm to PHA while on immunosuppression, are started on cyclosporine (Csa) as soon as cDGA is diagnosed. Csa is continued with target trough levels of 180 to 220 ng/ml. If subject cannot tolerate Csa, Csa may be changed to tacrolimus (FK506) with target trough level 7 to 10 ng/ml. When trough levels are outside of range, dosing is modified appropriately. Csa may be given every 8 to 12 hours enterally or IV before and after CTTI. The Csa dose is dependent on T cell numbers and the target Csa trough levels. Csa is weaned as per protocol.
DRUGTacrolimus
If unable to tolerate cyclosporine, then tacrolimus is given. Tacrolimus may be given every 8 to 12 hours enterally or IV before and after the CTTI transplant. Tacrolimus dose is dependent on the T cell numbers and the target tacrolimus trough levels. Tacrolimus is weaned as per protocol.
Steroids IV or enterally may be given before and after CTTI or CTTI and parathyroid transplantation. Administration and dosage depends on T cell numbers and symptoms. Pre-transplant steroids may be used when pre-transplant T cells \>4,000cumm. Steroids are weaned as per protocol.
DRUGDaclizumab
In addition, subjects with Atypical DiGeorge with PHA responses \>75,000cpm while on no immunosuppression or PHA responses \>40,000cpm while on immunosuppression, Daclizumab 1 mg/kg single dose IV may be given depending on T cell counts. Administration of Daclizumab depends on T cell numbers and T cell activation. A single dose may be given after the administration of rabbit anti-thymocyte globulin and before CTTI. If Daclizumab is not given before CTTI, and, depending on the T cell numbers and T cell activation, a single dose of Daclizumab may be given 3-5 days after CTTI.
DRUGMycophenolate mofetil
In addition, subjects with Atypical DiGeorge with PHA responses \>75,000cpm while on no immunosuppression or PHA responses \>40,000cpm while on immunosuppression, Mycophenolate mofetil 15 mg/kg/dose every 8 hours IV or enterally may be given depending on T cell counts. Mycophenolate mofetil may be given if the T cell count remains elevated 5 days after CTTI. If MMF is given, the dose is 15 mg/kg IV. MMF may be stopped at 35 days after CTTI or continued for up to six months after CTTI.
Sponsors
National Institutes of Health (NIH)
National Institute of Allergy and Infectious Diseases (NIAID)
Eunice Kennedy Shriver National Institute of Child Health and Human Development (NICHD)
Sumitomo Pharma Switzerland GmbH
Study design
Allocation
NON_RANDOMIZED
Intervention model
PARALLEL
Primary purpose
TREATMENT
Masking
NONE
Eligibility
Sex/Gender
ALL
Healthy volunteers
No
Inclusion criteria
Thymus Transplantation Inclusion: * Must have 1 of following: 22q11 or 10p13 hemizygosity; hypocalcemia requiring replacement; congenital heart defect; CHARGE association or CHD7 mutation; or abnormal ears plus mother w/diabetes (type I, type II, gestational). * \<50 CD3+ T cells/cumm or \<50 CD3+ T cells/cumm that are CD62L+ CD45RA+ (cluster of differentiation 45RA) (naïve phenotype), or \<5% of CD3+ count being CD62L+ CD45RA+ Atypical DiGeorge: * Must have, or have had, a rash. If rash present, rash biopsy must show T cells in skin. If rash & adenopathy resolved, must have \>50/cumm T cells & naive T cell must be \<50/cumm or \<5% of T cells. Typical DiGeorge: * CD3+ CD45RA+ CD62L+ T cells \<50/mm3 or \<5% of total T cells Parathyroid Transplantation Additional Inclusion: * 2 studies in recipient which PTH\<5 pg/ml when ionized calcium \<1.1 mmol/L. Can be done anytime pre-tx; 1 must be done while at Duke Hospital. * Parent(s) willing & eligible to be donors Thymus Transplantation Exclusion: * Heart surgery \<4 wks pre-tx * Heart surgery anticipated w/in 3 months after proposed tx * Rejection by surgeon or anesthesiologist as surgical candidate * Lack of sufficient muscle tissue to accept transplant of 4 grams/m2 BSA * HIV infection * Prior attempts at immune reconstitution, such as bone marrow tx or previous thymus tx * CMV(\>500 copies/ml blood by PCR on 2 tests) * Ventilator dependence Parathyroid Donor Inclusion: * \>18 years of age * Serum calcium in normal range * Normal PTH function * HLA typing consistent with parentage * Not on anticoagulation or can come off * Parent chosen will share HLA-DR allele with thymus donor that was not inherited by the recipient. If no HLA matching at all, then either parent is acceptable if the parent meets other criteria. Parathyroid Donor Exclusion: * \<18 years old * Hypoparathyroidism-low PTH in presence of low serum calcium & high serum phosphate * Hyperparathyroidism(or history)-elevated PTH in presence of high serum calcium and low serum phosphate. * History of cancer * Donor only living involved parent/guardian of recipient * Evidence of HIV-1, HIV-2, HTLV-1, HTLV-2, syphilis, hepatitis B, hepatitis C, West Nile virus, or Chagas disease * Creutzfeldt Jakob disease (CJD) * Elevated liver function studies: AST, ALT, alkaline phosphatase \>3x upper normal limit * Receipt of xenograft or risk factors for SARS, CJD and/or smallpox exposure. {If CJD risk factors but not active disease, parent may give permission for parathyroid use.} * Urine CMV positive * Positive CMV IgM * Positive IgM anti-EBV VCA * On blood thinners and cannot stop for parathyroid donation * Elevated PT or PTT (\>ULN) * Platelets\<100,000 * Positive Toxoplasma IgM * Donor will receive a history and physical; may be excluded based on PI's medical judgment. * Hemoglobin \<9g/dl * Infectious head or neck lesion * Goiter on ultrasound * Abnormal fiberoptic laryngoscopy of vocal cords * HLA inconsistent with parentage * Pregnancy * Positive HSV IgG isn't exclusion; post-tx prophylaxis needed for recipient if donor is HSV IgG+. * Positive VZV IgG isn't exclusion; post-tx prophylaxis needed if donor is VZV IgG+. * Medical concern of independent otolaryngologist. * Concern by medical psychologist/social worker that potential donor isn't competent or does not understand risks. * Questionnaire responses can lead to exclusion. Mother of DiGeorge Inclusion: • Provides consent to use blood/buccal sample. No exclusions except unwillingness to consent; or, provide blood/buccal sample.
Design outcomes
Primary
| Measure | Time frame | Description |
|---|---|---|
| Survival at 1 Year Post-CTTI | 1 year post-CTTI | Survival at 1 year post cultured thymus tissue implantation was assessed using the Kaplan Meier Estimated Survival. This mathematical function estimates the survival for a certain length of time. |
Secondary
| Measure | Time frame | Description |
|---|---|---|
| Immune Reconstitution Efficacy - Total CD3 T Cells | 1 year post-CTTI | The development of total CD3 T cells at one year as measured using flow cytometry |
| Immune Reconstitution Efficacy - Total CD4 T Cells | 1 year post-CTTI | The development of total CD4 T cells at one year as measured using flow cytometry |
| Immune Reconstitution Efficacy - Total CD8 T Cells | 1 year post-CTTI | The development of total CD8 T cells at one year as measured using flow cytometry |
| Survival at 2 Years Post-CTTI | 2 years post-CTTI | Survival at 2 years post cultured thymus tissue implantation was assessed using the Kaplan Meier Estimated Survival. This mathematical function estimates the survival for a certain length of time. |
| Immune Reconstitution Efficacy - Naive CD8 T Cells | 1 year post-CTTI | The development of total naive CD8 T cells at one year as measured using flow cytometry |
| Immune Reconstitution Efficacy - Response to Mitogens | 1 year post-CTTI | Measurement of the T cell proliferative response to the mitogen phytohemagglutin (PHA). |
| Thymus Allograft Biopsy | 2 to 3 months post-CTTI | Evidence, on biopsy of the thymus tissue implanted in muscle, that shows the development of new T cells. |
| Immune Reconstitution Efficacy - Naive CD4 T Cells | 1 year post-CTTI | The development of total naive CD4 T cells at one year as measured using flow cytometry |
Countries
United States
Participant flow
Pre-assignment details
The goal of this study is survival of subjects after cultured thymus tissue implantation (CTTI) regardless of the immunosuppressive regimen or of parathyroid co-transplantation.
Participants by arm
| Arm | Count |
|---|---|
| Cultured Thymus Tissue Implantation With Immunosuppression Participants enrolled into cultured thymus tissue for implantation (previously described as transplantation) with immunosuppression were given immunosuppression based on the subject's pre-implantation T cell number and function. | 14 |
| Total | 14 |
Withdrawals & dropouts
| Period | Reason | FG000 |
|---|---|---|
| Overall Study | Death | 4 |
Baseline characteristics
| Characteristic | Cultured Thymus Tissue Implantation With Immunosuppression |
|---|---|
| Age, Categorical <=18 years | 14 Participants |
| Age, Categorical >=65 years | 0 Participants |
| Age, Categorical Between 18 and 65 years | 0 Participants |
| Age, Continuous | 248 days STANDARD_DEVIATION 161 |
| Race/Ethnicity, Customized American Indian or Alaska Native | 2 Participants |
| Race/Ethnicity, Customized Black or African American | 3 Participants |
| Race/Ethnicity, Customized More than One Race (Caucasian/Asian) | 1 Participants |
| Race/Ethnicity, Customized White | 8 Participants |
| Region of Enrollment United States | 14 Participants |
| Sex: Female, Male Female | 5 Participants |
| Sex: Female, Male Male | 9 Participants |
Adverse events
| Event type | EG000 affected / at risk |
|---|---|
| deaths Total, all-cause mortality | 4 / 14 |
| other Total, other adverse events | 14 / 14 |
| serious Total, serious adverse events | 13 / 14 |
Outcome results
Primary
Survival at 1 Year Post-CTTI
Survival at 1 year post cultured thymus tissue implantation was assessed using the Kaplan Meier Estimated Survival. This mathematical function estimates the survival for a certain length of time.
Time frame: 1 year post-CTTI
Population: The study was designed to assess survival, without regard to the immune suppression used. No participants were enrolled into Arm 2. No subjects received a parathyroid transplant. Therefore, results are reported for Arm 1 only.
| Arm | Measure | Value (NUMBER) |
|---|---|---|
| Cultured Thymus Tissue With Immunosuppression | Survival at 1 Year Post-CTTI | 71 % of participants who survive to 1 year |
Secondary
Immune Reconstitution Efficacy - Naive CD4 T Cells
The development of total naive CD4 T cells at one year as measured using flow cytometry
Time frame: 1 year post-CTTI
Population: Data were only included for the 1 year time point if a T cell count was performed in relevant time period. The study was designed to assess survival, without regard to the immune suppression used. No participants were enrolled into Arm 2. No subjects received a parathyroid transplant. Therefore, results are reported for Arm 1 only.
| Arm | Measure | Value (MEDIAN) |
|---|---|---|
| Cultured Thymus Tissue With Immunosuppression | Immune Reconstitution Efficacy - Naive CD4 T Cells | 156 cells/mm3 |
Secondary
Immune Reconstitution Efficacy - Naive CD8 T Cells
The development of total naive CD8 T cells at one year as measured using flow cytometry
Time frame: 1 year post-CTTI
Population: Data were only included for the 1 year time point if a T cell count was performed in the relevant time period. The study was designed to assess survival, without regard to the immune suppression used. No participants were enrolled into Arm 2. No subjects received a parathyroid transplant. Therefore, results are reported for Arm 1 only.
| Arm | Measure | Value (MEDIAN) |
|---|---|---|
| Cultured Thymus Tissue With Immunosuppression | Immune Reconstitution Efficacy - Naive CD8 T Cells | 37 cells/mm3 |
Secondary
Immune Reconstitution Efficacy - Response to Mitogens
Measurement of the T cell proliferative response to the mitogen phytohemagglutin (PHA).
Time frame: 1 year post-CTTI
Population: Data were only included for the 1 year time point if a testing was performed in the relevant time period. The study was designed to assess survival, without regard to the immune suppression used. No participants were enrolled into Arm 2. No subjects received a parathyroid transplant. Therefore, results are reported for Arm 1 only.
| Arm | Measure | Value (MEDIAN) |
|---|---|---|
| Cultured Thymus Tissue With Immunosuppression | Immune Reconstitution Efficacy - Response to Mitogens | 139189 counts per minute (cpm) |
Secondary
Immune Reconstitution Efficacy - Total CD3 T Cells
The development of total CD3 T cells at one year as measured using flow cytometry
Time frame: 1 year post-CTTI
Population: Data were only included for the 1 year time point if a CD3 T cell count was performed in relevant time period. The study was designed to assess survival, without regard to the immune suppression used. No participants were enrolled into Arm 2. No subjects received a parathyroid transplant. Therefore, results are reported for Arm 1 only.
| Arm | Measure | Value (MEDIAN) |
|---|---|---|
| Cultured Thymus Tissue With Immunosuppression | Immune Reconstitution Efficacy - Total CD3 T Cells | 726 cells/mm3 |
Secondary
Immune Reconstitution Efficacy - Total CD4 T Cells
The development of total CD4 T cells at one year as measured using flow cytometry
Time frame: 1 year post-CTTI
Population: Data were only included for the 1 year time point if a CD4 T cell count was performed in relevant time period. The study was designed to assess survival, without regard to the immune suppression used. No participants were enrolled into Arm 2. No subjects received a parathyroid transplant. Therefore, results are reported for Arm 1 only.
| Arm | Measure | Value (MEDIAN) |
|---|---|---|
| Cultured Thymus Tissue With Immunosuppression | Immune Reconstitution Efficacy - Total CD4 T Cells | 593 cells/mm3 |
Secondary
Immune Reconstitution Efficacy - Total CD8 T Cells
The development of total CD8 T cells at one year as measured using flow cytometry
Time frame: 1 year post-CTTI
Population: Data were only included for the 1 year time point if a CD8 T cell count was performed in relevant time period. The study was designed to assess survival, without regard to the immune suppression used. No participants were enrolled into Arm 2. No subjects received a parathyroid transplant. Therefore, results are reported for Arm 1 only.
| Arm | Measure | Value (MEDIAN) |
|---|---|---|
| Cultured Thymus Tissue With Immunosuppression | Immune Reconstitution Efficacy - Total CD8 T Cells | 145 cells/mm3 |
Secondary
Survival at 2 Years Post-CTTI
Survival at 2 years post cultured thymus tissue implantation was assessed using the Kaplan Meier Estimated Survival. This mathematical function estimates the survival for a certain length of time.
Time frame: 2 years post-CTTI
Population: The study was designed to assess survival, without regard to the immune suppression used. No participants were enrolled into Arm 2. No subjects received a parathyroid transplant. Therefore, results are reported for Arm 1 only.
| Arm | Measure | Value (NUMBER) |
|---|---|---|
| Cultured Thymus Tissue With Immunosuppression | Survival at 2 Years Post-CTTI | 71 % of participants who survive to 2 years |
Secondary
Thymus Allograft Biopsy
Evidence, on biopsy of the thymus tissue implanted in muscle, that shows the development of new T cells.
Time frame: 2 to 3 months post-CTTI
Population: Data were only included if the participant had a biopsy of the thymus tissue implanted. The study was designed to assess survival, without regard to the immune suppression used. No participants were enrolled into Arm 2. No subjects received a parathyroid transplant. Therefore, results are reported for Arm 1 only.
| Arm | Measure | Category | Value (COUNT_OF_PARTICIPANTS) |
|---|---|---|---|
| Cultured Thymus Tissue With Immunosuppression | Thymus Allograft Biopsy | Inconclusive for thymopoiesis | 3 Participants |
| Cultured Thymus Tissue With Immunosuppression | Thymus Allograft Biopsy | Evidence of thymopoiesis | 7 Participants |
| Cultured Thymus Tissue With Immunosuppression | Thymus Allograft Biopsy | Evidence of rejection | 0 Participants |