Efficacy of Low Dose, SubQ Interleukin-2 (IL-2) to Expand Endogenous Regulatory T-Cells in Liver Transplant Recipients
| Status: | Recruiting |
|---|---|
| Healthy: | No |
| Age Range: | 18 - 65 |
| Updated: | 1/18/2019 |
| Start Date: | November 2016 |
| End Date: | June 2020 |
| Contact: | Susan McDermott, RN, MPH |
| Email: | smcderm2@bidmc.harvard.edu |
| Phone: | 617-632-9841 |
Efficacy of Low Dose, Subcutaneous Interleukin-2 (IL-2) to Expand Endogenous Regulatory T-Cells in Liver Transplant Recipients
The purpose of this investigation is to study if very low dose IL-2, given to liver
transplant patients by subcutaneous (under the skin) injections, over a 4 week period of
time, will cause an increase in the number of Treg cells in the blood.
transplant patients by subcutaneous (under the skin) injections, over a 4 week period of
time, will cause an increase in the number of Treg cells in the blood.
A common complication of organ transplantation is 'rejection' of the transplanted organ. This
occurs when the body's immune system tries to attack (or reject) the transplanted organ.
Drugs known as immunosuppressants (anti-rejection medications) are prescribed for patients
after transplantation to prevent rejection. But, anti-rejection medications are associated
with significant side effects including high blood pressure, high blood sugars, and high
cholesterol - all of which may increase the risk of heart and vascular complications.
Anti-rejection medications also increase the long-term risk of some types of cancer.
Sometimes, liver transplant patients who stop taking anti-rejection medications do not
experience rejection of their transplanted liver and the liver keeps working. These patients
are said to "tolerate" the transplanted liver, and this condition is referred to as
"tolerance". Doctors are working to learn more about why some liver transplant patients
develop tolerance after receiving a transplant, while others do not.
Studies have shown that patients who develop "tolerance" have an increase in a type of immune
cell called regulatory T-cells or "Tregs". This means Tregs may be important in preventing
rejection of a transplanted organ.
Studies have also shown that a human cytokine (a type of protein), called interleukin-2
(IL-2) aids in increasing the number of Treg cells in the body, and IL-2 has been given to
patients to successfully treat disorders of the immune system such as graft vs host disease -
a serious condition sometimes seen in patients after bone marrow transplantation.
The purpose of this investigation is to study if low dose IL-2, given to liver transplant
patients by subcutaneous (under the skin) injections, over a 4 week period of time, will
cause an increase in the number of Treg cells in the blood.
In addition, investigators will learn about the kinds of side effects low dose IL-2 will
cause and how severe those side effects will be.
occurs when the body's immune system tries to attack (or reject) the transplanted organ.
Drugs known as immunosuppressants (anti-rejection medications) are prescribed for patients
after transplantation to prevent rejection. But, anti-rejection medications are associated
with significant side effects including high blood pressure, high blood sugars, and high
cholesterol - all of which may increase the risk of heart and vascular complications.
Anti-rejection medications also increase the long-term risk of some types of cancer.
Sometimes, liver transplant patients who stop taking anti-rejection medications do not
experience rejection of their transplanted liver and the liver keeps working. These patients
are said to "tolerate" the transplanted liver, and this condition is referred to as
"tolerance". Doctors are working to learn more about why some liver transplant patients
develop tolerance after receiving a transplant, while others do not.
Studies have shown that patients who develop "tolerance" have an increase in a type of immune
cell called regulatory T-cells or "Tregs". This means Tregs may be important in preventing
rejection of a transplanted organ.
Studies have also shown that a human cytokine (a type of protein), called interleukin-2
(IL-2) aids in increasing the number of Treg cells in the body, and IL-2 has been given to
patients to successfully treat disorders of the immune system such as graft vs host disease -
a serious condition sometimes seen in patients after bone marrow transplantation.
The purpose of this investigation is to study if low dose IL-2, given to liver transplant
patients by subcutaneous (under the skin) injections, over a 4 week period of time, will
cause an increase in the number of Treg cells in the blood.
In addition, investigators will learn about the kinds of side effects low dose IL-2 will
cause and how severe those side effects will be.
Inclusion criteria:
1. Adult liver transplant recipients 2-4 years post transplantation
2. Male or female adult, age 18 - 65 years
3. Stable dosage of suppressant therapy for 1 month prior to study.
Exclusion criteria:
1. Recipient of multiple transplants (including solid organ, stem-cell, and bone marrow)
2. Serum liver panel (ALT, AST, Alkaline Phosphatase and Total Bilirubin) > 2 x ULN,
3. Serum creatinine > 1.5 x ULN,
4. eGFR of < 40 ml/min,
5. Detectable hepatitis viral load,
6. Abnormal ECG with clinically significant findings per study physician's judgement,
7. Active infection,
8. Presence or history of autoimmunity disorders,
9. Evidence of allograft rejection,
10. Liver biopsy or fibroscan evidence of advanced stage liver fibrosis (> Stage 2
Fibrosis),
11. Presence or history of cardiac or pulmonary disease,
12. Pregnant or nursing (lactating) women,
13. Health condition precludes participation in trial at study physician's judgment,
14. Inability to give consent.
We found this trial at
1
site
330 Brookline Ave
Boston, Massachusetts 02215
Boston, Massachusetts 02215
617-667-7000
Principal Investigator: Michael P Curry, MD
Phone: 617-632-9841
Beth Israel Deaconess Medical Center Beth Israel Deaconess Medical Center (BIDMC) is one of the...
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