Overview
The purpose of this study is to compare the efficacy and safety of human umbilical cord mesenchymal stem cells and low-dose IL-2 in the treatment of LN
Description
Allogeneic MSC transplantation has shown significant efficacy and good safety in the treatment of refractory autoimmune diseases such as lupus nephritis (LN), and has a broad application prospect. One of its mechanisms is that MSCs up-regulates the production of IL-2 and promotes the production of Treg cells. The breakthrough in this technology has brought new hope for patients with autoimmune diseases. Some small sample studies at home and abroad have shown that low-dose IL-2 can be used to treat LN. Recently, the research team found that a single dose of IL-2 showed a longer effect than repeated low-dose MSCs. However, there is still a lack of prospective randomized studies to confirm that the efficacy of allogeneic MSC is better than that of low-dose IL-2. Therefore, carrying out this prospective randomized study will make a real breakthrough in the clinical application of MSC in SLE, and open up a new field for the treatment of SLE for the benefit of mankind.
Eligibility
Inclusion Criteria:
Only patients with active lupus nephritis who meet all of the following criteria are
eligible for inclusion in this study:
- Before random assignment, records show that it meets at least 4 of the 11 SLE
classification criteria recommended by ACR in 1997.
- Age: age > 18 years old, ≤ 65 years old when obtaining informed consent
- SLEDAI-2K score ≥ 6
- Urinary total protein / creatinine ratio > 1.0 or 24-hour urinary protein > 1.0g, with
or without microscopic hematuria
- If they are fertile, they must agree to use effective contraception during the trial.
- In the case of women of childbearing age, urinary pregnancy and serum pregnancy tests
should be negative.
- Voluntarily sign informed consent and comply with the requirements of the research
programme
Exclusion Criteria:
Patients who met any of the following criteria could not be enrolled in this study:
- Patients who had received rituximab or any other B cell depletion therapy within 24
weeks before screening; patients who received unstable doses of mycophenolate mofetil,
cyclophosphamide or other immunosuppressants (including Cyclosporine, Tacrolimus,
Tripterygium wilfordii, Leflunomide, Azathioprine, Iguratimod) within the first 12
weeks of screening. Received biological agents or small molecule targeted drugs for
immune diseases within 4 weeks before screening, such as Etanercept, Infliximab,
Adalimumab Solution, Golimumab, Belimumab, Tocilizumab or JAK inhibitors;
- Plasmapheresis or immunosorbent therapy within 12 weeks before screening.
- Accompanied by severe and uncontrolled cardiovascular diseases, nervous system
diseases, lung diseases, liver diseases, endocrine and gastrointestinal diseases.
- Current or recent (within 4 weeks before random allocation) a history of severe active
or recurrent bacterial, viral, fungal, parasitic or other infections (including, but
not limited to, tuberculosis and atypical mycobacterial diseases, hepatitis B and C,
HIV infection, herpes zoster, but excluding onychomycosis). Or any infected person who
needs hospitalization and intravenous antibiotic treatment within 4 weeks before
screening or any infected person who needs treatment within 2 weeks before screening.
- Any major surgery has been performed within 12 weeks before screening, or major
surgery is required during the study period, which the researchers believe will pose
an unacceptable risk to the patient;
- Live vaccine will be given within 12 weeks before random allocation, or live vaccine
is expected to be needed / received during the study (except for herpes zoster
vaccination).
- Patients with a history of malignant tumors, including solid tumors and hematological
malignancies (except for excised or cured basal cell carcinoma of the skin);
- Pregnant or lactating women.