Focal Segmental Glomerulosclerosis Clinical Trial
— AMP-FSGSOfficial title:
AMPK-activation by Metformin in FSGS: AMP-FSGS
The primary objective of this study is to determine whether extended-release MF (in addition to standard of care (S-o-C)) is superior to placebo in reducing podocyte injury and promoting podocyte survival by 6-months in Focal Segmental Glomerulosclerosis (FSGS).
| Status | Recruiting |
| Enrollment | 30 |
| Est. completion date | November 2027 |
| Est. primary completion date | November 2027 |
| Accepts healthy volunteers | No |
| Gender | All |
| Age group | 18 Years to 80 Years |
| Eligibility | Inclusion Criteria: 1. Provision of signed and dated informed consent form 2. Stated willingness to comply with all study procedures and availability for the duration of the study 3. Male or female, aged greater than or equal to 18 years, but </= 80 years age at the time of signing the informed consent 4. Biopsy-confirmed primary FSGS as defined by expert renal pathology at either institutions. For homogeneity of diagnoses, demonstrable segmental or global sclerosis lesions (>/=1 glomerulus) with diffuse podocyte foot process effacement by electron microscopy (>/+ 50% of examined glomerular tufts). 5. Therapeutic plan by treating physician for immunomodulatory treatment using Glucocorticoids. 6. Ability to take oral medication and be willing to adhere to the MF or Placebo regimen 7. For females of reproductive potential: use of highly effective contraception for at least 1 month prior to screening and agreement to use such a method during study participation and for an additional 12 weeks after the end of VPA administration. For males of reproductive potential: use of condoms or other methods to ensure effective contraception with partner. Exclusion Criteria: 1. Liver disease: confirmed cirrhosis liver (any stage), acute hepatitis (> 2 fold increase in liver enzymes, any coagulopathy, hyperbilirubinemia, ascites or encephalopathy) 2. estimated GFR < 32 ml/min 3. Diabetes Mellitus diagnosis at the time of biopsy or need for oral hypoglycemic agents/Insulin, or taking Metformin for other indications 4. Treatment with another investigational drug or other intervention within 3 months 5. Current pregnancy or desire to become pregnant during the study period 6. Unwilling to use two forms of birth control (for women of childbearing age) 7. Under hospice care 8. Confirmed Dementia diagnoses in EMR problem list 9. Incarceration 10. Homelessness 11. Inability to consent 12. Currently enrolled in (or completed within the past 30 days) a study of an investigational drug or device. 13. Life expectancy of less than 6 months as determined by the clinical judgement of the patient's primary physician 14. Allergy or sensitivity to Metformin 15. Platelet count < 100,000/µL; INR > 1.5; Bleeding diathesis or blood thinner use contraindicating biopsy. 16. Simultaneous use of Carbonic anhydrase inhibitor agents 17. Use of systemic immunosuppressive medication for non-renal indications. |
| Country | Name | City | State |
|---|---|---|---|
| United States | Yale New Haven Hospital | New Haven | Connecticut |
| United States | Mount Sinai Hospital | New York | New York |
| Lead Sponsor | Collaborator |
|---|---|
| Yale University | United States Department of Defense |
United States,
| Type | Measure | Description | Time frame | Safety issue |
|---|---|---|---|---|
| Other | Body Mass Index (BMI) | Measured in kg/m2. Exploratory outcome intended for evaluation of adverse effects of metformin versus placebo. | 3 months post-randomization | |
| Other | Body Mass Index (BMI) | Measured in kg/m2. Exploratory outcome intended for evaluation of adverse effects of metformin versus placebo. | 6 months post-randomization | |
| Primary | Slope of urinary NPHS2:Creatinine ratio | Measure of podocinuria via evaluation of urine podocin mRNA(nphs2) (measured as number of molecules detected by qPCR in the collected urine pellet) over the creatinine concentration. Intended for evaluation of efficacy of metformin versus placebo. | 6 months following randomization | |
| Secondary | estimated Glomerular Filtration Rate (eGFR) | Calculated from serum creatinine (mg/dl) using the CKD-EPI formula. Intended for evaluation of efficacy of metformin versus placebo. | 6 months post-randomization | |
| Secondary | Slope of eGFR | Change in eGFR from randomization to 6 months by incorporating eGFR at all timepoints in study between baseline and 6 months post-randomization. eGFR calculated from serum creatinine (mg/dl) using the CKD-EPI formula. Intended for evaluation of efficacy of metformin versus placebo. | 6 months post-randomization | |
| Secondary | Urine protein:creatinine ratio | Calculated ratio of urine protein and creatinine, each collected from the electronic medical record. Intended for evaluation of clinical efficacy of metformin versus placebo. | 6 months post-randomization | |
| Secondary | Slope of urine protein:creatinine ratio | Change in urine protein:creatinine ratio from randomization to 6 months by incorporating urine protein:creatinine ratio at all timepoints in study between baseline and 6 months post-randomization. Intended for evaluation of clinical efficacy of metformin versus placebo. | 6 months post-randomization | |
| Secondary | Complete remission | Calculated as the number of patients in complete remission, defined as <0.5 gm urine protein excretion over 24 hours, or urine protein creatinine ratio < 0.5 at 6 months post-randomization. Intended for evaluation of clinical efficacy of metformin versus placebo. | 6 months post-randomization | |
| Secondary | Complete or partial remission | Calculated as the number of patients with complete remission (defined as <0.5 gm urine protein excretion over 24 hours, or urine protein creatinine ratio < 0.5) or partial remission (>50% reduction in proteinuria from pre-randomization). Intended for evaluation of clinical efficacy of metformin versus placebo. | 6 months post-randomization | |
| Secondary | Discontinuation of study drug | Number of patients who discontinued study drug for any reason within 6 months of randomization. Intended for evaluation of patient compliance of metformin use. | Within 6 months post-randomization | |
| Secondary | Modified Kidney Disease Quality of Life (KDQOL) score | Calculated as the mean (standard deviation) of all total scores. Total scores are calculated by combining scores of 8 subsections of the KDQOL, and range from 0 - 163, with higher scores representing better quality of life. Intended for evaluation of adverse effects of metformin versus placebo. | 1 month post-randomization | |
| Secondary | Modified Kidney Disease Quality of Life (KDQOL) score | Calculated as the mean (standard deviation) of all total scores. Total scores are calculated by combining scores of 8 subsections of the KDQOL, and range from 0 - 163, with higher scores representing better quality of life. Intended for evaluation of adverse effects of metformin versus placebo. | 6 months post-randomization | |
| Secondary | Hypoglycemia symptom scores | Calculated as the mean (standard deviation) of all total scores. Total scores are calculated by combining scores of 6 subsections of the questionnaire, and range from 0 - 18, with higher scores representing greater symptoms. Intended for evaluation of adverse effects of metformin versus placebo. | 6 months post-randomization | |
| Secondary | Gastrointenstinal symptom scores | Calculated as the mean (standard deviation) of all total scores. Total scores are calculated by combining scores of 15 subsections of the questionnaire, and range from 0 - 105, with higher scores representing greater symptoms. Intended for evaluation of adverse effects of metformin versus placebo. | 1 month post-randomization | |
| Secondary | Gastrointenstinal symptom scores | Calculated as the mean (standard deviation) of all total scores. Total scores are calculated by combining scores of 15 subsections of the questionnaire, and range from 0 - 105, with higher scores representing greater symptoms. Intended for evaluation of adverse effects of metformin versus placebo. | 6 months post-randomization | |
| Secondary | Kidney biopsy fibrosis scores | Evaluation of kidney fibrosis as measured by quantification of Masson's Trichrome staining under microscopy of biopsy at 6 months post-randomization. Scores will be grouped by the following: <10%, 10-25%, 25-50%, > 50%. Intended for evaluation of clinical efficacy of metformin versus placebo. | 6 months post-randomization | |
| Secondary | Number of patients with Lactate levels>2.5 | As determined from the electronic medical record. Intended for evaluation of adverse effects of metformin versus placebo. | Within 6 months post-randomization | |
| Secondary | Number of patients with Lactate levels>5 | As determined from the electronic medical record. Intended for evaluation of adverse effects of metformin versus placebo. | Within 6 months post-randomization | |
| Secondary | Number of patients with Vitamin B12 levels <lower limit of Normal | As determined from the electronic medical record. Intended for evaluation of adverse effects of metformin versus placebo. | Within 6 months post-randomization | |
| Secondary | Number of patients with serum glutamic-oxaloacetic transaminase (SGOT) >2 fold increase | As determined from the electronic medical record. Intended for evaluation of adverse effects of metformin versus placebo. | Within 6 months post-randomization | |
| Secondary | Number of patients with Serum Glutamic Pyruvic Transaminase (SGPT) >2 fold increase | As determined from the electronic medical record. Intended for evaluation of adverse effects of metformin versus placebo. | Within 6 months post-randomization | |
| Secondary | Number of patients with Serum amyloid P component (SAP) >2 fold increase | As determined from the electronic medical record. Intended for evaluation of adverse effects of metformin versus placebo. | Within 6 months post-randomization | |
| Secondary | Number of patients with Bililirubin-Total >2 | As determined from the electronic medical record. Intended for evaluation of adverse effects of metformin versus placebo. | Within 6 months post-randomization | |
| Secondary | Number of patients with Bilirubin indirect >1 | As determined from the electronic medical record. Intended for evaluation of adverse effects of metformin versus placebo. | Within 6 months post-randomization | |
| Secondary | Number of patients with hemoglobin (Hb) <9 | As determined from the electronic medical record. Intended for evaluation of disease progression and adverse effects of metformin versus placebo. | Within 6 months post-randomization | |
| Secondary | Number of patients with hematocrit (Hct) <27 | As determined from the electronic medical record. Intended for evaluation of disease progression and adverse effects of metformin versus placebo. | Within 6 months post-randomization | |
| Secondary | Number of patients with mean corpuscular volume (MCV) >100 | As determined from the electronic medical record. Intended for evaluation of disease progression and adverse effects of metformin versus placebo. | Within 6 months post-randomization | |
| Secondary | Number of patients with Total White Blood Cells (WBC) <1500 | As determined from the electronic medical record. Intended for evaluation of disease progression and adverse effects of metformin versus placebo. | Within 6 months post-randomization | |
| Secondary | Slope of Urine Nphs2 | Change in urine podocin mRNA(Nphs2), measured as number of molecules detected by qPCR in the collected urine pellet over the creatinine concentration. Slope measured by incorporating nphs2 measurements at all timepoints in study between baseline and 6 months post-randomization. Intended for evaluation of efficacy of metformin versus placebo. | 6 months post-randomization | |
| Secondary | Slope of Urine Aqp2 | Change in urine Aquaporin-2 mRNA(Aqp2), measured as number of molecules detected by qPCR in the collected urine pellet over the creatinine concentration. Slope measured by incorporating Aqp2 measurements at all timepoints in study between baseline and 6 months post-randomization. Intended for evaluation of efficacy of metformin versus placebo. | 6 months post-randomization | |
| Secondary | Slope of Urine Tgfb1 | Change in urine transforming growth factor-beta1 mRNA (Tgfb1), measured as number of molecules detected by qPCR in the collected urine pellet over the creatinine concentration. Slope measured by incorporating Tgfb1 measurements at all timepoints in study between baseline and 6 months post-randomization. Intended for evaluation of efficacy of metformin versus placebo. | 6 months post-randomization |
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