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NCT04472624 Clinical Trial

Short Term Induction of Ketosis in PKD

ADPKD Clinical Trial

RESET-PKD

Official title:
Short Term Induction of Ketosis in PKD

Clinical Trial Details — Status: Completed

Administrative data
NCT number NCT04472624
Other study ID # 20-1040
Secondary ID
Status Completed
Phase N/A
First received
Last updated
Start date July 1, 2020
Est. completion date July 1, 2021

Study information
Verified date September 2021
Source University of Cologne
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

Recently, it has been shown that ketose-inducing dietary interventions slow disease progression in animal models of polycystic kidney disease (PKD), even when the state of ketosis is only induced for a short period of time. The present study aims to investigate the effects of short term ketosis on total kidney volume (TKV) (and other parameters) in 10 ADPKD-patients with rapidly progressive disease.

Description:

Recently, dietary models inducing ketosis have been shown to inhibit disease progression in animal models of PKD. Those beneficial dietary models included time-restricted feeding (TRF) without caloric reduction, ad libitum administered ketogenic diet (KD) and acute short-term fasting in mouse, rat and feline models of PKD. In a PKD rat model, TRF without caloric reduction resulted in a strong inhibition of mTOR signaling, proliferation and fibrosis in the affected kidneys. The adminstration of an ad libitum fed KD led to similar results. In rat, mouse and feline models of PKD, acute fasting led to a significant reduction of cyst volume. Therefore, cystic cells seem to be metabolically inflexible and exhibit an altered metabolism characterized by increased glycolysis and, amongst others, defective fatty acid oxidation, similar to the Warburg effect in cancer. (Torres, Kruger et al. 2019) While those beneficial observations were made in mouse, rat and feline models of PKD, the effects of a ketogenic diet in human ADPKD patients have not been investigated yet, even though the adminstration of ketogenic diets is used as a treatment for epilepsy in children since the 1920s and fasting is one of the oldest medical procedures. Therefore, the aim of the present study is to investigate the effects of a short-period ketonic state in 10 ADPKD patients with fast progressive disease. 10 ADPKD-patients (aged 18-60 years, CKD G 1-3a) will be enrolled after giving informed consent. These 10 subjects will go through four trial-related visits. During these visits, physical examinations will be performed, blood will be drawn, urine will be collected and ketone body measurements in breath, blood and urine will be carried out. Each study visit includes an abdominal MRI-scan. Between visit 1 and visit 2, patients will eat their regular carbohydrate-rich diet. After visit 2, a ketonic state will be induced in those patients. Patients can choose whether the ketonic state will be induced by acute fasting for 72 hours (under sufficient water consumption and salt substitution) or by eating a KD for 14 days. Study visit 3 will take place within 72 hours after finishing the dietary intervention. After study visit 3, patients will restart eating their regular diet. Study visit 4 will provide follow-up data 3-6 weeks after the dietary intervention. After study completion, the relative difference of TKV measured by MRI-based volumetry of the kidneys immediately before and immediately after the ketonic state, will be compared to TKV growth/decline while eating a regular carbohydrate-rich diet. In general, patients are counselled in our outpatient department as part of "The German AD(H)PKD Registry" (more than 700 patients enrolled). As from those patients, clinical data, laboratory data and imaging studies are present, identification and recruitment of patients with fast rapidly progressing disease will be facilitated. Also, the investigators are closely liaised with the German self-help group PKDCure (PKD Familiaere Zystennieren e.V.), which is dedicated to ADPKD-linked research. This will facilitate recruitment of patients even more. Data obtained from the study visits will be collected. The parameters listed below constitute the core data set, additional parameters can be included if considered essential. Registered patients will be provided with diaries for the documentation of feeling of hunger, problems and discomforts as well as acetoacetate concentrations in breath. Patients are also provided with a portable breath-analyzer to measure acetoacetate concentrations in breath in between study visits. Study diaries are collected on Visit 4. Data capture will be performed at each study visit after enrollment.

Recruitment information / eligibility
Status Completed
Enrollment 10
Est. completion date July 1, 2021
Est. primary completion date July 1, 2021
Accepts healthy volunteers No
Gender All
Age group 18 Years to 60 Years
Eligibility Inclusion Criteria: - Male and female ADPKD-patients (diagnosed by genetics / typical MRI / ultrasound) - With evidence of fast progression, at least one of the following criteria 1. Mayo Class 1C-1E 2. Truncating PKD1-mutation 3. Hypertension < 35 years 4. Urological complications < 35 years 5. = 1 first class or second class family member with need of renal replacement therapy < 60 years 6. eGFR loss > 2,5 ml/min/1,73m2 per year 7. PROPKD-Score > 6 - Age = 18 and = 60 years - CKD stage 1-3a according to eGFR - Signed written informed consent Exclusion Criteria: - Currently under tolvaptan - BMI < 18 or > 35 - Diabetes mellitus (Type I, Type II, MODY, LADA) - Active alcoholism - Vegan or vegetarian lifestyle - Inability to sign or understand written informed consent - Anamnestically known circumstances which forbid the induction of a ketonic state by ketogenic diet or acute fasting (Liver damage (AST/ALT > 3x upper limit of normal, alkaline phosphatase > 6x upper limit of normal , Bilirubin = 3 mg/dl), Diabetes mellitus, Pyruvate carboxylase deficiency, defects of gluconeogenesis, defects of ketolysis / ketogenesis, hyperinsulinism, defects of fatty acid oxidation ) - Allergies or food intolerance against components of a ketogenic diet - Eating disorders (Anorexia nervosa / Bulimia) - Participation in a weight loss program (e.g. Optifast) or intake of medication to promote weight loss within the last six months - Ketogenic Diet > 1 month within the last 12 months - Chronic renal replacement therapy - Previous history of kidney transplantation - Uncontrolled local or systemic infection (according to clinical assessment) - Simultaneous participation in other interventional studies - Pregnant or breastfeeding women - Persons who are dependent of or employed by the study investigators - Contraindications against MRI examinations (stents, pacemakers or other metal inserts, claustrophobia) - Persons living in an establishment by court order or official instructions

Study Design

Related Conditions & MeSH terms

Intervention

Other:
Fasting
Acute fasting for 72 hours
Ketogenic diet
Intake of a ketogenic diet for 14 days

Locations
Country Name City State
Germany Department II of Internal Medicine, University Hospital Cologne Cologne

Sponsors (1)
Lead Sponsor Collaborator
University of Cologne

Country where clinical trial is conducted

Germany, 

References & Publications (1)

Torres JA, Kruger SL, Broderick C, Amarlkhagva T, Agrawal S, Dodam JR, Mrug M, Lyons LA, Weimbs T. Ketosis Ameliorates Renal Cyst Growth in Polycystic Kidney Disease. Cell Metab. 2019 Dec 3;30(6):1007-1023.e5. doi: 10.1016/j.cmet.2019.09.012. Epub 2019 Oct 17. — View Citation

Outcome
Type Measure Description Time frame Safety issue
Other Changes of renal functional panel in 24-h-urine Urin samples will be collected before and during the dietary intervention for the determination of creatinine, uric acid and urea (measurement unit mg/24h) Baseline and during 14 days of ketogenic diet or 3 days fasting
Other Changes of electrolytes and minerals in 24-h-urine Urin samples will be collected before and during the dietary intervention for the determination of sodium, natrium, potassium, magnesium, chloride, phosphate (measurement unit mmol/24h ) Baseline and during 14 days of ketogenic diet or 3 days fasting
Other Changes of glucose in 24-h-urine Urin samples will be collected before and during the dietary intervention Baseline and during 14 days of ketogenic diet or 3 days fasting
Other Changes of albumin in 24-h-urine Urin samples will be collected before and during the dietary intervention Baseline and during 14 days of ketogenic diet or 3 days fasting
Other Analysis of stool samples Stool samples will be collected before and during the dietary intervention and analysed Baseline and during 14 days of ketogenic diet or 3 days fasting
Other Changes of renal functional panel in spot urine Urin samples will be collected before and during the dietary intervention for the determination of creatinine, uric acid and urea (measurement unit g/24h) Baseline and during 14 days of ketogenic diet or 3 days fasting
Other Changes of electrolytes and minerals in spot urine Urin samples will be collected before and during the dietary intervention for the determination of sodium, natrium, potassium, magnesium, chloride, phosphate (measurement unit mmol/24h) Baseline and during 14 days of ketogenic diet or 3 days fasting
Other Changes of albumin in spot urine Urin samples will be collected before and during the dietary intervention Baseline and during 14 days of ketogenic diet or 3 days fasting
Other Changes of glucose in spot urine Urin samples will be collected before and during the dietary intervention Baseline and during 14 days of ketogenic diet or 3 days fasting
Other Changes in urinary doubly refractile lipid bodies Urin samples will be collected before and during the dietary intervention Baseline and during 14 days of ketogenic diet or 3 days fasting
Primary Relative difference of TKV immediately before and after the ketonic state MRI-based kidney volumetry at study visit 2 and study visit 3 Visit 2: 2-4 Weeks after enrolment; Visit 3: 3 - 21 days after Visit 2
Secondary Absolute and relative difference of TKV assessed by MRI-based volumetry at all study visits Baseline visit (V1) and final study visit (V4) after at maximum 95 days
Secondary Absolute and relative difference of height-adjusted total kidney volume (htTKV) assessed by MRI-based volumetry at all study visits Baseline visit (V1) and final study visit (V4) after at maximum 95 days
Secondary Absolute and relative difference of total liver volume (TLV) assessed by MRI-based volumetry at all study visits Baseline visit (V1) and final study visit (V4) after at maximum 95 days
Secondary Absolute and relative difference of cystic burden of kidneys and liver assessed by MRI at all study visits Baseline visit (V1) and final study visit (V4) after at maximum 95 days
Secondary Absolute and relative change of Renal Function Panel Measurement of creatinine, urea and uric acid in blood and urine samples (measurement unit mg/dl) Baseline visit (V1), study visit 2 (V2): 2-4 Weeks after enrolment; Visit 3: 3 - 21 days after Visit 2, and final study visit (V4) after at maximum 95 days
Secondary Absolute and relative change of electrolytes and minerals Measurement of electrolyte and minerals (sodium, natrium, potassium, magnesium, chloride, phosphate) in blood (measurement unit mmol/L) and urine samples (measurement unit mmol/24h) Baseline visit (V1), study visit 2 (V2): 2-4 Weeks after enrolment; Visit 3: 3 - 21 days after Visit 2, and final study visit (V4) after at maximum 95 days
Secondary Absolute and relative change of albumin Measurement in blood and urine samples Baseline visit (V1), study visit 2 (V2): 2-4 Weeks after enrolment; Visit 3: 3 - 21 days after Visit 2, and final study visit (V4) after at maximum 95 days
Secondary Absolute and relative change of glucose Measurement in blood and urine samples Baseline visit (V1), study visit 2 (V2): 2-4 Weeks after enrolment; Visit 3: 3 - 21 days after Visit 2, and final study visit (V4) after at maximum 95 days
Secondary Absolute and relative change of Hepatic Function Panel Measurement of Alanine aminotransferase(ALT), Aspartate Aminotransferase (ASP), Alkaline Phosphatase (ALP), gamma-glutamyl transferase (GGT) and Lactate Dehydrogenase (LD) in blood samples (measurement unit U/L) Baseline visit (V1), study visit 2 (V2): 2-4 Weeks after enrolment; Visit 3: 3 - 21 days after Visit 2, and final study visit (V4) after at maximum 95 days
Secondary Absolute and relative change of bilirubin Measurement in blood samples Baseline visit (V1), study visit 2 (V2): 2-4 Weeks after enrolment; Visit 3: 3 - 21 days after Visit 2, and final study visit (V4) after at maximum 95 days
Secondary Absolute and relative change of lipid panel Measurement of high density lipoprotein (HDL), low density lipoprotein (LDL), total cholesterol, triglycerides and lipoprotein(a) in blood samples Baseline visit (V1), study visit 2 (V2): 2-4 Weeks after enrolment; Visit 3: 3 - 21 days after Visit 2, and final study visit (V4) after at maximum 95 days
Secondary Absolute and relative change of inflammatory parameters Measurement of c-reactive protein (CRP) and high sensitivity c-reactive protein (hsCRP) in blood samples ( measurement unit mg/L) Baseline visit (V1), study visit 2 (V2): 2-4 Weeks after enrolment; Visit 3: 3 - 21 days after Visit 2, and final study visit (V4) after at maximum 95 days
Secondary Absolute and relative change in blood count Measurement of white blood cells, red blood cells, platelets in blood samples (measurement unit 10^9/L ) Baseline visit (V1), study visit 2 (V2): 2-4 Weeks after enrolment; Visit 3: 3 - 21 days after Visit 2, and final study visit (V4) after at maximum 95 days
Secondary Absolute and relative change of hemoglobin Measurement in blood samples Baseline visit (V1), study visit 2 (V2): 2-4 Weeks after enrolment; Visit 3: 3 - 21 days after Visit 2, and final study visit (V4) after at maximum 95 days
Secondary Absolute and relative change of hematokrit Measurement in blood samples Baseline visit (V1), study visit 2 (V2): 2-4 Weeks after enrolment; Visit 3: 3 - 21 days after Visit 2, and final study visit (V4) after at maximum 95 days
Secondary Absolute and relative change of betahydroxybutyrate level Measurement of betahydroxybutyrate level in blood samples for determination of ketosis Baseline visit (V1), study visit 2 (V2): 2-4 Weeks after enrolment; Visit 3: 3 - 21 days after Visit 2, and final study visit (V4) after at maximum 95 days
Secondary Absolute and relative change in blood gas analysis Measurement with blood gas analyzer for determination of ketosis Baseline visit (V1), study visit 2 (V2): 2-4 Weeks after enrolment; Visit 3: 3 - 21 days after Visit 2, and final study visit (V4) after at maximum 95 days
Secondary Analysis of the ketonic state with betahydroxybutyrate level Betahydroxybutyrate measurement from blood samples of the fingertip by patients at home Baseline visit (V1), during 14 days of ketogenic diet or 3 days fasting and final study visit (V4) after at maximum 95 days
Secondary Analysis of the ketonic state with ketonuria Ketonuria measured with urine stix by patients at home Baseline visit (V1), during 14 days of ketogenic diet or 3 days fasting and final study visit (V4) after at maximum 95 days
Secondary Analysis of the ketonic state with acetoacetate in breath determination of acetoacetate in breath by patients at home Baseline visit (V1), during 14 days of ketogenic diet or 3 days fasting and final study visit (V4) after at maximum 95 days
Secondary Absolute and relative change of height Determination of height Baseline visit (V1), V2 (2-4 Weeks after enrolment); Visit 3 (3 - 21 days after Visit 2 ) and final study visit (V4) after at maximum 95 days
Secondary Absolute and relative change of weight Determination of weight Baseline visit (V1), V2 (2-4 Weeks after enrolment); Visit 3 (3 - 21 days after Visit 2 ) and final study visit (V4) after at maximum 95 days
Secondary Absolute and relative change of waist circumference Determination of waist circumference Baseline visit (V1), V2 (2-4 Weeks after enrolment); Visit 3 (3 - 21 days after Visit 2 ) and final study visit (V4) after at maximum 95 days
Secondary Relative change of calorimetry Could be determined instead of anthropometric parameters Baseline visit (V1), V2 (2-4 Weeks after enrolment); Visit 3 (3 - 21 days after Visit 2 ) and final study visit (V4) after at maximum 95 days
Secondary Changes in Bioimpedance Bioimpedance measurements on each visit Baseline visit (V1), V2 (2-4 Weeks after enrolment); Visit 3 (3 - 21 days after Visit 2 ) and final study visit (V4) after at maximum 95 days
Secondary Feeling of hunger, discomforts and problems measured and documented at home in a study dietary in between study visits In between baseline visit (V1) and final study visit (V4) after at maximum 95 days
Secondary Acetoacetate-concentrations measured and documented at home in a study dietary in between study visits In between baseline visit (V1) and final study visit (V4) after at maximum 95 days
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