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An Exploratory Clinical Study on Autophagy During Fasting

Not Applicable
Recruiting
Conditions
Syndrome, Metabolic
Arthritis, Rheumatoid
Healthy
Interventions
Other: Fasting
Registration Number
NCT04739852
Lead Sponsor
Charite University, Berlin, Germany
Brief Summary

Autophagy is considered one of the key molecular mechanisms for the broad preventive and therapeutic effects of periodic fasting. While it is generally known that fasting induces autophagy, there are no human studies that focus on the size and temporal kinetics of autophagy and its association with fasting specific signaling pathways. The kinetics of autophagy in patients with chronic diseases will now be compared with the kinetics of autophagy in healthy subjects, who both fast according to the same scheme; and further changes in metabolic and inflammatory parameters will be investigated.

Detailed Description

Therapeutic fasting has been used for many decades in naturopathy and integrative medicine clinically successfully in the treatment of chronic diseases and pain syndromes. In particular, fasting therapy is used for chronic rheumatic, inflammatory, and metabolic diseases with increasing patient demand in specialized clinical facilities (fasting clinics).

Within the various historically developed forms of fasting, the fasting program according to the Buchinger Wilhelmi method has established itself worldwide as the most frequently applied method. This involves a subtotal caloric restriction with a daily caloric intake (200-400kcal/day) in the form of liquid components over a defined period of at least 10 days, accompanied by supporting measures of a health-promoting lifestyle program with elements such as exercise therapy, manual procedures, stress reduction and hydro-balneotherapy.

In early randomized studies and a systematic review, the effectiveness of inpatient fasting therapy for patients with rheumatoid arthritis was proven with 1a evidence. For the other indications, there is mainly empirical evidence or data from observation or prospective uncontrolled studies. In recent years, extensive basic science research activity has developed in the area of caloric restriction and intermittent fasting. In this context, a large number of favorable animal experimental findings have been demonstrated by defined fasting periods, including reductions in insulin, IGF-1, increases in adiponectins, insulin sensitivity, neurotrophic factors, and, over longer observation periods, a decrease in the incidence of cardiovascular, inflammatory, and metabolic, and more recently oncological diseases in a wide variety of animal species.

Numerous experimental studies have demonstrated that fasting or total or subtotal caloric restriction is a potent inducer of cellular autophagy. For autophagy, numerous beneficial effects on chronic diseases or disease defense functions have now been experimentally documented and also hypothesized for humans, including neurodegenerative and metabolic diseases, but also acute infections and inflammatory diseases. Unclear to date is the kinetics of the autophagy enhancing effect of fasting. In theoretical transfer from animal experimental data, an increase is postulated between 12 and 36h of fasting and possibly a decrease after several days.

Against this background, autophagy will now be investigated for the first time in blood samples from fasting healthy and diseased individuals in an exploratory clinical study.

Recruitment & Eligibility

Status
RECRUITING
Sex
All
Target Recruitment
60
Inclusion Criteria
  • One of the following diagnoses: rheumatoid arthritis, metabolic syndrome OR healthy volunteer
  • Beginning (first 24h) inpatient treatment or hospital stay at Immanuel Hospital Berlin, Department of Naturopathy OR healthy volunteer
  • Present written declaration of consent
Exclusion Criteria
  • Insufficient linguistic communication
  • Dementia or other cognitive disorder
  • Pregnancy or lactation
  • Simultaneous participation in another clinical trial

Study & Design

Study Type
INTERVENTIONAL
Study Design
PARALLEL
Arm && Interventions
GroupInterventionDescription
Metabolic SyndromeFastingParticipants with diagnosed metabolic syndrome
Healthy ParticipantsFastingHealthy participants
Rheumatoid ArthritisFastingParticipants with diagnosed rheumatoid arthritis
Primary Outcome Measures
NameTimeMethod
Exploratory Proteomics of Autophagy Processes Ichange from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up

- Change in protein levels of autophagy biomarkers (LC3II \& p62) of isolated PBMCs (peripheral blood mononuclear cells) by Western Blotting, change from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up

Exploratory Proteomics of Autophagy Processes IIchange from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up

- Change in protein levels and protein phosphorylation by untargeted mass spectrometry-based proteomics and phosphoproteomics of isolated PBMCs (peripheral blood mononuclear cells), change from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up

Secondary Outcome Measures
NameTimeMethod
Waist to Hip Ratiochange from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up
Rheumatoid factor (RF, IgM) (U/mL)Day 1 (baseline)

Evaluate RF status in participants with RA

Body fatchange from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up

Estimation of the body composition via bio-electrical impedance analysis (body fat and visceral fat in %)

Resting blood pressurechange from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up
Cutaneous carotenoid level (CCL)change from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up

Cutaneous carotenoid level (CCL), correlating with the overall antioxidant status, measured with a noninvasive skin carotenoid sensor (Biozoom®)

Heart ratechange from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up
Health Assessement Questionnaire (HAQ)change from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up

Change from Baseline in the HAQ, range from 0 to 3 while higher values meaning a higher grade of disability

Quality of Life questionnaire (WHO-5)change from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up

Change from Baseline in the WHO-5, range from 0 to 100 %, higher values meaning a higher grade of well-being

Behavioral Factors: alcohol consumptionDay 1 (baseline), after 2 and 6 weeks

Number of alcoholic beverages on average per week in the last month

Muscle masschange from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up

Estimation of the body composition via bio-electrical impedance analysis (muscle mass in kg)

Body Mass Index (kg/m2)change from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up
Mood questionnaire (Profile of Mood States, POMS)change from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up

Change from Baseline in Emotional Distress will be measured using the German Version of the Profile of Mood States (ASTS) short version (19 items, 7-point Likert scale; 0=not at all, 6=extremely). Lower scores indicate more stable mood profiles.

Sociodemographic MeasurementsDay 1 (baseline)

Age, gender, education level, household income, employment status, marital status, language spoken, complete family history, current and previous illness and co-morbidities, and current medications

Behavioral Factorschange from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up

Physical inactivity, coffee, health promoting activities via Likert Scales, range from 0 to 5 while higher values meaning a higher grade of agreement

Behavioral Factors: fasting experienceDay 1 (baseline)

Type, definition, duration and date of previous fasting experiences

Expectation questionsDay 1 (baseline)

For fasting on a 5-point likert scale from 1 (nothing at all) to 5 (very strong)

Erythrocyte sedimentation rate (ESR) in millimeters per hour (mm/h)change from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up

Evaluate change in ESR in participants with RA

Anti-cyclic citrullinated peptide (ACPA) (U/mL)change from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up

Evaluate change in ACPA levels in participants with RA

Metabolic processeschange from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up

Targeted and quantitative analysis by mass spectrometry of change in metabolites of plasma, change from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up

Lipid profilingchange from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up

Targeted and quantitative analysis by mass spectrometry of change in plasma lipids, change from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up

Disease Activity Score 28 (DAS-28-CRP)change from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up

Change from Baseline in the DAS-28-CRP, range from 2.0 to 10.0 while higher values meaning a higher disease activity and below of 2.6 meaning remission

Simplified Disease Activity Index Score (SDAI)change from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up

Change from Baseline in the SDAI, range from 0 to 86 with assumed range from 0.1 to 10mg/dL for CRP. Higher values mean a higher disease activity and below of 34 meaning remission.

Stress questionnaire (Cohen Perceived Stress Scale, CPSS)change from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up

Change from Baseline in the CPSS, range from 0 to 4 in each item. Scores are obtained by reversing responses (e.g., 0 = 4, 1 = 3, 2 = 2, 3 = 1 \& 4 = 0) to the positively stated items and then summing across all scale items, higher values meaning a higher grade of perceived stress.

General Self-efficacy Short Scale (ASKU)change from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up

Assessing full scale, range 3-15, higher score meaning a better outcome

Electrolyteschange from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up

potassium (mmol/L) sodium (mmol/L)

Mindful Attention Awareness Scale (MAAS)change from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up

Assessing full scale, range from 15 to 90, higher score values meaning a better outcome.

Creatinine in µmol per liter (µmol/L)change from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up
Blood lipids and fasting glucosechange from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up

triglycerides (mmol/L) total cholesterol (mmol/L) LDL (mmol/L) HDL (mmol/L) fasting glucose (mmol/L)

Insulin (mU/L)change from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up
CrP (mg/L)change from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up

Evaluate change in CrP levels in participants with RA

Transcription expression patternschange from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up

Change of the gene expression profile by RNA sequencing of isolated PBMCs (peripheral blood mononuclear cells), change from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up

Numerical Analog Scaleschange from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up

Assessing stress, back pain, headache, shoulder/neck tension, sleep quality and duration, exhaustion, nervousness, digestive complaints, mood on 0-10 points each.

Hospital Anxiety and Depression Scale (HADS)change from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up

Assessing full scale, range 0-42, lower score meaning a better outcome

Behavioral Factors: smokingDay 1 (baseline), after 2 and 6 weeks

Number of cigarettes on average per week in the last month

Estimated glomerular filtration rate (eGFR) in milliliter per minute (mL/min)change from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up
ß-Hydroxybutyratechange from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up

Evaluate change in ketone body production by POCT

Proteome/phosphoproteome/ubiquitinome patternschange from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up

Evaluate proteome expression patterns through blood based proteome, phosphoproteome, and ubiquitinome analysis assessed prior to intervention (pre) vs. after 5-day fasting, day 2 of refeeding and 7 days post intervention

Epigentic patternschange from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up

Evaluate epigentic methylation patterns through blood based epigenome analysis assessed prior to intervention (pre) vs. after 5-day fasting, day 2 of refeeding and 7 days post intervention

Exosomal protein patternschange from baseline over 5 fasting days, to day 3 refeeding and to 7 days follow up

Evaluate exosomal protein content through blood based metabolome analysis assessed prior to intervention (pre) vs. after 5-day fasting, day 2 of refeeding and 7 days post intervention

Trial Locations

Locations (1)

Hochschulambulanz für Naturheilkunde der Charité-Universitätsmedizin Berlin am Immanuel-Krankenhaus

🇩🇪

Berlin, Germany

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