Trial in Elderly with Musculoskeletal Problems due to Underlying Sarcopenia—Faeces to Unravel the Gut and Inflammation Translationally (TEMPUS-FUGIT): protocol of a cross-sequential study to explore the gut-muscle axis in the development and treatment of sarcopenia in community-dwelling older adults

The TEMPUS-FUGIT-project is a single center study conducted in the University Hospitals (UZ) Leuven, Leuven, Belgium. The study set-up is two-fold, consisting of an observational, cross-sectional, case–control phase and a longitudinal, interventional, phase.

In the cross-sectional study phase, the primary objective is to compare GM composition and intestinal inflammatory markers between 100 healthy community-dwelling older adults without sarcopenia and 100 community-dwelling older adults with sarcopenia.

The longitudinal phase of TEMPUS-FUGIT has a triple-blinded randomized controlled trial (RCT) set-up. This comprises a 12-weeks program of single or combined, optimized, and individualized anabolic interventions (a physical exercise program, protein and/or omega-3 polyunsaturated fatty acids (PUFA) supplementation). The effects of these interventions on GM composition and fecal intestinal inflammatory markers will be assessed in 100 sarcopenic older adults. To this end, participants will be 1:1 allocated into one of five intervention groups, which differ in the combination of the exercise and nutritional interventions.

An overview of the general set-up of the TEMPUS-FUGIT study is given in Fig. 2. More details on the interventions have been previously published by Dedeyne et al. and will be summarized further in this manuscript [29].

In TEMPUS-FUGIT 100 healthy community-dwelling non-sarcopenic older adults (aged ≥ 65 years) will be recruited to be compared with 100 older adults with sarcopenia defined according to the revised definition of the European Working Group on Sarcopenia in Older People (EWGSOP2) [30]. The sarcopenic older adults will also participate in the longitudinal (interventional) phase of the study.

The sarcopenic and the non-sarcopenic group will be gender-matched, whereas for age and Body Mass Index (BMI), caliper matching (maximum tolerated difference between matched persons) will be applied [31]. Sarcopenic older adults will be recruited from the ongoing triple blinded RCT ‘Exercise and Nutrition for Healthy AgeiNg’ (ENHANce) study (Clinical Trial number NCT 03649698) [29]. Participants will be recruited from the environment of Leuven, Flanders, Belgium. To ensure recruitment of a sufficient number of study persons, contacts have been established with the geriatric outpatient clinic (including falls prevention clinic) and representatives of service flats and day care centers or organizations for older adults. Furthermore, medical staff collaborating to the project will use their network for recruitment. Also health care specialists, i.e., general practitioners, pharmacists and physiotherapists will be requested to refer patients who may be eligible for this study. Also information about the study will be distributed by organizations and websites that target older persons, advertisements in local newspapers and distributions of flyers. Older adults, who were initially screened for the ENHANce study but failed to meet the inclusion criteria for sarcopenia, will be re-contacted to participate in the non-sarcopenic control group of the TEMPUS-FUGIT study.

Sarcopenic participants should be diagnosed with probable (low muscle strength), confirmed (low muscle strength & mass) or severe sarcopenia (low muscle strength, mass and physical performance) by EWGSOP2 [30], whereas healthy controls should not have sarcopenia. Furthermore, controls as well as sarcopenic participants should meet the following inclusion criteria: ≥ 65 years, community-dwelling or assisted living, able to communicate in Dutch both orally and written, have a Mini-Mental State Examination (MMSE) Score ≥ 21 points, be in the possession of a freezer for preservation of fecal samples, absence of diabetes and no intake of diabetes medication, no intake of corticoids, absence of terminal illness with prognosis < 6 months, no antibiotics use in the past 3 months, absence of ongoing or previous (< 5 years) malignancy of the gastrointestinal tract, no Irritable Bowel Syndrome (IBS) or IBD, no chronic kidney disease (glomerular filtration rate (eGFR) < 30 ml/min/1.73m²) and absence of disorders, recent complaints, injury or surgery that prevent participation to the study according to the researchers. Additionally, sarcopenic participants should not have followed a rehabilitation or physical exercise program > 2/week in the last six months and should have a protein intake ≤ 1.5 g per kg body weight (BW) per day.

For the cross-sectional phase, outcome measurements will be taken at the baseline test visit.

For the longitudinal phase in sarcopenic participants, outcome measurements will be collected from the baseline test visit until the week 12 visit. The primary outcome of this phase is:

GM analyses will comprise determination of within sample diversity (α-diversity), including sample richness, taxa abundance, evenness, and taxa distribution through the following indices: Chao 1, Shannon and Simpson’s indices, abundance-based coverage estimators (ACE) index and the Good’s Coverage index. Taxa abundance will be expressed as Operational Taxonomic Units (OTU) and/or Amplicon Sequence Variants (ASV). Sequencing reads will be demultiplexed with LotuS (version 1.565) and processed further with the DADA2 pipeline (version 1.6.0), using the RDP classifier version 2.12 for taxonomy assignment (default parameters). Between sample dissimilarity (β-diversity) will be determined with Bray–Curtis dissimilarity (through a distance based non-parametrical permutational analysis of variance (PERMANOVA) test) and weighted and unweighted UniFrac (through principal coordinates analysis (PCoA)), respectively. Comparisons of relative GM abundance between sarcopenic and non-sarcopenic older adults will be performed through linear discriminant analysis (LDA) effect size (LEfSe). GM analyses, as well as visualization of the results will be performed using R vegan and phyloseq packages [54]. Enterotyping (or community-typing) will be performed based on the Dirichlet-multi-nominal Model (DMM) approach in R (dmn function) as previously described on a combined genus-level abundance matric containing the study samples as well as 1106 Flemish Gut Flora Project (FGFP) samples to increase accuracy [55, 56]. Continuous data will be checked for normality with the Shapiro–Wilk test. The t-test will be performed for between-group analysis of continuous clinical parameters, if normally distributed. For GM analyses, non-parametric testing will be applied. The Mann–Whitney U test will be performed in case of non-parametric distribution. Correlations between microbiota species and clinical parameters will be assessed with Spearman correlation. Linear regression models adjusted for putative confounders (e.g., age) will be used to check for associations between GM species abundance and clinical parameters. To determine possible effects of the interventions on GM in different groups, linear mixed models will be applied. Multiple testing corrections will be applied if it is applicable (Benjamini-Hochberg- False Discovery Rate (FDR)). An FDR of ≤ 0.10 will be taken into account for GM analyses [57]. Level of significance will be a p-value of ≤ 0.05. A bioinformatician from VIB and a statistician from LBiostat will be consulted for the statistical analyses.

In TEMPUS-FUGIT, a pragmatic sample of 100 sarcopenic people from the longitudinal phase, will be compared with 100 non-sarcopenic volunteers. Therefore, 110 non-sarcopenic controls will be recruited, in order to ensure 100 included control persons that, similarly to the sarcopenic participants, have a protein intake < 1.5 g/kg BW/day. Indeed, based on previous similar data, we expect, a drop-out of 5.88% in the non-sarcopenic control group due to a protein intake > 1.5 g/kg BW/day, [58]. Due to the exploratory character of this study, no sample size calculation was performed. Based on previous studies, 100 participants in each group is considered as sufficient for this study [16, 18, 29].

The first version of the protocol dates from July 7^th 2021 and was accepted was to the Ethics Committee of UZ/KU Leuven on July 14^th 2021. Modifications to the protocol possibly impacting the study conduct, patient benefits and/or patient safety, changes of study aims, changes of study design, sample size, patient population and study procedures will require an amendment. Any amendment will be approved by the local Ethics Committee (EC) and will be agreed upon by the study team.

TEMPUS-FUGIT was approved by the Ethical Committee (S65127) and registered at Clinical Trials.gov (NCT05008770). The researchers obtain written informed consent from each individual willing to participate in the study, according to good clinical practice. With this study protocol, a thorough overview is given of the methodology of the TEMPUS-FUGIT project, based on the Standard Protocol Items, Recommendations for Interventional Trails (SPIRIT) guidelines [59].

Dissemination of the results will take place through publications in scientific and professional journals and by international conferences. Adverse events will be registered by the study coordinator. The study coordinator monitors all data and reports to the principal investigator. All study-related data will be handled and stored confidentially under supervision of the study coordinator. Protocol amendments will be reported on ClinicalTrails.gov. The study is performed an accordance with the principles of the Declaration of Helsinki.