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Follistatin 344

FS-344, Activin-Binding Protein, FST344

Quick Stats
Studies 2
Trials 73
Recruiting NA INTERVENTIONAL NCT06683222

Mediating Role of Myokines in the Dialogue Between Muscle and Bone Tissue in a Population of Healthy Women Aged 20-89 Years

View on ClinicalTrials.gov Updated Dec 15, 2025

Brief Summary

The main hypothesis is that muscle acts on bone tissue via the secretion of myokines (myostatin, follistatin, irisin). This is based on previous results showing that muscle mass in different patient populations with very different body mass indexes (anorexic or obese patients) is significantly and independently associated with bone mineral density.

Detailed Description

Bone densitometry using X-ray absorptiometry (DXA) is the reference technique for measuring Bone Mineral Density (BMD). According to the International Osteoporosis Foundation (IOF), if a single site is to be preferred, it should be the total hip or femoral neck, using a single NHANES III reference curve. It should be stressed, however, that this curve was obtained from a North American population with anthropometric parameters, notably body mass index (BMI), that differ from those of the European population, particularly the Caucasian population. Apparently, only one reference curve has been obtained in France, from the OFELY study in 1993. Given the age of this cohort and the possibility of BMI changes over time in the Caucasian population, but even more so, the impossibility of transposing this curve onto new DXAs of different brands, new reference curves need to be developed. DMS IMAGING is therefore financing the MONIKA study, with the CHU de Nîmes as sponsor. As part of this study, some 425 healthy female volunteers aged between 20 and 89 will be recruited from three centers (Nîmes, Montpellier, Lyon). A DXA examination at various bone sites (femur, rachis, radius and whole body) will provide up-to-date normalcy curves for BMD, but also for body composition (fat and lean mass), which are currently lacking. Access to this population could also enable us to better understand bone physiology and the links that may exist between bone tissue and muscle and fat tissue.For example, the serum concentration of leptin, a hormone secreted by adipose tissue, is associated with bone mass in non-obese women.More recent data show that skeletal muscle also has a secretory activity, characterized by the production of myokines.In humans, there are various arguments in favour of myostatin's action on bone tissue.However, clinical studies in humans are very limited.Through two clinical studies, myokine levels were assessed in two populations with very different BMIs. Female patients suffering from anorexia nervosa, for example, showed decreased myostatin levels, increased follistatin levels and comparable irisin levels, in parallel with very low BMD, compared with a population of young, non-malignant women. In obese women with high BMD, it was also shown that myostatin and follistatin levels were high, whereas irisin levels were lower than in a control population. Furthermore, the effect of lean body mass on BMD was partially mediated by irisin. These results are still preliminary, having been obtained on a small group of subjects, and merit further investigation on a representative population scale. However, there are apparently no age-dependent reference values for these myokines. In addition to the involvement of these myokines in the muscle-bone complex, these factors could also be involved in the muscle-fat complex, since new functions are now being attributed to them, such as lipolysis, which could affect the concentrations of certain adipokines, such as leptin, which in turn could have an impact on bone formation and resorption. The main hypothesis is that muscle acts on bone tissue via the secretion of myokines (myostatin, follistatin, irisin). This is based on previous results showing that muscle mass in different patient populations with very different BMIs (anorexic or obese patients) is significantly and independently associated with BMD.

Interventions

Name: Blood sample
Type: DIAGNOSTIC_TEST
Description: 36 ml of blood in 3 x 7 ml dry tubes, 1 x 5 ml EDTA tube, 1 x 5 ml heparinized tube, 1 x 5 ml anti-protease tube)
Name: Saliva sample
Type: DIAGNOSTIC_TEST
Description: 5 ml of saliva will be taken.
Name: Grip test
Type: DIAGNOSTIC_TEST
Description: The grip strength of the dominant arm will be measured with the participant in a standing position, with the arm close to the body and the elbow at 90◦ flexion, while the non-dominant arm will be positioned alongside the body. Three measurements will be taken for the dominant hand, and the mean value will be calculated and used for analysis. One minute is allowed between each repetition, to avoid muscle fatigue. Dynamometer quality control is ensured by regularly checking known resistance values.
Name: MicroFET2® maximum isometric force test
Type: OTHER
Description: The microFET2 device is used to test isometric force. The microFET2 dynamometer is battery-powered and ergonomically designed to fit in the palm of the hand. The system is microprocessor-controlled to provide accurate, repeatable muscle force readings. The microFET Clinical software automatically performs calculations and validity tests, and allows graphs to be generated from the data, enabling reports of different patient tests to be compared
Name: Maximum isometric knee extension bench test.
Type: OTHER
Description: The maximal isometric knee extension strength test on a specially-adapted strength bench consists in performing 3 maximal contractions with 1 minute's rest between each test.
Name: The SPPB (Short Physical Performance Battery)
Type: OTHER
Description: Battery of tests comprising a balance test, a walking speed test and a chair-lift test
Name: The 6-minute walking test.
Type: OTHER
Description: Muscular function will be determined by the 6-minute walk test to assess aerobic endurance. Participants will be asked to walk for 6 min as fast as possible on a shuttle track. The distance (m) covered in 6 min will be measured. Walking speed (m/s) will be calculated as the distance (m) covered in 6 min. A walking speed \<0.8 m/s has been defined as a low value.
Name: Segmental impedancemetry examination.
Type: OTHER
Description: Segmental impedancemetry involves measuring body composition using the body's resistance to the passage of a low-intensity electric current. This test is harmless to the body.
Name: Indirect calorimetry test.
Type: OTHER
Description: An Indirect calorimetry is the standard method for measuring energy expenditure at rest. It is based on the principle that the human body burns nutrients using O2 and producing CO2.
Name: Fardellone's questionnaire
Type: OTHER
Description: Completion of a questionnaires on calcium intake (Fardellone)
Name: ONAPS questionnaire
Type: OTHER
Description: The ONAPS questionnaire contains questions on physical activity and sedentariness
Name: Dietary intake.questionnaire
Type: OTHER
Description: The dietary intake questionnaire contains questions regarding the person's eating habits - how many meals a day, where they eat, whether they eat alone, what foods they eat/drink and whether they are following a particular diet and, if so, the reasons why.

Primary Outcomes

Measure: Myostatin
TimeFrame: Baseline
Description: Plasma concentration of myostatin will be measured in pg/ml by Enzyme-Linked Immuno Sorbent Assay
Measure: Follistatin
TimeFrame: Baseline
Description: Plasma concentration of follistatin will be measured in pg/ml by Enzyme-Linked Immuno Sorbent Assay
Measure: Irisin
TimeFrame: Baseline
Description: Plasma concentration of irisin will be measured in pg/ml by Enzyme-Linked Immuno Sorbent Assay
Measure: Bone Mineral Density
TimeFrame: Baseline
Description: Bone densitometry using X-ray absorptiometry (DXA) measured in g/cm²
Measure: Lean body mass
TimeFrame: Baseline
Description: Impedencemetry, measured in Kg

Trial Information

NCT ID

NCT06683222

Status

Recruiting

Study Type

INTERVENTIONAL

Phases

NA

Sponsor

Centre Hospitalier Universitaire de Nīmes

Last Updated

December 15, 2025

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