Obesity Clinical Trial
Official title:
Immunometabolic Effects of Non-drug Strategies in the Clinical Management of Obesity: Translational Study
Forty women aged between 18 and 75 years-old with a BMI> 30kg/m2 are recruited to participate
in the evaluation of their medical management. They participate in an 8-week protocol as part
of hospital medical treatment for weight loss at the Oxford Polyclinic in Cannes (IPOCA). The
effects of 2 independent variables will be studied: (1) an adapted physical activity program
and (2) nutritional supplementation with R-α-Lipoic acid (2x300mg/d) versus placebo
(double-blind). The volunteers are randomly assigned to the different groups: Placebo with or
without exercise groups and ALA with or without exercise groups. At the start of the protocol
(T0), at 4 weeks (T4) and at 8 weeks (T8), various measurements are carried out (physical
capacities, nutritional status, body composition, distribution of adipose mass by CT-scan). A
venous sample taken for all participants is done at T0, T4 and T8 to investigate the immune
profile of circulating T lymphocytes.
This project is part of a translational research project to assess current care and to
investigate the immunometabolic effects of a non-drug medical care of obesity (adapted
physical activities, nutritional supplementation with α-lipoic acid, quality of food intake).
Obesity-related inflammation is central to the development of type 2 diabetes and potentiated
by advancing age, inactive behavior and sedentary lifestyle. Metabolism and immunity are
entangled in their respective effects: the pathways of inflammation are involved in
metabolism and the metabolic state plays a predominant role in immune function. Physical
activity and calorie restriction are first-line, non-drug strategies recommended in reducing
obesity and insulin resistance and then prevent type 2 diabetes. However, the impact of their
combined effects on circulating immune cells or those residing in adipose tissue and skeletal
muscle, remains insufficiently understood to allow a nutritional prescription (i.e., quality
of nutritional intake and efficient doses of physical activity) favorable to preventive
medical care, individualized, and effective. If the risk associated with an increase in
visceral fat mass is linked to a change in the pro/anti-inflammatory status, it is essential
to reduce this risk by acting on its cause, regardless of the weight loss. In a context of
low-grade inflammation, these effects could lead to an anti-inflammatory profile of T cells,
specifically regulatory T cells (Treg) whose metabolism is extremely "flexible" at the
periphery and into visceral adipose tissue (directly involved in inflammation of obesity).
ALA (Alpha-Lipoic Acid) is known to play a pivotal role in cellular redox status and energy
metabolism by modulating inflammatory and metabolic signaling pathways such as those of
NF-kB, JNK, PI3K/Akt, p38 MAPK, AMPK or PPARβ/δ. As ALA is a possible metabolic modulator, it
would affect the metabolism of T cells. And therefore ALA could be a complementary measure to
non-drug strategies by potentiating the correction of the inflammatory state linked to
obesity.
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