| Abstract | Insulin plays a major role in the regulation of skeletal muscle protein turnover but its mechanism of action is not fully understood, especially in vivo during catabolic states. These aspects are presently reviewed. Insulin inhibits the ATP-ubiquitin proteasome proteolytic pathway which is presumably the predominant pathway involved in the breakdown of muscle protein. Evidence of the ability of insulin to stimulate muscle protein synthesis in vivo was also presented. Many catabolic states in rats, e.g. streptozotocin diabetes, glucocorticoid excess or sepsis-induced cytokines, resulted in a decrease in insulin action on protein synthesis or degradation. The effect of catabolic factors would therefore be facilitated. In contrast, the antiproteolytic action of insulin was improved during hyperthyroidism in man and early lactation in goats. Excessive muscle protein breakdown should therefore be prevented. In other words, the anabolic hormone insulin partly controlled the 'catabolic drive'. Advances in the understanding of insulin signalling pathways and targets should provide information on the interactions between insulin action, muscle protein turnover and catabolic factors. |
| Authors | J Grizard, D Dardevet, M Balage, D Larbaud, S Sinaud, I Savary, K Grzelkowska, C Rochon, I Tauveron, C Obled
(Affiliation: Unité d'étude du métabolisme azoté, Inra centre de Clermont-Ferrand/Theix, Saint-Genès-Champanelle, France.)
|
| Journal | Reproduction, nutrition, development
(Reprod Nutr Dev)
1999 Jan-Feb
Vol. 39
Issue 1
Pg. 61-74
ISSN: 0926-5287 FRANCE |
| PMID | 10222500
(Publication Type: Journal Article, Review)
|
| Chemical References |
- Cytokines
- Glucocorticoids
- Muscle Proteins
- Insulin
|
| Topics |
- Animals
- Cytokines
(pharmacology)
- Diabetes Mellitus, Experimental
(metabolism)
- Glucocorticoids
(pharmacology)
- Humans
- Insulin
(metabolism, pharmacology)
- Muscle Proteins
(biosynthesis, metabolism)
- Muscle, Skeletal
(drug effects, metabolism)
- Rats
- Signal Transduction
|
