TY - JOUR
T1 - The effect of acute and chronic administration of the β-agonist, cimaterol, on protein synthesis in ovine skin and muscle
AU - Nash, J. E.
AU - Rocha, H. J.G.
AU - Buchan, V.
AU - Calder, G. A.
AU - Milne, E.
PY - 1994/4
Y1 - 1994/4
N2 - The action of intravenous infusion of the β-agonist cimaterol (2.5 mg/d) on whole-body N retention and protein synthesis in peripheral tissues was examined in growing sheep. Wool growth was determined from skin patch clippings and adjusted to total fibre production. Protein synthesis was measured, using sequential large dose injections of [l-13C]valine, leucine and phenylalanine and then [ring-d5]-phenylalanine, on biopsy samples from skin and m. longissimus dorsi taken before β-agonist administration, at day 3 and day 15 of cimaterol infusion, and 15 d after withdrawal of the drug. Cimaterol increased total N retention by 19–2 3 g N/d (P 0 01) over three successive 5 d periods. In contrast, wool growth was significantly reduced by 07 g N/d (P 0 001) and the proportion of total N retained in wool declined from 0–71 to 0.25 (P 0–01). The reduction in wool growth was accompanied by a decrease in protein fractional synthesis rate (FSR) in skin (11.6 v. 6 3 %/d, P 0.01). Muscle protein FSR, on the other hand, was markedly stimulated during cimaterol infusion (1.45 v 3.01 %/d, P 0.001) as was RNA concentration (P 0 001), RNA: protein (P 0.001) and protein :DNA (P 0.05). The estimated increase in total protein synthesis in muscle (+ 24 to 30 g/d) due to cimaterol administration was counterbalanced by reductions for skin (— 25 to 27 g/d); this may account for the lack of changes in whole-body protein synthesis following β-agonist administration reported in other studies. Although N retention rapidly returned to control values following withdrawal of the drug, both wool growth and skin protein synthesis remained depressed, while muscle protein FSR declined, but not to pre-treatment values. These results suggest a persistent action of cimaterol, but whether this is a function of residue concentrations or long-term metabolic responses is not known.
AB - The action of intravenous infusion of the β-agonist cimaterol (2.5 mg/d) on whole-body N retention and protein synthesis in peripheral tissues was examined in growing sheep. Wool growth was determined from skin patch clippings and adjusted to total fibre production. Protein synthesis was measured, using sequential large dose injections of [l-13C]valine, leucine and phenylalanine and then [ring-d5]-phenylalanine, on biopsy samples from skin and m. longissimus dorsi taken before β-agonist administration, at day 3 and day 15 of cimaterol infusion, and 15 d after withdrawal of the drug. Cimaterol increased total N retention by 19–2 3 g N/d (P 0 01) over three successive 5 d periods. In contrast, wool growth was significantly reduced by 07 g N/d (P 0 001) and the proportion of total N retained in wool declined from 0–71 to 0.25 (P 0–01). The reduction in wool growth was accompanied by a decrease in protein fractional synthesis rate (FSR) in skin (11.6 v. 6 3 %/d, P 0.01). Muscle protein FSR, on the other hand, was markedly stimulated during cimaterol infusion (1.45 v 3.01 %/d, P 0.001) as was RNA concentration (P 0 001), RNA: protein (P 0.001) and protein :DNA (P 0.05). The estimated increase in total protein synthesis in muscle (+ 24 to 30 g/d) due to cimaterol administration was counterbalanced by reductions for skin (— 25 to 27 g/d); this may account for the lack of changes in whole-body protein synthesis following β-agonist administration reported in other studies. Although N retention rapidly returned to control values following withdrawal of the drug, both wool growth and skin protein synthesis remained depressed, while muscle protein FSR declined, but not to pre-treatment values. These results suggest a persistent action of cimaterol, but whether this is a function of residue concentrations or long-term metabolic responses is not known.
KW - Agonists Cimaterol: Protein synthesis: Wool growth: Sheep
KW - β
UR - http://www.scopus.com/inward/record.url?scp=0028269004&partnerID=8YFLogxK
U2 - 10.1079/BJN19940158
DO - 10.1079/BJN19940158
M3 - Article
C2 - 7912105
AN - SCOPUS:0028269004
SN - 0007-1145
VL - 71
SP - 501
EP - 513
JO - British Journal of Nutrition
JF - British Journal of Nutrition
IS - 4
ER -