Abstract
Exercise-induced lipolysis and hormones possibly involved in the regulation of lipid
metabolism in association with exercise (plasma catecholamines, ACTH, HGH, TSH, insulin)
were studied in 11 WHO stage 1 to 2 hypertensive men (mean age 37 yearsl during a
30-min steady-state submaximal (65% of V̇O2 max) and near-maximal exercise seated on a bicycle ergometer. To assess the contribution
of the sympathetic system to the regulation of lipolysis and to define the type of
(β-receptors mediating the catecholamine effects on lipolysis, all patients were again
studied under identical conditions after a 4-week treatment with the (β-1- β-2-receptor
antagonist pindolol (15 mg daily) and with the (β-1-receptor blocker acebutolol (500
mg daily). Eight patients were even restudied after a 16-month treatment with acebutolol.
Plasma glycerol levels increased progressively (P < 0.001) during exercise reflecting increased exercise-induced lipolysis. The concomitant
significant rise of noradrenalin, adrenaline, ACTH, and HGH and the parallel fall
in plasma insulin suggest that all these hormones are involved in the adjustment of
exercise-induced lipolysis. However, the impaired cate-cholamine-induced lipolysis
under (β-receptor blockade was not accompanied by significant compensatory increases
of ACTH, HGH, or TSH or a fall in insulin during exercise. Both (β-receptor antagonists
resulted in a similar 27% inhibition of lipolysis confirming that the catecholamine-induced
increase of lipolysis is mainly mediated via (β-1-adrenoceptors.
After 16 months of treatment with acebutolol, the degree of inhibition of the exercise-induced
lipolysis was unchanged. However, FFA were significantly reduced (28%, P < 0.05) and HGH significantly (100%, P < 0.05) increased.
Key words
lipolysis - catecholamines - ACTH - HGH - TSH - insulin - exercise - β-receptor blockade
