Skeletal muscle and whole-body protein turnover in cirrhosis
- 1 June 1990
- journal article
- research article
- Published by Portland Press Ltd. in Clinical Science
- Vol. 78 (6) , 613-619
- https://doi.org/10.1042/cs0780613
Abstract
1. We investigated arteriovenous exchanges of tyrosine and 3-methylhistidine across leg tissue in the postabsorptive state as specific indices of net protein balance and myofibrillar protein breakdown, respectively, in eight patients with cirrhosis and in 11 healthy control subjects. Whole-body protein turnover was also measured using L-[1-13C]leucine. 2. Leg efflux of tyrosine was 45% greater in cirrhotic patients than in normal control subjects [-6.5(1.4 to -19.1) vs. - 4.2 (-2.2 to -7.7) .mu.mol min-1 100 mg-1 of leg, median (range), P < 0.0025]. 3-Methylhistidine efflux was not significantly altered. 3. In cirrhosis, whole-body leucine flux was normal but whole-body leucine oxidation was elevated so that whole-body protein synthesis was depressed by 17%. 4. The results indicate the predominant mechanism of muscle wasting in cirrhosis to be a fall in muscle protein synthesis, which is accompanied by a overall fall in whole-body protein turnover.This publication has 21 references indexed in Scilit:
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