Fetal growth and insulin resistance in adult life: Role of skeletal muscle morphology

被引:31
作者
Thompson, CH
Sanderson, AL
Sandeman, D
Stein, C
Borthwick, A
Radda, GK
Phillips, DIW
机构
[1] UNIV NEWCASTLE UPON TYNE, DEPT BIOCHEM & GENET, NEWCASTLE, ENGLAND
[2] SOUTHAMPTON GEN HOSP, MRC, ENVIRONM EPIDEMIOL UNIT, SOUTHAMPTON SO9 4XY, HANTS, ENGLAND
关键词
glycogen; glycogen synthase; near-infrared spectroscopy; plethysmography;
D O I
10.1042/cs0920291
中图分类号
R-3 [医学研究方法]; R3 [基础医学];
学科分类号
1001 ;
摘要
1. Thinness at birth is associated with insulin resistance in adult life and an apparent delay in activation of glycolysis/glycogenolysis in exercising skeletal muscle, As developmental abnormalities of skeletal muscle histology or metabolism may explain this association we examined muscle histology, biochemistry and blood Bow in a group of 27 adult women whose birth details were known. 2. Subjects were examined by near-infrared spectroscopy to determine forearm muscle oxygen supply, and by muscle biopsy and forearm plethysmography, Those,vith a ponderal index at birth < 23 kg/m(3) were insulin resistant (assessed by the short insulin-tolerance test - mean rate constants for glucose disappearance = 4.14 compared with 4.83%/min, P = 0.045) and had significantly more rapid muscle reoxygenation than the remainder of the subjects (13 compared with 22 s, P = 0.004). 3. Thinness at birth did not influence muscle capillary density, muscle glycogen content, glycogen synthase activity, citrate synthase activity or resting forearm blood flow. 4. Insulin resistance seen after fetal malnutrition was not associated with abnormal muscle histology, resting muscle blood Bow mitochondrial volume or glycogen content. 5. The increase in muscle reoxygenation rate in adult subjects who were thin at birth could occur to promote oxidative ATP synthesis in compensation for the delay in activation of glycolysis/glycogenolysis. It suggests altered regulation structure of the muscle microcirculation. Thrse changes appear to antedate the structural and biochemical changes seen in muscle from patients with established diabetes.
引用
收藏
页码:291 / 296
页数:6
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