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最大间歇运动期间骨骼肌糖原磷酸化酶和丙酮酸脱氢酶的调节

Regulation of skeletal muscle glycogen phosphorylase and PDH during maximal intermittent exercise.

作者信息

Parolin M L, Chesley A, Matsos M P, Spriet L L, Jones N L, Heigenhauser G J

机构信息

Department of Medicine, McMaster University, Hamilton, Ontario L8N 3Z5.

出版信息

Am J Physiol. 1999 Nov;277(5):E890-900. doi: 10.1152/ajpendo.1999.277.5.E890.

Abstract

The time course for the activation of glycogen phosphorylase (Phos) and pyruvate dehydrogenase (PDH) and their allosteric regulators was determined in human skeletal muscle during repeated bouts of maximal exercise. Six subjects completed three 30-s bouts of maximal isokinetic cycling separated by 4-min recovery periods. Muscle biopsies were taken at rest and at 6, 15, and 30 s of exercise during bouts 1 and 3. Phos was rapidly activated within the first 6 s of bout 1 from 12% at rest to 47% at 6 s. The activation of PDH increased from 14% at rest to 48% at 6 s and 95% at 15 s of bout 1. Phos reverted back to basal values at the end of the first bout, whereas PDH remained fully activated. In contrast, in the third bout, PDH was 42% at rest and was activated more rapidly and was nearly completely activated by 6 s, whereas Phos remained at basal levels (range 14-20%). Lactate accumulation was marked in the first bout and increased progressively from 2.7 to 76.1 mmol/kg dry wt with no further increase in bout 3. Glycogen utilization was also marked in the first bout and was negligible in bout 3. The rapid activation of Phos and slower activation of PDH in bout 1 was probably due to Ca(2+) release from the sarcoplasmic reticulum. Lactate accumulation appeared to be due to an imbalance of the relative activities of Phos and PDH. The increase in H(+) concentration may have served to reduce pyruvate production by inhibiting Phos transformation and may have simultaneously activated PDH in the third bout such that there was a better matching between pyruvate production and oxidation and minimal lactate accumulation. As each bout progressed and with successive bouts, there was a decreasing ability to stimulate substrate phosphorylation through phosphocreatine hydrolysis and glycolysis and a shift toward greater reliance on oxidative phosphorylation.

摘要

在人体骨骼肌进行多次最大运动期间,测定了糖原磷酸化酶(Phos)和丙酮酸脱氢酶(PDH)及其变构调节因子的激活时间进程。六名受试者完成了三次30秒的最大等速骑行,每次之间有4分钟的恢复期。在第1次和第3次运动期间,于静息状态以及运动6秒、15秒和30秒时采集肌肉活检样本。在第1次运动的前6秒内,Phos迅速激活,从静息时的12%升至6秒时的47%。第1次运动时,PDH的激活率从静息时的14%升至6秒时的48%和15秒时的95%。在第1次运动结束时,Phos恢复到基础值,而PDH仍保持完全激活状态。相比之下,在第3次运动中,PDH静息时为42%,激活更快,到6秒时几乎完全激活,而Phos保持在基础水平(范围为14 - 20%)。第1次运动时乳酸积累明显,从2.7 mmol/kg干重逐渐增加至76.1 mmol/kg干重,第3次运动时没有进一步增加。糖原利用在第1次运动时也很明显,在第3次运动时可忽略不计。第1次运动中Phos的快速激活和PDH的较慢激活可能是由于肌浆网释放Ca(2+)。乳酸积累似乎是由于Phos和PDH相对活性的不平衡。H(+)浓度的增加可能通过抑制Phos转化减少了丙酮酸生成,并且可能同时在第3次运动中激活了PDH,从而使丙酮酸生成与氧化之间有更好的匹配,乳酸积累最小。随着每次运动的进行以及连续运动,通过磷酸肌酸水解和糖酵解刺激底物磷酸化的能力下降,转而更依赖氧化磷酸化。

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