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生长激素缺乏症成年人的生活质量受损与外周疲劳状态下发现的改变的骨骼肌氧化代谢无关。

Impaired quality of life in growth hormone-deficient adults is independent of the altered skeletal muscle oxidative metabolism found in conditions with peripheral fatigue.

机构信息

Department of Paediatric Endocrinology, Great North Children's Hospital, Newcastle-upon-Tyne, UK; Institute of Genetic Medicine, Newcastle University, Newcastle-upon-Tyne, UK.

出版信息

Clin Endocrinol (Oxf). 2014 Jan;80(1):107-14. doi: 10.1111/cen.12252. Epub 2013 Jun 20.

Abstract

CONTEXT

Growth hormone-deficient (GHD) adults often report impaired quality of life (QoL) - with fatigue, a key element. This deficit can improve following GH replacement. The basis of this response is unclear. Perturbations in skeletal muscle metabolism have been demonstrated in several conditions in which fatigue is a prominent symptom. We wished to define the role of skeletal muscle metabolism in the impaired QoL observed in patients with GHD.

OBJECTIVE

To compare in vivo skeletal muscle mitochondrial oxidative phosphorylation using phosphorus-31 magnetic resonance spectroscopy in matched untreated GHD adults, treated GHD adults and healthy volunteers.

DESIGN

Twenty-two untreated GHD adults, 23 treated GHD adults and 20 healthy volunteers were recruited at a regional centre. All patients underwent assessment of muscle mitochondrial function (τ₁/₂ PCr) and proton handling using spectroscopy. Fasting biochemical analyses and anthropometric measurement were obtained. All patients completed the QoL-AGHDA and physical activity assessment (IPAQ) questionnaires.

RESULTS

Untreated and treated GHD adults complained of significantly increased fatigue and an impaired QoL (P = 0·002) when compared to healthy controls. There was no difference in maximal mitochondrial function (P = 0·53) nor pH recovery (P = 0·38) of skeletal muscle between the three groups. Untreated GHD patients had significantly lower IGF-1 than both treated GHD and healthy volunteers (P < 0·001), but there was no association between τ₁/₂ PCr and serum IGF-1 (r = -0·13, P = 0·32).

CONCLUSIONS

The impaired QoL seen in GHD adults is not associated with the skeletal muscle spectroscopic 'footprint' of altered mitochondrial oxidative function, anaerobic glycolysis or proton clearance that are a feature of several conditions in which fatigue is a prominent feature. These data suggest that the pathophysiology of fatigue and impaired QoL in GHD may have a significant central rather than peripheral (skeletal muscle) component.

摘要

背景

生长激素缺乏症(GHD)成年人常报告生活质量(QoL)受损-疲劳是关键要素。这种缺陷可以在生长激素替代后得到改善。这种反应的基础尚不清楚。在疲劳是突出症状的几种情况下,已经证明了骨骼肌肉代谢的紊乱。我们希望确定骨骼肌肉代谢在 GHD 患者观察到的受损 QoL 中的作用。

目的

使用磷-31 磁共振波谱比较未经治疗的 GHD 成年人、治疗后的 GHD 成年人和健康志愿者的体内骨骼肌线粒体氧化磷酸化。

设计

在一个区域中心招募了 22 名未经治疗的 GHD 成年人、23 名治疗后的 GHD 成年人和 20 名健康志愿者。所有患者均接受了肌肉线粒体功能(τ₁/₂ PCr)和质子处理的光谱评估。进行了空腹生化分析和人体测量。所有患者均完成了 QoL-AGHDA 和体力活动评估(IPAQ)问卷。

结果

未经治疗和治疗后的 GHD 成年人与健康对照组相比,疲劳感明显增加,生活质量受损(P = 0.002)。三组之间的最大线粒体功能(P = 0.53)或骨骼肌肉 pH 恢复(P = 0.38)均无差异。未经治疗的 GHD 患者的 IGF-1 明显低于治疗后的 GHD 和健康志愿者(P < 0.001),但 τ₁/₂ PCr 与血清 IGF-1 之间无关联(r = -0.13,P = 0.32)。

结论

GHD 成年人的受损 QoL 与骨骼肌光谱中改变的线粒体氧化功能、无氧糖酵解或质子清除的“特征”无关,这些特征是疲劳是突出特征的几种情况下的特征。这些数据表明,GHD 中疲劳和受损 QoL 的病理生理学可能具有重要的中枢成分,而不是外周(骨骼肌肉)成分。

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