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氯化钠对食用低钙饮食的泼尼松龙治疗大鼠钙平衡、甲状旁腺功能和羟脯氨酸排泄的影响。

Effects of NaCl on calcium balance, parathyroid function and hydroxyproline excretion in prednisolone-treated rats consuming low calcium diet.

作者信息

Goulding A, McIntosh J

出版信息

J Nutr. 1986 Jun;116(6):1037-44. doi: 10.1093/jn/116.6.1037.

Abstract

The short-term effects of dietary sodium chloride supplementation on calcium balance were examined in an animal model of corticosteroid-mediated osteoporosis. Changes in calcium and phosphate balance, parathyroid function and bone resorption elicited by salt supplements alone (8 g/100 g diet), prednisolone alone (2.2 mg/kg body wt per day) and both salt and prednisolone in combination were measured in rats consuming a low calcium diet (0.1% calcium) for 10 d. Parathyroid function was monitored by measuring urinary cyclic AMP excretion. Bone resorption was monitored by measuring urinary hydroxyproline excretion. Salt alone raised urinary calcium, cyclic AMP and hydroxyproline; prednisolone alone depressed net calcium absorption and urinary hydroxyproline but had no effect on urinary calcium. Salt and prednisolone each depressed calcium retention independently and together produced an additive adverse effect on calcium balance. Thus high dietary salt intakes augment urinary calcium loss, raise parathyroid activity, increase bone resorption and adversely affect calcium balance in prednisolone-treated growing rats with a restricted dietary calcium intake. These findings support the view that high salt intakes may exaggerate bone loss during chronic glucocorticoid therapy. Because people also develop osteoporosis during glucocorticoid therapy and respond to dietary salt supplements by increasing urinary calcium excretion and parathyroid hormone, high salt intakes may accelerate bone loss in patients receiving chronic glucocorticoid therapy. The beneficial effects of dietary salt restriction on the conservation of bone mass warrant investigation in these patients.

摘要

在皮质类固醇介导的骨质疏松症动物模型中,研究了补充膳食氯化钠对钙平衡的短期影响。在食用低钙饮食(0.1%钙)10天的大鼠中,测量了单独补充盐(8 g/100 g饮食)、单独使用泼尼松龙(每天2.2 mg/kg体重)以及盐和泼尼松龙联合使用所引起的钙和磷平衡、甲状旁腺功能及骨吸收的变化。通过测量尿中环磷酸腺苷(cAMP)排泄来监测甲状旁腺功能。通过测量尿羟脯氨酸排泄来监测骨吸收。单独补充盐会增加尿钙、cAMP和羟脯氨酸;单独使用泼尼松龙会降低净钙吸收和尿羟脯氨酸,但对尿钙无影响。盐和泼尼松龙各自独立地降低钙潴留,并且共同对钙平衡产生累加的不利影响。因此,在饮食钙摄入受限的泼尼松龙治疗的生长大鼠中,高盐饮食会增加尿钙流失、提高甲状旁腺活性、增加骨吸收并对钙平衡产生不利影响。这些发现支持了高盐摄入可能会加剧慢性糖皮质激素治疗期间骨质流失这一观点。由于人们在糖皮质激素治疗期间也会发生骨质疏松症,并且对膳食盐补充剂的反应是增加尿钙排泄和甲状旁腺激素,高盐摄入可能会加速接受慢性糖皮质激素治疗患者的骨质流失。饮食限盐对保存骨量的有益作用值得在这些患者中进行研究。

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