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早产儿中骨化三醇导致血清钙和骨钙素水平升高。一项前瞻性随机研究。

Elevated serum calcium and osteocalcin levels from calcitriol in preterm infants. A prospective randomized study.

作者信息

Koo W W, Tsang R C, Poser J W, Laskarzewski P, Buckley D, Johnson R, Steichen J J

出版信息

Am J Dis Child. 1986 Nov;140(11):1152-8. doi: 10.1001/archpedi.1986.02140250078039.

Abstract

The hypothesis of this study was that pharmacologic doses of calcitriol (1,25-dihydroxyvitamin D3) would result in elevated levels of serum osteocalcin, the major noncollagenous bone protein, and calcium in infants of very low birth weight (less than 1500 g). Twenty-four infants of very low birth weight but of the appropriate weight for gestational age were matched in 250-g weight ranges and randomized into calcitriol treatment and control groups on the first day after birth. Treated infants received 4 micrograms/kg of calcitriol intravenously on entry and on the second and third study days. Controls did not receive calcitriol. Four infants from each group were hypocalcemic (serum calcium level, less than 7.0 mg/dL [less than 1.75 mmol/L]) on entry (five to 20 hours after birth) to the study. Seven infants received calcium replacement; data analyses with and without these infants were similar. Of the remaining 17 infants, eight were in the treatment group and nine were in the control group. Calcitriol significantly increased serum calcium and osteocalcin concentrations on days 2, 3, and 4 after birth compared with the control group. None of eight treated infants manifested hypocalcemia after calcitriol vs eight of nine controls. There were no acute changes in heart rate, respiratory rate, systolic blood pressure, or urinary calcium loss nor were there changes at the infusion site, but the diastolic blood pressure increased with treatment. Although high doses of calcitriol may elevate serum calcium concentrations in infants of very low birth weight, we suggest that the long-term or subtle biologic effects of high doses of calcitriol remain to be studied and that its routine use not be recommended at present.

摘要

本研究的假设是,药理剂量的骨化三醇(1,25 - 二羟维生素D3)会使极低出生体重(低于1500克)婴儿的血清骨钙素(主要的非胶原蛋白骨蛋白)和钙水平升高。24名极低出生体重但孕周合适的婴儿按250克体重范围进行匹配,并在出生后的第一天随机分为骨化三醇治疗组和对照组。治疗组婴儿在入组时以及研究的第二天和第三天静脉注射4微克/千克骨化三醇。对照组未接受骨化三醇治疗。每组有4名婴儿在入组研究时(出生后5至20小时)血钙过低(血清钙水平低于7.0毫克/分升[低于1.75毫摩尔/升])。7名婴儿接受了钙剂补充;纳入或不纳入这些婴儿的数据分析结果相似。在其余17名婴儿中,8名在治疗组,9名在对照组。与对照组相比,骨化三醇在出生后第2、3和4天显著提高了血清钙和骨钙素浓度。8名接受治疗的婴儿在使用骨化三醇后均未出现低钙血症,而9名对照组婴儿中有8名出现低钙血症。心率、呼吸频率、收缩压或尿钙流失均无急性变化,输液部位也无变化,但舒张压随治疗而升高。尽管高剂量骨化三醇可能会提高极低出生体重婴儿的血清钙浓度,但我们建议,高剂量骨化三醇的长期或细微生物学效应仍有待研究,目前不建议常规使用。

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