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新生儿败血症对极低出生体重早产儿骨转换的影响。

The effect of neonatal sepsis on bone turnover in very-low birth weight premature infants.

作者信息

Eliakim Alon, Shiff Yaakov, Nemet Dan, Dolfin Tzipora

机构信息

Neonatal Intensive Care Unit, Meir General Hospital, Kfar Saba, Israel.

出版信息

J Pediatr Endocrinol Metab. 2003 Mar;16(3):413-8. doi: 10.1515/jpem.2003.16.3.413.

Abstract

Neonatal sepsis is very common in preterm infants, and severe morbidity during the neonatal period is a major cause of osteopenia of prematurity. We examined the effect of neonatal sepsis on bone turnover markers in premature infants. Twenty-four premature infants participated in the study. Ten of the premature infants developed sepsis during their hospitalization in the neonatal intensive care unit (mean gestational age [GA] 27.3 +/- 0.4 weeks; mean birth weight [BW] 898 +/- 82 g). Fourteen infants who did not develop sepsis served as controls (GA: 26.8 +/- 0.8 weeks, BW: 892 +/- 66 g). Blood samples for bone turnover markers were collected during the initial sepsis workup, and at the end of the first week of treatment, and were compared to the corresponding weekly changes in bone markers in the controls. In addition, samples were collected at the end of the 10th week of life to determine long-term effects of sepsis on bone turnover. Bone osteoblastic activity was assessed by measurements of circulating osteocalcin, bone-specific alkaline phosphatase (BSAP) and the C-terminal procollagen peptide (PICP) levels. Bone resorption was assessed by measurements of circulating carboxy terminal cross-links telopeptide of type I collagen (ICTP). There were no significant differences in the weekly changes of all bone turnover markers in premature infants who developed or did not develop sepsis. No significant differences were found in bone turnover markers at the age of 10 weeks between the groups. Neonatal sepsis in premature infants was not associated with biochemical evidence of reduced bone turnover.

摘要

新生儿败血症在早产儿中非常常见,新生儿期的严重发病是早产儿骨质减少的主要原因。我们研究了新生儿败血症对早产儿骨转换标志物的影响。24名早产儿参与了该研究。其中10名早产儿在新生儿重症监护病房住院期间发生了败血症(平均胎龄[GA]27.3±0.4周;平均出生体重[BW]898±82克)。14名未发生败血症的婴儿作为对照(GA:26.8±0.8周,BW:892±66克)。在最初的败血症检查期间以及治疗第一周结束时采集用于检测骨转换标志物的血样,并与对照组中骨标志物的相应每周变化进行比较。此外,在出生后第10周结束时采集样本,以确定败血症对骨转换的长期影响。通过测量循环中的骨钙素、骨特异性碱性磷酸酶(BSAP)和I型前胶原C端肽(PICP)水平来评估骨成骨细胞活性。通过测量循环中的I型胶原羧基末端交联端肽(ICTP)来评估骨吸收。发生或未发生败血症的早产儿所有骨转换标志物的每周变化均无显著差异。两组在10周龄时骨转换标志物未发现显著差异。早产儿的新生儿败血症与骨转换降低的生化证据无关。

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