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采用连续测定B型利钠肽对极早产儿有症状动脉导管未闭进行个体化布洛芬治疗。

Individualized ibuprofen treatment using serial B-type natriuretic peptide measurement for symptomatic patent ductus arteriosus in very preterm infants.

作者信息

Shin Jeonghee, Lee Eun Hee, Lee Jee Hyun, Choi Byung Min, Hong Young Sook

机构信息

Department of Pediatrics, Korea University College of Medicine, Seoul, Korea.

出版信息

Korean J Pediatr. 2017 Jun;60(6):175-180. doi: 10.3345/kjp.2017.60.6.175. Epub 2017 Jun 22.

Abstract

PURPOSE

Plasma level of B-type natriuretic peptide (BNP), an emerging, sensitive, and specific biomarker of hemodynamically significant patent ductus arteriosus (PDA), rapidly decreases in infants receiving cyclooxygenase inhibitors for ductal closure. We investigated the usefulness of serial BNP measurement as a guide for individual identification of early constrictive responses to ibuprofen in preterm infants with symptomatic PDA (sPDA).

METHODS

Before March 2010, the standard course of pharmacological treatment was initiated with indomethacin (or ibuprofen) and routinely followed by 2 additional doses at intervals of 24 hours. After April 2010, individualized pharmacological treatment was used, starting with the first dose of ibuprofen and withholding additional ibuprofen doses if the BNP concentration was <600 pg/mL and clinical symptoms of PDA improved.

RESULTS

The BNP-guided group received significantly fewer doses of ibuprofen than the standard group did during the first course of treatment and the entire study period. The need for further doses of cyclooxygenase inhibitors and for surgical ligation was not significantly different between the 2 groups. No significant differences were seen in clinical outcomes and/or complications related to sPDA and/or pharmacological treatment.

CONCLUSION

Individualized BNP-guided pharmacological treatment may be used clinically to avoid unnecessary doses of cyclooxygenase inhibitors without increasing the ductal closure failure and the short-term morbidity related to sPDA.

摘要

目的

B型利钠肽(BNP)血浆水平是血流动力学显著的动脉导管未闭(PDA)一种新出现的、敏感且特异的生物标志物,在接受环氧化酶抑制剂以促使导管闭合的婴儿中会迅速下降。我们研究了连续测量BNP作为指导,用于个别识别有症状PDA(sPDA)的早产儿对布洛芬早期收缩反应的有用性。

方法

2010年3月之前,药物治疗的标准疗程以吲哚美辛(或布洛芬)开始,并常规间隔24小时再给予两剂。2010年4月之后,采用个体化药物治疗,从第一剂布洛芬开始,如果BNP浓度<600 pg/mL且PDA临床症状改善,则不再给予额外的布洛芬剂量。

结果

在第一个疗程和整个研究期间,BNP指导组接受的布洛芬剂量明显少于标准组。两组在进一步使用环氧化酶抑制剂和手术结扎的必要性方面没有显著差异。在与sPDA和/或药物治疗相关的临床结局和/或并发症方面未观察到显著差异。

结论

个体化的BNP指导药物治疗可在临床上用于避免不必要的环氧化酶抑制剂剂量,而不会增加导管闭合失败率以及与sPDA相关的短期发病率。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4c97/5500385/bab1b8e65848/kjped-60-175-g001.jpg

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