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运用WINROP筛查算法预测巴西早产婴儿群体中的增殖性视网膜病变。

Predicting proliferative retinopathy in a Brazilian population of preterm infants with the screening algorithm WINROP.

作者信息

Hård Anna-Lena, Löfqvist Chatarina, Fortes Filho Joao Borges, Procianoy Renato Soibelmann, Smith Lois, Hellström Ann

机构信息

Department of Ophthalmology, Institute of Neuroscience and Physiology, University of Gothenburg, Gothenburg, Sweden.

出版信息

Arch Ophthalmol. 2010 Nov;128(11):1432-6. doi: 10.1001/archophthalmol.2010.255.

Abstract

OBJECTIVE

To retrospectively validate the WINROP (weight, insulinlike growth factor I, neonatal, retinopathy of prematurity [ROP]) algorithm in a Brazilian population. WINROP aims to predict ROP and is based on longitudinal weight measurements from birth until postmenstrual age 36 weeks. WINROP has predicted 100% of severe ROP in 3 neonatal intensive care unit settings in the United States and Sweden.

METHODS

In children admitted to the neonatal intensive care unit at Hospital de Clínicas de Porto Alegre, Porto Alegre, Brazil, from April 2002 to October 2008, weight measurements had been recorded once a week for children screened for ROP, 366 of whom had a gestational age of 32 weeks or less. The participating children had a median gestational age of 30 weeks (range, 24-32 weeks) at birth and their median birth weight was 1215 g (range, 505-2000 g).

RESULTS

For 192 of 366 children (53%), no alarm or low-risk alarm after postmenstrual age 32 weeks occurred. Of these, 190 of 192 did not develop proliferative disease. Two boys with severe sepsis who were treated for ROP received low-risk alarms at postmenstrual age 33 and 34 weeks, respectively. The remaining 174 children (47%) received high- or low-risk alarms before or at 32 weeks. Of these infants, 21 (12%) developed proliferative ROP.

CONCLUSIONS

In this Brazilian population, WINROP, with limited information on specific gestational age and date of weight measurement, detected early 90.5% of infants who developed stage 3 ROP and correctly predicted the majority who did not. Adjustments to the algorithm for specific neonatal intensive care unit populations may improve the results for specific preterm populations.

摘要

目的

在巴西人群中对WINROP(体重、胰岛素样生长因子I、新生儿、早产儿视网膜病变[ROP])算法进行回顾性验证。WINROP旨在预测ROP,其基于从出生到孕龄36周的纵向体重测量数据。WINROP在美国和瑞典的3个新生儿重症监护病房环境中预测出了100%的重度ROP。

方法

2002年4月至2008年10月期间,在巴西阿雷格里港临床医院新生儿重症监护病房收治的儿童中,每周对筛查ROP的儿童进行一次体重测量,其中366名儿童的孕龄为32周或更小。参与研究的儿童出生时的中位孕龄为30周(范围24 - 32周),中位出生体重为1215克(范围505 - 2000克)。

结果

366名儿童中有192名(53%)在孕龄达32周后未出现警报或低风险警报。其中,192名中的190名未发生增殖性疾病。两名因ROP接受治疗的患有严重脓毒症的男孩,分别在孕龄33周和34周时收到低风险警报。其余174名儿童(47%)在32周之前或32周时收到高风险或低风险警报。在这些婴儿中,21名(12%)发生了增殖性ROP。

结论

在这个巴西人群中,WINROP在关于特定孕龄和体重测量日期的信息有限的情况下,早期检测出了90.5%发生3期ROP的婴儿,并正确预测了大多数未发生ROP的婴儿。针对特定新生儿重症监护病房人群对该算法进行调整,可能会改善特定早产儿人群的预测结果。

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