标准化婴儿神经发育评估(SINDA)在低风险样本中识别4-5岁发育迟缓风险儿童的预测效度。
Predictive validity of the Standardized Infant NeuroDevelopmental Assessment (SINDA) to identify 4-5 year-old children at risk of developmental delay in a low-risk sample.
作者信息
Rosinda Selena J, Hoekstra Pieter J, Hadders-Algra Mijna, de Bildt Annelies, Heineman Kirsten R
机构信息
University of Groningen, University Medical Center Groningen, Department of Child and Adolescent Psychiatry, Groningen, the Netherlands; University of Groningen, University Medical Center Groningen, Department of Paediatrics, Beatrix Children's Hospital, Division of Developmental Neurology, Groningen, the Netherlands; Accare Child Study Center, Groningen, the Netherlands.
University of Groningen, University Medical Center Groningen, Department of Child and Adolescent Psychiatry, Groningen, the Netherlands; Accare Child Study Center, Groningen, the Netherlands.
出版信息
Early Hum Dev. 2024 Sep;196:106097. doi: 10.1016/j.earlhumdev.2024.106097. Epub 2024 Aug 5.
BACKGROUND
Early detection of developmental problems is important as it allows for early intervention. Previous studies, in high-risk infants, found high predictive values of atypical scores on the Standardized Infant NeuroDevelopmental Assessment (SINDA) for later neurodevelopmental disorders (i.e., cerebral palsy, intellectual disability).
AIMS
The present study explored SINDA's predictive values to identify risk of developmental delay at 4-5 years.
STUDY DESIGN
Cohort study.
SUBJECTS
786 low-risk Dutch children (367 boys; median gestational age: 40 (27-42) weeks; mean birth weight: 3455 (SD 577) grams).
OUTCOME MEASURES
The SINDA was assessed at 2-12 months and risk of developmental delay was assessed using the Ages and Stages Questionnaire (ASQ) at 4-5 years. SINDA's predictive values were determined for five ASQ domains and the total ASQ score for children at risk of marked (all ASQ domains deviant) and any (one or more ASQ domains deviant) developmental delay.
RESULTS
Presence of one atypical SINDA scale score showed low to moderate sensitivities (12-88 %, depending on the SINDA scale and ASQ domain involved), moderate to high specificities (66-94 %), low positive predictive values (PPVs; 3-16 %), and high negative predictive values (NPVs; 95-100 %) for children at risk of marked and any developmental. Presence of multiple atypical SINDA scale scores predicted deviant ASQ domains slightly better (sensitivities = 11-62 %, specificities = 90-98 %, PPVs = 6-30 %, and NPVs = 95-100 %).
CONCLUSIONS
In low-risk infants, SINDA's predictive value is low for detecting children at risk of marked and any developmental delay at 4-5 years, as reflected by the low sensitivities. One of the explanations is the relatively low prevalence of developmental delay in low-risk populations. This might have consequences for the application of the SINDA in general healthcare settings (e.g. child health clinics), but further studies are needed to draw this conclusion.
背景
早期发现发育问题很重要,因为这有助于早期干预。先前针对高危婴儿的研究发现,标准化婴儿神经发育评估(SINDA)中的非典型分数对后期神经发育障碍(如脑瘫、智力残疾)具有较高的预测价值。
目的
本研究探讨了SINDA对识别4至5岁发育迟缓风险的预测价值。
研究设计
队列研究。
研究对象
786名荷兰低风险儿童(367名男孩;中位胎龄:40(27 - 42)周;平均出生体重:3455(标准差577)克)。
观察指标
在2至12个月时进行SINDA评估,并在4至5岁时使用年龄与发育进程问卷(ASQ)评估发育迟缓风险。确定了SINDA对于有明显发育迟缓风险(所有ASQ领域均异常)和任何发育迟缓风险(一个或多个ASQ领域异常)儿童的五个ASQ领域以及总ASQ分数的预测价值。
结果
存在一个非典型SINDA量表分数对有明显发育迟缓和任何发育迟缓风险的儿童显示出低至中度的敏感性(12 - 88%,取决于所涉及的SINDA量表和ASQ领域)、中度至高特异性(66 - 94%)、低阳性预测值(PPV;3 - 16%)和高阴性预测值(NPV;95 - 100%)。存在多个非典型SINDA量表分数对异常ASQ领域的预测略好(敏感性 = 11 - 62%,特异性 = 90 - 98%,PPV = 6 - 30%,NPV = 95 - 100%)。
结论
在低风险婴儿中,SINDA对检测4至5岁有明显发育迟缓和任何发育迟缓风险儿童的预测价值较低,这体现在敏感性较低。其中一个解释是低风险人群中发育迟缓的患病率相对较低。这可能会对SINDA在一般医疗环境(如儿童健康诊所)中的应用产生影响,但需要进一步研究来得出这一结论。
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