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新西兰先天性甲状腺功能减退症国家新生儿筛查修订方案的评估。

Evaluation of the revised New Zealand national newborn screening protocol for congenital hypothyroidism.

作者信息

Heather Natasha L, Hofman Paul L, de Hora Mark, Carll Joan, Derraik José G B, Webster Dianne

机构信息

New Zealand Newborn Metabolic Screening Programme, LabPlus, Auckland District Health Board, Auckland, New Zealand.

Starship Children's Hospital, Auckland District Health Board, Auckland, New Zealand.

出版信息

Clin Endocrinol (Oxf). 2017 Mar;86(3):431-437. doi: 10.1111/cen.13250. Epub 2016 Oct 21.

DOI:10.1111/cen.13250
PMID:27696498
Abstract

OBJECTIVE

The aim of this study was to assess the performance of the revised New Zealand (NZ) newborn screening TSH cut-offs for congenital hypothyroidism (CHT).

METHODS

Screening data over 24 months were obtained from the NZ newborn metabolic screening programme, which utilizes a 2-tier system of direct clinical referral for infants with markedly elevated TSH, and second samples from those with mild TSH elevation. We evaluated the impact of a reduced TSH threshold (50 to 30 mIU/l blood) for direct notification and a lower cut-off (15 to 8 mIU/l blood) applied to second samples and babies older than 14 days.

RESULTS

In 2013 and 2014, 117 528 infants underwent newborn screening for CHT. Fifty-two CHT cases were identified by screening (47 general newborn population, five repeat testing in low-birth-weight infants) and one case was missed. Thirty-two infants with screening TSH ≥30 mIU/l were directly referred at a median of 9 days (5-14) and 15 with TSH 15-29 mIU/l were referred after a second sample at a median of 20 days (9-52, P < 0·001). All directly referred infants were confirmed as CHT cases with no earlier referrals as a result of the reduced threshold. The lower TSH cut-off applied to second samples lead to the identification of six extra cases of CHT (15% increase) from seven extra clinical referrals.

CONCLUSIONS

The NZ screening programme achieved a 15% increase in CHT case detection for minimal increase in workload or anxiety for families of healthy infants. A further decrease in the threshold for direct referral may allow earlier diagnoses.

摘要

目的

本研究旨在评估修订后的新西兰(NZ)先天性甲状腺功能减退症(CHT)新生儿筛查促甲状腺激素(TSH)临界值的性能。

方法

从NZ新生儿代谢筛查项目中获取了24个月的筛查数据,该项目采用两级系统,对于TSH明显升高的婴儿直接进行临床转诊,对于TSH轻度升高的婴儿采集第二份样本。我们评估了降低直接通知的TSH阈值(从50降至30 mIU/L血液)以及应用于第二份样本和14日龄以上婴儿的更低临界值(从15降至8 mIU/L血液)的影响。

结果

2013年和2014年,117528名婴儿接受了CHT新生儿筛查。通过筛查确定了52例CHT病例(47例来自普通新生儿群体,5例为低体重儿重复检测),漏诊1例。32例筛查TSH≥30 mIU/L的婴儿在中位数9天(5 - 14天)时直接转诊,15例TSH为15 - 29 mIU/L的婴儿在采集第二份样本后于中位数20天(9 - 52天)转诊(P < 0.001)。所有直接转诊的婴儿均被确诊为CHT病例,且由于阈值降低没有更早的转诊情况。应用于第二份样本的更低TSH临界值通过额外的7次临床转诊发现了6例额外的CHT病例(增加了15%)。

结论

NZ筛查项目在工作量或对健康婴儿家庭的焦虑增加最小的情况下,CHT病例检测增加了15%。进一步降低直接转诊的阈值可能会实现更早的诊断。

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