How Well Does the Capillary Thyroid-stimulating Hormone Test for Newborn Thyroid Screening Predict the Venous Free Thyroxine Level?

Overview

Journal Arch Dis Child

Specialty Pediatrics

Date 2016 Mar 12

PMID 26966265

Citations 4

Authors

Tzveta Pokrovska

Jeremy Jones

M Guftar Shaikh

Sarah Smith

Malcolm D C Donaldson

Affiliations

Soon will be listed here.

Abstract

Objectives: To determine, in newborn infants referred with elevated capillary thyroid-stimulating hormone (TSH), a threshold below which a frankly subnormal venous free thyroxine (fT4) level of <10 pmol/L is unlikely, so that treatment with levo-thyroxine (L-T4) might be deferred until venous thyroid function tests (TFTs) become available.

Subjects And Methods: All infants referred in Scotland since 1979 with capillary TSH elevation were studied, with particular focus on infants screened using the AutoDELFIA assay between 2002 and 2013.

Results: Of the 321 infants referred with capillary TSH elevation using AutoDELFIA, 35 were excluded (fT4/TSH unavailable (12), venous sample either preceding or >10 days after capillary sampling (13, 10)), leaving 286 eligible for analysis (208 definite/probable hypothyroidism, 61 transient TSH elevation, 17 of uncertain thyroid status). Capillary TSH and venous T4 were strongly correlated (Spearman's rank correlation coefficient -0.707355). The optimal capillary TSH threshold for predicting a venous fT4 of <10 pmol/L was found to be >40 mU/L (90.3% sensitivity and 65.9% specificity compared with 90.25% and 59.1% for >35 mU/L and 88.3% and 68.2% for >45 mU/L). 93 infants (32.5%) had capillary TSH ≤40 mU/L at referral of whom 15 (9.7%) had venous fT4 <10 pmol/L, comprising seven with true congenital hypothyroidism, five with transient TSH elevation and three with uncertain status, two of whom died.

Conclusion: For infants in whom capillary TSH is ≤40 mU/L, it is reasonable to defer L-T4 treatment until venous TFT results are known provided that the latter become available quickly.

Citing Articles

An Overview on Different L-Thyroxine (l-T) Formulations and Factors Potentially Influencing the Treatment of Congenital Hypothyroidism During the First 3 Years of Life.

Stagi S, Municchi G, Ferrari M, Wasniewska M Front Endocrinol (Lausanne). 2022; 13:859487.

PMID: 35757415 PMC: 9218053. DOI: 10.3389/fendo.2022.859487.

Primary Thyroid Stimulating Hormone Screening for Congenital Hypothyroidism in King Abdullah Hospital, Bisha, Saudi Arabia.

Abbas M, Tayrab E, Elmakki A, Tayrab J, Al-Shahrani A, Miskeen E Cureus. 2020; 12(3):e7166.

PMID: 32190524 PMC: 7057246. DOI: 10.7759/cureus.7166.

Newborn Screening Guidelines for Congenital Hypothyroidism in India: Recommendations of the Indian Society for Pediatric and Adolescent Endocrinology (ISPAE) - Part I: Screening and Confirmation of Diagnosis.

Desai M, Sharma R, Riaz I, Sudhanshu S, Parikh R, Bhatia V Indian J Pediatr. 2018; 85(6):440-447.

PMID: 29380252 DOI: 10.1007/s12098-017-2575-y.

Trends in Scottish newborn screening programme for congenital hypothyroidism 1980-2014: strategies for reducing age at notification after initial and repeat sampling.

Mansour C, Ouarezki Y, Jones J, Fitch M, Smith S, Mason A Arch Dis Child. 2017; 102(10):936-941.

PMID: 28600385 PMC: 5739820. DOI: 10.1136/archdischild-2016-312156.

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