Incorporation of second-tier biomarker testing improves the specificity of newborn screening for mucopolysaccharidosis type i

Dawn S. Peck; Jean M. Lacey; Amy L. White; Gisele Pino; April L. Studinski; Rachel Fisher; Ayesha Ahmad; Linda Spencer; Sarah Viall; Natalie Shallow; Amy Siemon; J. Austin Hamm; Brianna K. Murray; Kelly L. Jones; Dimitar Gavrilov; Devin Oglesbee; Kimiyo Raymond; Dietrich Matern; Piero Rinaldo; Silvia Tortorelli

doi:10.3390/ijns6010010

Incorporation of second-tier biomarker testing improves the specificity of newborn screening for mucopolysaccharidosis type i

Dawn S. Peck, Jean M. Lacey, Amy L. White, Gisele Pino, April L. Studinski, Rachel Fisher, Ayesha Ahmad, Linda Spencer, Sarah Viall, Natalie Shallow, Amy Siemon, J. Austin Hamm, Brianna K. Murray, Kelly L. Jones, Dimitar Gavrilov, Devin Oglesbee, Kimiyo Raymond, Dietrich Matern, Piero Rinaldo, Silvia Tortorelli

Laboratory Medicine and Pathology

Research output: Contribution to journal › Article › peer-review

4 Scopus citations

Abstract

Enzyme-based newborn screening for Mucopolysaccharidosis type I (MPS I) has a high false-positive rate due to the prevalence of pseudodeficiency alleles, often resulting in unnecessary and costly follow up. The glycosaminoglycans (GAGs), dermatan sulfate (DS) and heparan sulfate (HS) are both substrates for α-L-iduronidase (IDUA). These GAGs are elevated in patients with MPS I and have been shown to be promising biomarkers for both primary and second-tier testing. Since February 2016, we have measured DS and HS in 1213 specimens submitted on infants at risk for MPS I based on newborn screening. Molecular correlation was available for 157 of the tested cases. Samples from infants with MPS I confirmed by IDUA molecular analysis all had significantly elevated levels of DS and HS compared to those with confirmed pseudodeficiency and/or heterozygosity. Analysis of our testing population and correlation with molecular results identified few discrepant outcomes and uncovered no evidence of false-negative cases. We have demonstrated that blood spot GAGs analysis accurately discriminates between patients with confirmed MPS I and false-positive cases due to pseudodeficiency or heterozygosity and increases the specificity of newborn screening for MPS I.

Original language	English (US)
Article number	10
Journal	International Journal of Neonatal Screening
Volume	6
Issue number	1
DOIs	https://doi.org/10.3390/ijns6010010
State	Published - 2020

Keywords

Biomarkers
GAGs
MPS I
Newborn screening
Postanalytical interpretation
Second-tier testing

ASJC Scopus subject areas

Pediatrics, Perinatology, and Child Health
Immunology and Microbiology (miscellaneous)
Obstetrics and Gynecology

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10.3390/ijns6010010

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Peck, D. S., Lacey, J. M., White, A. L., Pino, G., Studinski, A. L., Fisher, R., Ahmad, A., Spencer, L., Viall, S., Shallow, N., Siemon, A., Hamm, J. A., Murray, B. K., Jones, K. L., Gavrilov, D., Oglesbee, D., Raymond, K., Matern, D., Rinaldo, P., & Tortorelli, S. (2020). Incorporation of second-tier biomarker testing improves the specificity of newborn screening for mucopolysaccharidosis type i. International Journal of Neonatal Screening, 6(1), Article 10. https://doi.org/10.3390/ijns6010010

Peck, DS, Lacey, JM, White, AL, Pino, G, Studinski, AL, Fisher, R, Ahmad, A, Spencer, L, Viall, S, Shallow, N, Siemon, A, Hamm, JA, Murray, BK, Jones, KL, Gavrilov, D, Oglesbee, D, Raymond, K, Matern, D, Rinaldo, P & Tortorelli, S 2020, 'Incorporation of second-tier biomarker testing improves the specificity of newborn screening for mucopolysaccharidosis type i', International Journal of Neonatal Screening, vol. 6, no. 1, 10. https://doi.org/10.3390/ijns6010010

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abstract = "Enzyme-based newborn screening for Mucopolysaccharidosis type I (MPS I) has a high false-positive rate due to the prevalence of pseudodeficiency alleles, often resulting in unnecessary and costly follow up. The glycosaminoglycans (GAGs), dermatan sulfate (DS) and heparan sulfate (HS) are both substrates for α-L-iduronidase (IDUA). These GAGs are elevated in patients with MPS I and have been shown to be promising biomarkers for both primary and second-tier testing. Since February 2016, we have measured DS and HS in 1213 specimens submitted on infants at risk for MPS I based on newborn screening. Molecular correlation was available for 157 of the tested cases. Samples from infants with MPS I confirmed by IDUA molecular analysis all had significantly elevated levels of DS and HS compared to those with confirmed pseudodeficiency and/or heterozygosity. Analysis of our testing population and correlation with molecular results identified few discrepant outcomes and uncovered no evidence of false-negative cases. We have demonstrated that blood spot GAGs analysis accurately discriminates between patients with confirmed MPS I and false-positive cases due to pseudodeficiency or heterozygosity and increases the specificity of newborn screening for MPS I.",

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doi = "10.3390/ijns6010010",

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AU - Peck, Dawn S.

AU - Lacey, Jean M.

AU - White, Amy L.

AU - Pino, Gisele

AU - Studinski, April L.

AU - Fisher, Rachel

AU - Ahmad, Ayesha

AU - Spencer, Linda

AU - Viall, Sarah

AU - Shallow, Natalie

AU - Siemon, Amy

AU - Hamm, J. Austin

AU - Murray, Brianna K.

AU - Jones, Kelly L.

AU - Gavrilov, Dimitar

AU - Oglesbee, Devin

AU - Raymond, Kimiyo

AU - Matern, Dietrich

AU - Rinaldo, Piero

AU - Tortorelli, Silvia

PY - 2020

Y1 - 2020

N2 - Enzyme-based newborn screening for Mucopolysaccharidosis type I (MPS I) has a high false-positive rate due to the prevalence of pseudodeficiency alleles, often resulting in unnecessary and costly follow up. The glycosaminoglycans (GAGs), dermatan sulfate (DS) and heparan sulfate (HS) are both substrates for α-L-iduronidase (IDUA). These GAGs are elevated in patients with MPS I and have been shown to be promising biomarkers for both primary and second-tier testing. Since February 2016, we have measured DS and HS in 1213 specimens submitted on infants at risk for MPS I based on newborn screening. Molecular correlation was available for 157 of the tested cases. Samples from infants with MPS I confirmed by IDUA molecular analysis all had significantly elevated levels of DS and HS compared to those with confirmed pseudodeficiency and/or heterozygosity. Analysis of our testing population and correlation with molecular results identified few discrepant outcomes and uncovered no evidence of false-negative cases. We have demonstrated that blood spot GAGs analysis accurately discriminates between patients with confirmed MPS I and false-positive cases due to pseudodeficiency or heterozygosity and increases the specificity of newborn screening for MPS I.

AB - Enzyme-based newborn screening for Mucopolysaccharidosis type I (MPS I) has a high false-positive rate due to the prevalence of pseudodeficiency alleles, often resulting in unnecessary and costly follow up. The glycosaminoglycans (GAGs), dermatan sulfate (DS) and heparan sulfate (HS) are both substrates for α-L-iduronidase (IDUA). These GAGs are elevated in patients with MPS I and have been shown to be promising biomarkers for both primary and second-tier testing. Since February 2016, we have measured DS and HS in 1213 specimens submitted on infants at risk for MPS I based on newborn screening. Molecular correlation was available for 157 of the tested cases. Samples from infants with MPS I confirmed by IDUA molecular analysis all had significantly elevated levels of DS and HS compared to those with confirmed pseudodeficiency and/or heterozygosity. Analysis of our testing population and correlation with molecular results identified few discrepant outcomes and uncovered no evidence of false-negative cases. We have demonstrated that blood spot GAGs analysis accurately discriminates between patients with confirmed MPS I and false-positive cases due to pseudodeficiency or heterozygosity and increases the specificity of newborn screening for MPS I.

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Incorporation of second-tier biomarker testing improves the specificity of newborn screening for mucopolysaccharidosis type i

Abstract

Keywords

ASJC Scopus subject areas

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