Biotinidase deficiency: Spectrum of molecular, enzymatic and clinical information from newborn screening Ontario, Canada (2007-2014)

Srinitya Gannavarapu; Chitra Prasad; Jennifer DiRaimo; Melanie Napier; Sharan Goobie; Murray Potter; Pranesh Chakraborty; Maria Karaceper; Tatiana Munoz; Andreas Schulze; Jennifer MacKenzie; Lihua Li; Michael T. Geraghty; Osama Y. Al-Dirbashi; C. Anthony Rupar

doi:10.1016/j.ymgme.2015.08.010

Biotinidase deficiency: Spectrum of molecular, enzymatic and clinical information from newborn screening Ontario, Canada (2007-2014)

Srinitya Gannavarapu, Chitra Prasad, Jennifer DiRaimo, Melanie Napier, Sharan Goobie, Murray Potter, Pranesh Chakraborty, Maria Karaceper, Tatiana Munoz, Andreas Schulze, Jennifer MacKenzie, Lihua Li, Michael T. Geraghty, Osama Y. Al-Dirbashi, C. Anthony Rupar

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19 Citas (Scopus)

Resumen

Untreated profound biotinidase deficiency results in a wide range of clinical features, including optic atrophy, cutaneous abnormalities, hearing loss and developmental delay. Ontario, Canada incorporated this treatable deficiency in newborn screening over the past 8. years. This study elucidates the molecular, biochemical, and clinical findings from the pilot project. Information from initial screens, serum biotinidase activity level assays, molecular testing, and family history for 246 positive newborns screens were analyzed. A mutation spectrum was created for the province of Ontario, including common mutations such as D444H, D444H/A171T, Q456H, C33fs, and R157H. Individuals with partial deficiency were separated into 3 groups: D444H homozygotes (Group 1); compound heterozygotes for D444H with another profound allele (Group 2); compound heterozygotes with two non-D444H alleles (Group 3). Biochemical phenotype-genotype associations in partial deficiency showed a significant difference in serum biotinidase activity in between any given two groups. Three children with partial deficiency discontinued biotin for varied lengths of time. Two of whom became symptomatic with abnormal gait, alopecia, skin rashes and developmental delay. A need for more congruency in diagnostic, treatment and educational practices was highlighted across the province. Heterogeneity and variation in clinical presentations and management was observed in patients with the partial deficiency.

Idioma original	English
Páginas (desde-hasta)	146-151
Número de páginas	6
Publicación	Molecular Genetics and Metabolism
Volumen	116
N.º	3
DOI	https://doi.org/10.1016/j.ymgme.2015.08.010
Estado	Published - nov. 2015
Publicado de forma externa	Sí

Nota bibliográfica

Funding Information:
The authors would like to thank the laboratory members and genetic counselors of metabolic teams at the Hospital for Sick Children, Newborn Screening Ontario (NSO) and London Health Sciences Center: Betty Wan, Dina Grespan, Dr. Jack Rip, Gulanaar Hassam, Mehrdad Yazdanpanah, Roger Dewar, Suzanne Waddel, and Wendy McCaul. We would also like to thank Dr. Barry Wolf, for his helpful discussion and guidance. The project was funded by Children's Foundation (Grant No. 2315 ) at the Children's Hospital, London Health Sciences Centre (LHSC), London Ontario, Canada.

Publisher Copyright:
© 2015 Elsevier Inc..

ASJC Scopus Subject Areas

Endocrinology, Diabetes and Metabolism
Biochemistry
Molecular Biology
Genetics
Endocrinology

ODS de las Naciones Unidas

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Gannavarapu, S., Prasad, C., DiRaimo, J., Napier, M., Goobie, S., Potter, M., Chakraborty, P., Karaceper, M., Munoz, T., Schulze, A., MacKenzie, J., Li, L., Geraghty, M. T., Al-Dirbashi, O. Y., & Rupar, C. A. (2015). Biotinidase deficiency: Spectrum of molecular, enzymatic and clinical information from newborn screening Ontario, Canada (2007-2014). Molecular Genetics and Metabolism, 116(3), 146-151. https://doi.org/10.1016/j.ymgme.2015.08.010

Gannavarapu, S, Prasad, C, DiRaimo, J, Napier, M, Goobie, S, Potter, M, Chakraborty, P, Karaceper, M, Munoz, T, Schulze, A, MacKenzie, J, Li, L, Geraghty, MT, Al-Dirbashi, OY & Rupar, CA 2015, 'Biotinidase deficiency: Spectrum of molecular, enzymatic and clinical information from newborn screening Ontario, Canada (2007-2014)', Molecular Genetics and Metabolism, vol. 116, n.º 3, pp. 146-151. https://doi.org/10.1016/j.ymgme.2015.08.010

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title = "Biotinidase deficiency: Spectrum of molecular, enzymatic and clinical information from newborn screening Ontario, Canada (2007-2014)",

abstract = "Untreated profound biotinidase deficiency results in a wide range of clinical features, including optic atrophy, cutaneous abnormalities, hearing loss and developmental delay. Ontario, Canada incorporated this treatable deficiency in newborn screening over the past 8. years. This study elucidates the molecular, biochemical, and clinical findings from the pilot project. Information from initial screens, serum biotinidase activity level assays, molecular testing, and family history for 246 positive newborns screens were analyzed. A mutation spectrum was created for the province of Ontario, including common mutations such as D444H, D444H/A171T, Q456H, C33fs, and R157H. Individuals with partial deficiency were separated into 3 groups: D444H homozygotes (Group 1); compound heterozygotes for D444H with another profound allele (Group 2); compound heterozygotes with two non-D444H alleles (Group 3). Biochemical phenotype-genotype associations in partial deficiency showed a significant difference in serum biotinidase activity in between any given two groups. Three children with partial deficiency discontinued biotin for varied lengths of time. Two of whom became symptomatic with abnormal gait, alopecia, skin rashes and developmental delay. A need for more congruency in diagnostic, treatment and educational practices was highlighted across the province. Heterogeneity and variation in clinical presentations and management was observed in patients with the partial deficiency.",

author = "Srinitya Gannavarapu and Chitra Prasad and Jennifer DiRaimo and Melanie Napier and Sharan Goobie and Murray Potter and Pranesh Chakraborty and Maria Karaceper and Tatiana Munoz and Andreas Schulze and Jennifer MacKenzie and Lihua Li and Geraghty, {Michael T.} and Al-Dirbashi, {Osama Y.} and Rupar, {C. Anthony}",

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AU - Prasad, Chitra

AU - DiRaimo, Jennifer

AU - Napier, Melanie

AU - Goobie, Sharan

AU - Potter, Murray

AU - Chakraborty, Pranesh

AU - Karaceper, Maria

AU - Munoz, Tatiana

AU - Schulze, Andreas

AU - MacKenzie, Jennifer

AU - Li, Lihua

AU - Geraghty, Michael T.

AU - Al-Dirbashi, Osama Y.

AU - Rupar, C. Anthony

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Biotinidase deficiency: Spectrum of molecular, enzymatic and clinical information from newborn screening Ontario, Canada (2007-2014)

Resumen

Nota bibliográfica

ASJC Scopus Subject Areas

ODS de las Naciones Unidas

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