Beyond predicting diagnosis: Is there a role for measuring biotinidase activity in liver glycogen storage diseases?

dc.contributor.author

El-Gharbawy, Areeg

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Tolun, Adviye A

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Halaby, Carine A

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Austin, Stephanie L

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Kishnani, Priya S

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Bali, Deeksha S

dc.date.accessioned

2023-03-01T14:29:59Z

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2023-03-01T14:29:59Z

dc.date.issued

2022-06

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2023-03-01T14:29:58Z

dc.description.abstract

Introduction

Biotinidase synthesis is needed to recycle biotin for essential metabolic reactions. Biotinidase activity is lower than normal levels in advanced liver disease but is higher in hepatic glycogen storage disorders (GSDs), however the cause of this association remains unclear.

Methods

In this study, biotinidase activity was measured in plasma samples from 45 individuals with hepatic GSDs; GSDI (a, b; n = 25) and GSD III (a, b; n = 20), complemented by a chart review to associate biotinidase activity levels with clinical laboratory and imaging findings known to be implicated in these GSDs.

Results

Our findings showed variation in biotinidase activity levels among subjects with GSD I and III; biotinidase activity correlated positively with hypertriglyceridemia in subjects with GSD I (r = 0.47, P = 0.036) and GSD III (r = 0.58, P = 0.014), and correlated negatively with age (r = -0.50, P = 0.03) in patients with GSD III. Additionally, biotinidase activity was reduced, albeit within the normal range in subjects with evidence of fibrosis/cirrhosis, as compared to subjects with hepatomegaly with or without steatosis (P = 0.002).

Discussions

These findings suggest that abnormal lipid metabolism in GSD I and III and progressive liver disease in GSD III may influence biotinidase activity levels. We suggest that a prospective, multi-center, longitudinal study designed to assess the significance of monitoring biotinidase activity in a larger cohort with hepatic GSDs is warranted to confirm this observation.

Take-home message

Altered lipid metabolism and advancing liver fibrosis/cirrhosis may influence biotinidase activity levels in patients with hepatic glycogen storage disease. Thus, longitudinal monitoring of biotinidase activity, when combined with clinical and other biochemical findings may be informative.
dc.identifier

S2214-4269(22)00016-7

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2214-4269

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2214-4269

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https://hdl.handle.net/10161/26669

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eng

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Elsevier BV

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Molecular genetics and metabolism reports

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10.1016/j.ymgmr.2022.100856

dc.subject

Biomarker

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Biotinidase

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GSD type I

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GSD type III

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Hepatic glycogen storage disease

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Long-term disease monitoring

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Beyond predicting diagnosis: Is there a role for measuring biotinidase activity in liver glycogen storage diseases?

dc.type

Journal article

duke.contributor.orcid

Kishnani, Priya S|0000-0001-8251-909X

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Bali, Deeksha S|0000-0003-2550-8073

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100856

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Duke

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School of Medicine

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Basic Science Departments

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Clinical Science Departments

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Institutes and Centers

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Molecular Genetics and Microbiology

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Pediatrics

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Pediatrics, Medical Genetics

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Duke Clinical Research Institute

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Institutes and Provost's Academic Units

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Initiatives

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Duke Innovation & Entrepreneurship

pubs.publication-status

Published

pubs.volume

31

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