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Molecular and cellular pathology of very-long-chain acyl-CoA dehydrogenase deficiency.


ABSTRACT:

Background

Very-long-chain acyl-CoA dehydrogenase (VLCAD) deficiency (VLCADD) is diagnosed in the US through newborn screening (NBS). NBS often unequivocally identifies affected individuals, but a growing number of variant patterns can represent mild disease or heterozygous carriers.

Aims

To evaluate the validity of standard diagnostic procedures for VLCADD by using functional in vitro tools.

Methods

We retrospectively investigated 13 patient samples referred to our laboratory because of a suspicion of VLCADD but with some uncertainty to the diagnosis. All 13 patients were suspected of having VLCADD either because of abnormal NBS or suggestive clinical findings. ACADVL genomic DNA sequencing data were available for twelve of them. Ten of the patients had an abnormal NBS suggestive of VLCADD, with three samples showing equivocal results. Three exhibited suggestive clinical findings and blood acylcarnitine profile (two of them had a normal NBS and the third one was unscreened). Assay of VLCAD activity and immunoblotting or immunohistologic staining for VLCAD were performed on fibroblasts. Prokaryotic mutagenesis and expression studies were performed for nine uncharacterized ACADVL missense mutations.

Results

VLCAD activity was abnormal in fibroblast cells from 9 patients (8 identified through abnormal NBS, 1 through clinical symptoms). For these 9 patients, immunoblotting/staining showed the variable presence of VLCAD; all but one had two mutated alleles. Two patients with equivocal NBS results (and a heterozygous genotype) and the two patients with normal NBS exhibited normal VLCAD activity and normal VLCAD protein on immunoblotting/staining thus ruling out VLCAD deficiency. Nine pathogenic missense mutations were characterized with prokaryotic expression studies and showed a decrease in enzyme activity and variable stability of VLCAD antigen.

Conclusions

These results emphasize the importance of functional investigation of abnormal NBS or clinical testing suggestive but not diagnostic of VLCADD. A larger prospective study is necessary to better define the clinical and metabolic ramifications of the defects identified in such patients.

SUBMITTER: Schiff M 

PROVIDER: S-EPMC3628282 | biostudies-literature | 2013 May

REPOSITORIES: biostudies-literature

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Publications

Molecular and cellular pathology of very-long-chain acyl-CoA dehydrogenase deficiency.

Schiff Manuel M   Mohsen Al-Walid AW   Karunanidhi Anuradha A   McCracken Elizabeth E   Yeasted Renita R   Vockley Jerry J  

Molecular genetics and metabolism 20130213 1


<h4>Background</h4>Very-long-chain acyl-CoA dehydrogenase (VLCAD) deficiency (VLCADD) is diagnosed in the US through newborn screening (NBS). NBS often unequivocally identifies affected individuals, but a growing number of variant patterns can represent mild disease or heterozygous carriers.<h4>Aims</h4>To evaluate the validity of standard diagnostic procedures for VLCADD by using functional in vitro tools.<h4>Methods</h4>We retrospectively investigated 13 patient samples referred to our laborat  ...[more]

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