AI Article Synopsis
- * Recent research has expanded the understanding of how different mutations in the ARSA gene affect disease severity by studying both common and rare mutations.
- * The study identified eight new mutations and found that the level of enzyme activity linked to these mutations correlates with patient symptoms, emphasizing the need for detailed analysis to aid in diagnosing and predicting patient outcomes.
Article Abstract
Metachromatic Leukodystrophy (MLD) is a rare inherited lysosomal storage disorder caused by the deficiency of Arylsulfatase A (ARSA). The disease manifests itself with a broad spectrum of clinical variants, all characterized by progressive neurodegeneration in the central and peripheral nervous systems. The correlation between mutations in the ARSA gene, residual enzymatic activity associated with the mutated alleles and patients' phenotype, which has been extensively drawn for common ARSA mutations, has recently been expanded to rare ones. In this context, functional studies on the rare allelic variances acquire particular relevance for patients' prognostic evaluation. Here we have characterized eight newly identified ARSA mutations, through lentiviral vector-based expression studies on cell lines and ARSA defective murine fibroblasts. In each case, the residual activity associated with the new mutant allele correlates well with the patient's phenotype. Therefore, our results confirm the importance of functional characterization of mutant alleles for a precise genotype-based classification and definition of prognosis in MLD patients, which is particularly relevant for pre-symptomatic diagnosis.
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| http://dx.doi.org/10.1002/humu.21093 | DOI Listing |
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