Abstract
The mucopolysaccharidoses (MPSs) include 11 different conditions caused by specific enzyme deficiencies in the degradation pathway of glycosaminoglycans (GAGs). Although most MPS types present increased levels of GAGs in tissues, including blood and urine, diagnosis is challenging as specific enzyme assays are needed for the correct diagnosis. Enzyme assays are usually performed in blood, with some samples (as leukocytes) providing a final diagnosis, while others (such as dried blood spots) still being considered as screening methods. The identification of variants in the specific genes that encode each MPS-related enzyme is helpful for diagnosis confirmation (when needed), carrier detection, genetic counseling, prenatal diagnosis (preferably in combination with enzyme assays) and phenotype prediction. Although the usual diagnostic flow in high-risk patients starts with the measurement of urinary GAGs, it continues with specific enzyme assays and is completed with mutation identification; there is a growing trend to have genotype-based investigations performed at the beginning of the investigation. In such cases, confirmation of pathogenicity of the variants identified should be confirmed by measurement of enzyme activity and/or identification and/or quantification of GAG species. As there is a growing number of countries performing newborn screening for MPS diseases, the investigation of a low enzyme activity by the measurement of GAG species concentration and identification of gene mutations in the same DBS sample is recommended before the suspicion of MPS is taken to the family. With specific therapies already available for most MPS patients, and with clinical trials in progress for many conditions, the specific diagnosis of MPS as early as possible is becoming increasingly necessary. In this review, we describe traditional and the most up to date diagnostic methods for mucopolysaccharidoses.
Highlights
The mucopolysaccharidoses (MPSs) comprises 11 lysosomal diseases in which there is a deficiency in a specific step of the degradation of glycosaminoglycans (GAGs)
We provide an overview of the tools available for the diagnosis of MPS, and it discusses the use of these tools in the investigation of suspected patients, in the screening of high-risk groups and in newborn screening
To aid clinicians in recognizing high-risk groups that should be investigated by selective screening, the combination of signs and symptoms of MPS may be summarized in suspicion scores or mnemonics
Summary
The mucopolysaccharidoses (MPSs) comprises 11 lysosomal diseases in which there is a deficiency in a specific step of the degradation of glycosaminoglycans (GAGs). This deficiency leads to storage of GAGs in tissues and to a range of clinical consequences, which may include CNS impairment, depending on the specific MPS type [1,2]. The diagnosis of MPSs is currently based on the evaluation of GAGs, measurement of enzyme activities and identification of genetic variants. We provide an overview of the tools available for the diagnosis of MPS, and it discusses the use of these tools in the investigation of suspected patients, in the screening of high-risk groups and in newborn screening
Sign-in/Register to view highlights & summary Sign-in/Register to access full text options 
Free) 
Talk to us
Join us for a 30 min session where you can share your feedback and ask us any queries you have
Schedule a call
