Optimizing the Molecular Diagnosis of GALNS: Novel Methods to Define and Characterize Morquio-A Syndrome-Associated Mutations

Caciotti, Anna; Tonin, Rodolfo; Rigoldi, Miriam; Ferri, Lorenzo; Catarzi, Serena; Cavicchi, Catia; Procopio, Elena; Ficcadenti, Anna; Fiumara, Agata; Barone, Rita; Garavelli, Livia; Rocco, Maja Di; Filocamo, Mirella; Antuzzi, Daniela; Scarpa, Maurizio; Mooney, Sean D.; Li, Biao; Bianca, Sebastiano; Concolino, Daniela; Casalone, Rosario; Monti, Elena; Pantaleo, Maria Abbondanza; Giglio, Sabrina; Guerrini, Renzo; Parini, Rossella; Morrone, Amelia

doi:10.1002/humu.22751

Cited by 28 publications

(26 citation statements)

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“…(Gly290Ser)–[59]Likely pathogenicc.1043C>Ap. (Thr348Asn)–[14]Likely pathogenicc.1156C>Tp. (Arg386Cys)rs118204437; ClinVar ID:700[43]Likely pathogenicc.1219A>Cp.…”

Section: Resultsmentioning

confidence: 99%

“…(Lys503Valfs*226)–[14]Likely pathogenicc.1519T>Cp. (Cys507Arg)–[14]Likely pathogenicc.1520G>Tp. (Cys507Phe)ClinVar ID:93169[40]Not enough evidenceNC_000016.9: g.88836836_88899132del62296––[14]Likely pathogenicc.1002+307G>C––[15]Not enough evidence GLB1 (NM_000404.3; NP_000395.2)Single nucleotide variationMissense variant–Novel; Morrone A et al in publication–c.817_818delinsCTp.…”

Section: Resultsmentioning

confidence: 99%

“…(Cys507Arg)–[14]Likely pathogenicc.1520G>Tp. (Cys507Phe)ClinVar ID:93169[40]Not enough evidenceNC_000016.9: g.88836836_88899132del62296––[14]Likely pathogenicc.1002+307G>C––[15]Not enough evidence GLB1 (NM_000404.3; NP_000395.2)Single nucleotide variationMissense variant–Novel; Morrone A et al in publication–c.817_818delinsCTp. (Trp273Leu)–[44]Likely pathogenicc.1480-2A>G–rs587776526; ClinVar ID: 946[39]Pathogenic ARSB (NM_000046.4; NP_000037.2)c.245T>Cp.…”

Section: Resultsmentioning

confidence: 99%

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Molecular diagnosis of patients affected by mucopolysaccharidosis: a multicenter study

et al. 2019

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Mucopolysaccharidoses (MPS) are a subgroup of 11 monogenic lysosomal storage disorders due to the deficit of activity of the lysosomal hydrolases deputed to the degradation of mucopolysaccharides. Although individually rare, all together they account for at least 1:25,000 live births. In this study, we present the genetic analysis of a population of 71 MPS patients enrolled in a multicenter Italian study. We re-annotated all variants, according to the latest recommendations, and re-classified them as suggested by the American College of Medical Genetics and Genomics. Variant distribution per type was mainly represented by missense mutations. Overall, 10 patients had received no molecular diagnosis, although 6 of them had undergone either HSCT or ERT, based on clinical and enzymatic evaluations. Moreover, nine novel variants are reported. Conclusions : Our analysis underlines the need to complete the molecular diagnosis in patients previously diagnosed only on a biochemical basis, suggests a periodical re-annotation of the variants and solicits their deposition in public databases freely available to clinicians and researchers. We strongly recommend a molecular diagnosis based on the analysis of the “trio” instead of the sole proband. These recommendations will help to obtain a complete and correct diagnosis of mucopolysaccharidosis, rendering also possible genetic counseling. What is known • MPS are a group of 11 metabolic genetic disorders due to deficits of enzymes involved in the mucopolysaccharides degradation. • Molecular analysis is commonly performed to confirm enzymatic assays. What is new • Eighty-six percent of the 71 patients we collected received a molecular diagnosis; among them, 9 novel variants were reported. • We stress the importance of molecular diagnosis in biochemically diagnosed patients, encourage a periodical re-annotation of variants according to the recent nomenclature and their publication in open databases. Electronic supplementary material The online version of this article (10.1007/s00431-019-03341-8) contains supplementary material, which is available to authorized users.

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“…(Gly290Ser)–[59]Likely pathogenicc.1043C>Ap. (Thr348Asn)–[14]Likely pathogenicc.1156C>Tp. (Arg386Cys)rs118204437; ClinVar ID:700[43]Likely pathogenicc.1219A>Cp.…”

Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

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Molecular diagnosis of patients affected by mucopolysaccharidosis: a multicenter study

et al. 2019

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“…Birth prevalence of MPS IVA ranges from 1 per 71 000 to 1 per 500 000 according to reports from several countries including Australia, Brazil, Canada, Germany, Japan, Netherlands, Saudi Arabia, Taiwan, United Arab Emirates and UK 3. A German study estimated the incidence of MPS IVA at 1 per 270 0004 whereas, in Italy, the incidence has been estimated at 1 per 300 000 live births 5…”

Section: Introductionmentioning

confidence: 99%

Mucopolysaccharidosis type IVA (Morquio A): a close differential diagnosis of spondylo-epiphyseal dysplasia

et al. 2017

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Patients with mucopolysaccharidoses (MPS) have a plethora of multisystemic manifestations depending on the particular type, and atypical presentations are not uncommon. MPS type IVA (Morquio A syndrome) has predominant musculoskeletal system involvement and corneal clouding with normal intelligence and can be misdiagnosed as primary skeletal disorders in clinical practice. The absence of corneal clouding with normal urinary glycosaminoglycans (GAGs) level in a proportion of patients with MPS IVA makes the correct diagnosis even more challenging for physicians. Healthcare providers across specialties should have a high degree of suspicion for MPS IVA in all patients with suspected spondylo-epiphyseal dysplasia as early diagnosis and early treatment significantly improve the clinical outcome and activity of daily living.

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“…São características típicas o encurtamento dos ossos longos com alargamento metafisário, a hipoplasia de tórax e ilíaco, o avanço de idade óssea nos ossos do carpo e tarso, e os núcleos de ossificação adicional nas mãos com falange em delta (Huber et al, 2009 processo odontóide e alterações da epífise femural proximal. Na forma clássica, o início dos sintomas ocorre antes dos 3 anos e a estatura final encontra-se abaixo dos 120 cm, com redução da taxa de crescimento aos 18 meses de vida (Caciotti et al, 2015). Existem mais de 275 mutações diferentes relacionadas com a MPS-IVA, sendo portanto, uma explicão plausível para a variabilidade fenotípica da doença.…”

Section: Displasia Campomélica E Doenças Relacionadas (Grupo 18)unclassified

Estudo genético-clínico das displasias esqueléticas, com enfoque nas osteocondrodisplasias com acometimento do esqueleto axial, associado ao envolvimento epifisário e/ou metafisário

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Optimizing the Molecular Diagnosis of GALNS: Novel Methods to Define and Characterize Morquio-A Syndrome-Associated Mutations

Cited by 28 publications

References 60 publications

Molecular diagnosis of patients affected by mucopolysaccharidosis: a multicenter study

Molecular diagnosis of patients affected by mucopolysaccharidosis: a multicenter study

Mucopolysaccharidosis type IVA (Morquio A): a close differential diagnosis of spondylo-epiphyseal dysplasia

Estudo genético-clínico das displasias esqueléticas, com enfoque nas osteocondrodisplasias com acometimento do esqueleto axial, associado ao envolvimento epifisário e/ou metafisário

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