ABSTRACT
Objective:To explore the treatment of the patients with severe phenotype of mucopolysaccharidosis (MPS) type ⅣA by analysing the clinical feature and diagnosis.Methods:Two pediatric patients diagnosed as MPS ⅣA in severe form were enrolled in Children′s Hospital Affiliated to Zhengzhou University from August 2021 to April 2022.Two children from 2 pedigrees with the main manifestations of short stature and bone deformities were retrospectively included.The clinical manifestations, biochemical indexes, and bone imaging findings were retrospectively analyzed.Peripheral blood leukocytes were collected and subjected to the N-acetylgalactosamine-6-sulfatase (GALNS) assay and genetic sequencing.Gene analysis of amniotic fluid cells at the 18 th week of the second pregnancy of the mother of case 2 was performed for prenatal diagnosis.Allogeneic hematopoietic stem cell transplantation (allo-HSCT) was performed in both patients and to explore the treatment of patients with MPS ⅣA. Results:Both cases presented clinical manifestations of short stature, joint laxity, pectus carinatum, and genu valgus.X-ray examination revealed the decreased bone mineral density, ulnar deviation of the radial epiphysis, kyphosis and scoliosis.The respiratory and skeletal systems were affected in both patients, and the optic nerve was suspiciously affected. GALNS gene analysis showed that there were 2 missense mutations of c. 1019G>A (p.G340D) and c. 706C>G (p.H236D) in case 1, and 2 missense mutations of c. 425A>G (p.H142R) and c. 463G>A (p.G155R) were detected in case 2.Mutations in both cases were inherited from their fathers and mothers, which were all newly discovered that have not been reported.Only the c. 463G>A mutation was detected in the amniotic fluid cells of the mother of case 2.It is confirmed that case 2 was the carrier of MPS ⅣA, whose gene mutation was from the mother, and case 2 did not suffer the same disease as the proband.Both cases were treated with allo-HSCT with full donor chimerism and no severe transplant complications were reported.Their GALNS activity was within the normal range, and the scores of activities of daily living were higher than those before transplantation. Conclusions:The MPS ⅣA patients with severe phenotype is a rare autosomal recessive disease caused by GALNS mutations that is difficult to diagnose and poor prognosis.Early detection, diagnosis, and effective treatment contribute to improve the long-term quality of life.The allo-HSCT is an effective therapeutic strategy for MPS ⅣA.
ABSTRACT
PURPOSE: Mucopolysaccharidosis IVA (MPS IVA; Morquio A syndrome) is rare lysosomal storage disorder caused by N-acetylgalactosamine-6-sulfatase (GALNS) deficiency. Only a few MPS IVA cases have been reported in the Korean literature; there is a paucity of research about clinical or radiologic findings for this disorder. Therefore, we studied clinical findings, radiological features, and genetic data of Korean MPS IVA patients for determining factors that may allow early diagnosis and that may thus improve the patients' quality of life. METHODS: MPS IVA was confirmed via assay for enzymatic activity of leukocytes in 10 patients. The GALNS gene was analyzed. Patients' charts were retrospectively reviewed for obtaining clinical features and evaluated for radiological skeletal surveys, echocardiography, pulmonary function test, and ophthalmologic test results. RESULTS: Nine patients had severe clinical phenotype, and 1 had an intermediate phenotype, on the basis of clinical phenotype criteria. Radiologic findings indicated skeletal abnormalities in all patients, especially in the hips and extremities. Eight patients had an odontoid hypoplasia, and 1 showed mild atlantoaxial subluxation and cord myelopathy. Genetic analysis indicated 10 different GALNS mutations. Two mutations, c.451C>A and c.1000C>T, account for 37.5% (6/16) and 25% (4/16) of all mutations in this samples, respectively. CONCLUSION: An understanding of the clinical and radiological features involved in MPS IVA may allow early diagnosis of MPS IVA. Adequate evaluations and therapy in the early stages may improve the quality of life of patients suffering from skeletal abnormalities and may reduce life-threatening effects of atlantoaxial subluxation.
Subject(s)
Humans , Early Diagnosis , Echocardiography , Extremities , Hip , Leukocytes , Mucopolysaccharidoses , Mucopolysaccharidosis IV , Phenotype , Quality of Life , Respiratory Function Tests , Retrospective Studies , Spinal Cord Diseases , Stress, PsychologicalABSTRACT
En el desarrollo de una estrategia de terapia génica para la mucopolisacaridosis IV A (enfermedad de Morquio A), en el presente trabajo se evaluó la capacidad de un vector adenoasociado (AAV) para expresar el gen de la enzima sulfatasa N-acetilgalactosamina-6-sulfato (GALNS, N-acetylgalactosamine-6-sulfate sulfatase) en células HEK293, fibroblastos humanos con mucopolisacaridosis IV A y condrocitos de ratón con mucopolisacaridosis IV A. En el lisado celular, la actividad de la GALNS se incrementó entre 5 y 24 veces los valores observados en las células sin transfectar. La coexpresión con el gen del factor activador de sulfatasas 1 (SUMF1, sultatase modifiying factor 1) permitió un incremento en la actividad de la GALNS en el lisado celular de hasta 4,5 veces los valores observados en las células cotransfectadas con AAV-GALNS. La actividad de la GALNS en el medio de cultivo sólo se detectó en células cotransfectadas con AAV-SUMF1. Estos resultados constituyen evidencia valiosa sobre la posibilidad de realizar la corrección del defecto genético en la mucopolisacaridosis IV A empleando vectores AAV...
Toward the development of a gene therapy strategy for the mucopolysaccharidosis IV A (MPS IV A, Morquio A), in this work we evaluated the capability of an AAV vector to express the N-acetilgalactosamine-6-sulfate sulfatase (GALNS) gene in HEK293 cells, human mucopolysaccharidosis IV A fibroblasts and murine MPS IV A chondrocites. GALNS activity in lysated cells was increased between 5 and 24 folds compared to nontransfected cells. Also, the effect of coexpression with the sultatase modifiying factor 1 (SUMF1) was evaluated.GALNS activity was increased up to 4.5 folds in lysated cells compared to those values observed in AAV-GALNS transduced cells. Noteworthy, enzyme activity was only detected in culture media when cells were cotransfected with AAV-GALNS and AAV-SUMF1. These results represent a valuable step in the development of a gene therapy strategy for mucopolysaccharidosis IV A using AAV vectors...
Subject(s)
Dependovirus , Mucopolysaccharidosis IV , Genetic TherapyABSTRACT
Morquio A Syndrome (mucopolysaccharidosis IVA - MPS IVA, OMIM# 253000) is an autosomal recessive inborn error of metabolism caused by the deficiency of N-acetylgalactosamine-6-sulfate sulfatase (GALNS). We investigated five unrelated Brazilian MPS IVA families for mutations in exons 4, 5, 9 and 10 of the GALNS gene. Six out of the 10 mutant alleles were identified. Taken together with a previous study, which included six unrelated families, common mutations among Brazilian patients were p.N164T, p.G116S and p.G301C. Among one hundred control subjects three novel silent mutations were found (p.A107A; GCC -> GCT, p.Y108Y; TAC -> TAT, p.P357P; CCG -> CCA). Screening starting with exons 4, 5, 9, 10 and 11 may be a good strategy for genotyping of Brazilian patients since these exons include 73 percent of all mutations identified in the current and previous studies.