Epidemiological, clinical and biochemical characterization of the p.(Ala359Asp) SMPD1 variant causing Niemann–Pick disease type B

Acuña, Mariana; Martínez, Paula; Moraga, Carol; He, Xingxing; Moraga, Mauricio; Hunter, B.; Nüernberg, Peter; Gutiérrez, Rodrigo A.; González, Maurício; Schuchman, Edward H.; Santos, José Luis; Miquel, Juan Francisco; Mabe, Paulina; Zanlungo, Silvana

doi:10.1038/ejhg.2015.89

Cited by 22 publications

(27 citation statements)

References 28 publications

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“…These and other findings have assisted physicians, genetic counselors and families in predicting the phenotypic outcome in individual NPD patients, and in the future may lead to large-scale screening for this disorder in specific populations. For example, one particularly interesting recent study examined a single mutation (A359D) that occurs in >90% of type B patients in Chile [61]. Screening for this mutation among healthy individuals living in Santiago indicated that the carrier frequency for type B NPD within Chile was ~1/106, predicting a disease incidence of ~1/45,000.…”

Section: Molecular Geneticsmentioning

confidence: 99%

Types A and B Niemann-Pick disease

Schuchman

Desnick

2017

Molecular Genetics and Metabolism

201

157

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The eponym Niemann-Pick disease (NPD) refers to a group of patients who present with varying degrees of lipid storage and foam cell infiltration in tissues, as well as overlapping clinical features including hepatosplenomegaly, pulmonary insufficiency and/or central nervous system (CNS) involvement. Due to the pioneering work of Roscoe Brady and co-workers, we now know that there are two distinct metabolic abnormalities that account for NPD. The first is due to the deficient activity of the enzyme acid sphingomyelinase (ASM; “types A & B” NPD), and the second is due to defective function in cholesterol transport (“type C” NPD). Herein only types A and B NPD will be discussed. Type A NPD patients exhibit hepatosplenomegaly in infancy and profound CNS involvement. They rarely survive beyond 2–3 years of age. Type B patients also have hepatosplenomegaly and pathologic alterations of their lungs, but there are usually no CNS signs. The age of onset and rate of disease progression varies greatly among type B patients, and they frequently live into adulthood. Intermediate patients also have been reported with mild to moderate neurological findings. All patients with types A and B NPD have mutations in the gene encoding ASM (SMPD1), and thus the disease is more accurately referred to as ASM deficiency (ASMD). Herein we will review the clinical, pathological, biochemical, and genetic findings in types A and B NPD, and emphasize the seminal contributions of Dr. Brady to this disease. We will also discuss the current status of therapy for this disorder.

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Section: Molecular Geneticsmentioning

confidence: 99%

Types A and B Niemann-Pick disease

Schuchman

Desnick

2017

Molecular Genetics and Metabolism

201

157

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“…Although NPA and NPB are pan-ethnic, NPA is more frequent in individuals with Ashkenazi Jewish ancestry than in the general population, with an estimated carrier frequency close to 1:80 and a disease incidence of 1/40,000 (Schuchman and Desnick, 2014 ). In other populations, such as in Chile, the carrier frequency for the type B mutation A359D occurs in 90% of patients close to a 1:106 rate, predicting a disease incidence of 1/45,000 (Acuña et al, 2016a , b ).…”

Section: Np Diseasesmentioning

confidence: 99%

“…More than 180 pathogenic mutations in the SMPD1 gene in patients with NPA and NPB have been identified, which are concentrated in exon two (Schuchman and Desnick, 2017 ). Recently, the ASMase crystal structure has been determined in humans (Xiong et al, 2016 ) and mouse (Gorelik et al, 2016 ), which may facilitate genotype-phenotype mutation analysis (Acuña et al, 2016b ; Zampieri et al, 2016 ).…”

Section: Np Diseasesmentioning

confidence: 99%

Lysosomal and Mitochondrial Liaisons in Niemann-Pick Disease

et al. 2017

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Lysosomal storage disorders (LSD) are characterized by the accumulation of diverse lipid species in lysosomes. Niemann-Pick type A/B (NPA/B) and type C diseases Niemann-Pick type C (NPC) are progressive LSD caused by loss of function of distinct lysosomal-residing proteins, acid sphingomyelinase and NPC1, respectively. While the primary cause of these diseases differs, both share common biochemical features, including the accumulation of sphingolipids and cholesterol, predominantly in endolysosomes. Besides these alterations in lysosomal homeostasis and function due to accumulation of specific lipid species, the lysosomal functional defects can have far-reaching consequences, disrupting intracellular trafficking of sterols, lipids and calcium through membrane contact sites (MCS) of apposed compartments. Although MCS between endoplasmic reticulum and mitochondria have been well studied and characterized in different contexts, emerging evidence indicates that lysosomes also exhibit close proximity with mitochondria, which translates in their mutual functional regulation. Indeed, as best illustrated in NPC disease, alterations in the lysosomal-mitochondrial liaisons underlie the secondary accumulation of specific lipids, such as cholesterol in mitochondria, resulting in mitochondrial dysfunction and defective antioxidant defense, which contribute to disease progression. Thus, a better understanding of the lysosomal and mitochondrial interactions and trafficking may identify novel targets for the treatment of Niemann-Pick disease.

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“…Particularly, both p.L304P and p.R498L are frequent Ashkenazi Jewish mutations and have been clearly associated to the severe NPA phenotype in this population [Levran et al., , 1992]. However, 12 mutations (p.R230C, p.W246C, p.D253H, p.D253E, p.A283T, p.Q294K, p.L343P, p.A359D, p.M384I, p.H423Y, p.H577R, and p.R602P) cause a severe impairment of ASM activity and were found in homozygosity or in association with another severe mutation in NPB patients [Simonaro et al, , Pittis et al., ; Pavlů‐Pereira et al., ; Desnick et al., , Hollak et al., , Acuna et al., ]. It is worth noting that eight of them (p.R230C, p.D253H, p.D253E, p.Q294K, p.L343P, p.M384I, p.H423Y, and p.H577R) were found in NPB patients with an intermediate clinical phenotype [Simonaro et al, , Pittis et al., ; Pavlů‐Pereira et al., ; Desnick et al., , Hollak et al., ].…”

Section: Genotype–phenotype Correlationmentioning

confidence: 99%

SMPD1 Mutation Update: Database and Comprehensive Analysis of Published and Novel Variants

et al. 2015

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Niemann-Pick Types A and B (NPA/B) diseases are autosomal recessive lysosomal storage disorders caused by the deficient activity of acid sphingomyelinase (ASM) because of the mutations in the SMPD1 gene. Here, we provide a comprehensive updated review of already reported and newly identified SMPD1 variants. Among them, 185 have been found in NPA/B patients. Disease-causing variants are equally distributed along the SMPD1 gene; most of them are missense (65.4%) or frameshift (19%) mutations. The most frequently reported mutation worldwide is the p.R610del, clearly associated with an attenuated NP disease type B phenotype. The available information about the impact of 52 SMPD1 variants on ASM mRNA and/or enzymatic activity has been collected and whenever possible, phenotype/genotype correlations were established. In addition, we created a locus-specific database easily accessible at http://www.inpdr.org/genes that catalogs the 417 SMPD1 variants reported to date and provides data on their in silico predicted effects on ASM protein function or mRNA splicing. The information reviewed in this article, providing new insights into the genotype/phenotype correlation, is extremely valuable to facilitate diagnosis and genetic counseling of families affected by NPA/B.

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Epidemiological, clinical and biochemical characterization of the p.(Ala359Asp) SMPD1 variant causing Niemann–Pick disease type B

Cited by 22 publications

References 28 publications

Types A and B Niemann-Pick disease

Types A and B Niemann-Pick disease

Lysosomal and Mitochondrial Liaisons in Niemann-Pick Disease

SMPD1 Mutation Update: Database and Comprehensive Analysis of Published and Novel Variants

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