The genotype–phenotype correlation in Pompe disease

Kroos, Marian A.; Hoogeveen‐Westerveld, Marianne; Ploeg, Ans van der; Reuser, Arnold

doi:10.1002/ajmg.c.31318

Cited by 110 publications

(125 citation statements)

References 79 publications

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“…Early onset infantile PD results from a complete deficiency of the enzyme (activity < 1%), while late onset PD (juvenile or adult) results from partial deficiency of GAA (1-30%). Onset may occur as early in childhood or as late as at the sixth decade of life 6,7 (B). The cause of PD is the progressive accumulation of intralysosomal glycogen due to the inability of the cell to breakdown the lysosomal glycogen into glucose.…”

Section: Pathophysiologymentioning

confidence: 99%

“…Mutations can be similar (homozygote); or, different (compound heterozygote); however, both within the GAA gene. The most common mutation observed in PDJ-A patients, including Brazilians, is the intronic alteration c.-32-13 T > G (IVS1-13T > G), which is observed in more than two-thirds of the patients worldwide 7,30 . The type and combination of these mutations will determine the amount of residual GAA activity in the cells 6,7 .…”

Section: Genetic Aspects Of Juvenile and Adult Pompe Disease Patientsmentioning

confidence: 99%

“…The most common mutation observed in PDJ-A patients, including Brazilians, is the intronic alteration c.-32-13 T > G (IVS1-13T > G), which is observed in more than two-thirds of the patients worldwide 7,30 . The type and combination of these mutations will determine the amount of residual GAA activity in the cells 6,7 . The combination of two severe mutations leads to a complete lack of GAA protein and, as a consequence, an extremely low residual GAA activity (< 1%); such genotype is associated with the severe early onset PD On the other hand, any other combination of mutations, being at least one of then considered a "milder" mutation, such as the classic c. -32-13 T > G, enzyme production will occur, even if abnormally, resulting in different levels of residual GAA activity of up to 30% of the normal value 6,7 .…”

Section: Genetic Aspects Of Juvenile and Adult Pompe Disease Patientsmentioning

confidence: 99%

“…The type and combination of these mutations will determine the amount of residual GAA activity in the cells 6,7 . The combination of two severe mutations leads to a complete lack of GAA protein and, as a consequence, an extremely low residual GAA activity (< 1%); such genotype is associated with the severe early onset PD On the other hand, any other combination of mutations, being at least one of then considered a "milder" mutation, such as the classic c. -32-13 T > G, enzyme production will occur, even if abnormally, resulting in different levels of residual GAA activity of up to 30% of the normal value 6,7 . Patients with at least one mild mutation constitute most cases of juvenile and late-onset PD and present a clinical phenotype with a slower progression 1,7 .…”

Section: Genetic Aspects Of Juvenile and Adult Pompe Disease Patientsmentioning

confidence: 99%

“…family history and genetic counseling PD is an autosomal recessive disease caused by pathogenic mutations in both alleles of the GAA gene 1,7 . Parents of individuals with PD are healthy obligatory heterozygotes with a risk of PD recurrence in their future offspring of approximately 25%.…”

Section: Anesthesia/surgerymentioning

confidence: 99%

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Guidelines for the diagnosis, treatment and clinical monitoring of patients with juvenile and adult Pompe disease

Llerena

Nascimento

Oliveira

et al. 2015

Arq. Neuro-Psiquiatr.

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Pompe disease (PD) is a potentially lethal illness involving irreversible muscle damage resulting from glycogen storage in muscle fiber and activation of autophagic pathways. A promising therapeutic perspective for PD is enzyme replacement therapy (ERT) with the human recombinant enzyme acid alpha-glucosidase (Myozyme®). The need to organize a diagnostic flowchart, systematize clinical follow-up, and establish new therapeutic recommendations has become vital, as ERT ensures greater patient longevity. A task force of experienced clinicians outlined a protocol for diagnosis, monitoring, treatment, genetic counseling, and rehabilitation for PD patients. The study was conducted under the coordination of REBREPOM, the Brazilian Network for Studies of PD. The meeting of these experts took place in October 2013, at L’Hotel Port Bay in São Paulo, Brazil. In August 2014, the text was reassessed and updated. Given the rarity of PD and limited high-impact publications, experts submitted their views.

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Section: Pathophysiologymentioning

confidence: 99%

Section: Genetic Aspects Of Juvenile and Adult Pompe Disease Patientsmentioning

confidence: 99%

Section: Genetic Aspects Of Juvenile and Adult Pompe Disease Patientsmentioning

confidence: 99%

Section: Genetic Aspects Of Juvenile and Adult Pompe Disease Patientsmentioning

confidence: 99%

Section: Anesthesia/surgerymentioning

confidence: 99%

See 3 more Smart Citations

Guidelines for the diagnosis, treatment and clinical monitoring of patients with juvenile and adult Pompe disease

Llerena

Nascimento

Oliveira

et al. 2015

Arq. Neuro-Psiquiatr.

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Disorders of Muscle Glycogen Metabolism

Vissing

2013

Muscle Disease

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Transcription factor EB (TFEB) is a new therapeutic target for Pompe disease

et al. 2013

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A recently proposed therapeutic approach for lysosomal storage disorders (LSDs) relies upon the ability of transcription factor EB (TFEB) to stimulate autophagy and induce lysosomal exocytosis leading to cellular clearance. This approach is particularly attractive in glycogen storage disease type II [a severe metabolic myopathy, Pompe disease (PD)] as the currently available therapy, replacement of the missing enzyme acid alpha-glucosidase, fails to reverse skeletal muscle pathology. PD, a paradigm for LSDs, is characterized by both lysosomal abnormality and dysfunctional autophagy. Here, we show that TFEB is a viable therapeutic target in PD: overexpression of TFEB in a new muscle cell culture system and in mouse models of the disease reduced glycogen load and lysosomal size, improved autophagosome processing, and alleviated excessive accumulation of autophagic vacuoles. Unexpectedly, the exocytosed vesicles were labelled with lysosomal and autophagosomal membrane markers, suggesting that TFEB induces exocytosis of autophagolysosomes. Furthermore, the effects of TFEB were almost abrogated in the setting of genetically suppressed autophagy, supporting the role of autophagy in TFEB-mediated cellular clearance.

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The genotype–phenotype correlation in Pompe disease

Cited by 110 publications

References 79 publications

Guidelines for the diagnosis, treatment and clinical monitoring of patients with juvenile and adult Pompe disease

Guidelines for the diagnosis, treatment and clinical monitoring of patients with juvenile and adult Pompe disease

Disorders of Muscle Glycogen Metabolism

Transcription factor EB (TFEB) is a new therapeutic target for Pompe disease

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