<i>LAMP2</i> exon‐copy number variations in Danon disease heterozygote female probands: Infrequent or underdetected?

Majer, Filip; Piherová, Lenka; Řeboun, Martin; Stara, Veronika; Pelák, Ondřej; Norambuena, Patricia; Stránecký, Viktor; Krebsová, Alice; Vlášková, Hana; Dvořáková, Lenka; Kmoch, Stanislav; Kalina, Tomáš; Kubánek, Miloš; Sikora, Jakub

doi:10.1002/ajmg.a.40430

Cited by 9 publications

(21 citation statements)

References 20 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…The majority were null (nonsense, frame‐shifting deletions/insertions) or splicing mutations. Missense mutations (only nine reported) and large rearrangements involving one or more exons were rare. A synonymous substitution (c.864G> A) caused exon 6 skipping, indicating that apparently silent variations may be damaging when localized close to the splice sites .…”

Section: Lamp2 Gene Mutation Analysis and Genotype‐phenotype Correlatmentioning

confidence: 99%

Review: Danon disease: Review of natural history and recent advances

Cenacchi

Papa

Pegoraro

et al. 2019

Neuropathology Appl Neurobio

View full text Add to dashboard Cite

Danon disease is a severe multisystem disorder clinically characterized by hypertrophic cardiomyopathy, skeletal myopathy and mental retardation in male patients, and by a milder phenotype (predominantly involving cardiac muscle) in female patients. The disease is inherited as an X‐linked dominant trait. The primary deficiency of lysosome‐associated membrane protein‐2 (LAMP‐2) causes disruption of autophagy, leading to an impaired fusion of lysosomes to autophagosomes and biogenesis of lysosomes. We surveyed over 500 Danon disease patients reported in the literature from the first description to the present, in order to summarize the clinical, pathological and molecular data and treatment perspectives. An early molecular diagnosis is of crucial importance for genetic counselling and for therapeutic interventions: in male patients, the prognosis is poor due to rapid progression towards heart failure, and only heart transplantation modifies the disease course.

show abstract

Section: Lamp2 Gene Mutation Analysis and Genotype‐phenotype Correlatmentioning

confidence: 99%

Review: Danon disease: Review of natural history and recent advances

Cenacchi

Papa

Pegoraro

et al. 2019

Neuropathology Appl Neurobio

View full text Add to dashboard Cite

show abstract

“…Importantly, characterization of the LAMP2 mutations in DD patients #3 and #4 mandated an individualized methodological approach that was far beyond the standard WES analytics in both patients. 13,14 WES testing was negative or inconclusive in 21 patients (47%). Table 2 summarizes the molecular genetic analyses, WBC XCI, and myocardial LAMP2 IHC findings in the female DD patients.…”

Section: Lamp2 Flow Cytometry In White Blood Cellsmentioning

confidence: 99%

“…10 Patients #2 and #3 carried heterozygous deletion exon copy number variants encompassing LAMP2 exons 4-9C and 4-8, respectively. 13 Patient #4 had an Xq24 re-arrangement that caused a heterozygous deletion of several C-terminal exons of CUL4B and the complete deletion of LAMP2, ATP1B4, TMEM255A, and ZBTB33 genes. 14 Patient #5 was heterozygous for a novel frameshift c.445_449delGACCT mutation in the LAMP2 exon 4 (Supporting Information, Figure S1A).…”

Section: Lamp2 Flow Cytometry In White Blood Cellsmentioning

confidence: 99%

“…XCI triggers mosaic expression of the wild-type and mutant LAMP2 alleles in tissues of female DD patients ( Figure 1B, C). 10,[12][13][14] Setting thresholds for skewing or extreme skewing of XCI is arbitrary. Importantly,~98% of females have WBC XCI ratios within the >5:95/<95:5 range.…”

Section: Danon Disease Screening Studiesmentioning

confidence: 99%

“…copy number variants) can be easily missed. 13 Contrary to these high-throughput genomic analytical techniques, the outlined FC method is a selective protein-level expression test. Unlike to analyses of WBCs homogenates by western blotting, 8 the fraction of LAMP2def cells is directly quantified by the FC method.…”

Section: Laboratory Diagnostic Implicationsmentioning

confidence: 99%

See 2 more Smart Citations

Danon disease is an underdiagnosed cause of advanced heart failure in young female patients: a LAMP2 flow cytometric study

et al. 2020

Self Cite

View full text Add to dashboard Cite

Aims Danon disease (DD) is a rare X-linked disorder caused by mutations in the lysosomal-associated membrane protein type 2 gene (LAMP2). DD is difficult to distinguish from other causes of dilated or hypertrophic cardiomyopathy (HCM) in female patients. As DD female patients regularly progress into advanced heart failure (AHF) aged 20-40 years, their early identification is critical to improve patient survival and facilitate genetic counselling. In this study, we evaluated the prevalence of DD among female patients with non-ischemic cardiomyopathy, who reached AHF and were younger than 40 years. Methods and results The study cohort comprised 60 female patients: 47 (78%) heart transplant recipients, 2 (3%) patients treated with ventricular assist device, and 11 (18%) patients undergoing pre-transplant assessment. Aetiology of the cardiomyopathy was known in 15 patients (including two DD patients). LAMP2 expression in peripheral white blood cells (WBC) was tested by flow cytometry (FC) in the remaining 45 female patients. Whole exome sequencing was used as an alternative independent testing method to FC. Five additional female DD patients (two with different novel LAMP2 mutations) were identified by FC. The total prevalence of DD in this cohort was 12%. HCM phenotype (57% vs. 9%, * P = 0.022) and delta waves identified by electrocardiography (43% vs. 0%, ** P = 0.002) were significantly more frequent in DD female patients. Conclusions Danon disease is an underdiagnosed cause of AHF in young female patients. LAMP2 expression testing in peripheral WBCs by FC can be used as an effective screening/diagnostic tool to identify DD in this patient population.

show abstract

Alu‐mediated Xq24 deletion encompassing CUL4B, LAMP2, ATP1B4, TMEM255A, and ZBTB33 genes causes Danon disease in a female patient

Majer

Kousal

Dušek

et al. 2019

American J of Med Genetics Pt A

Self Cite

View full text Add to dashboard Cite

Cullin 4B (CUL4B), lysosomal-associated membrane protein Type 2 (LAMP2), ATP1B4, TMEM255A, and ZBTB33 are neighboring genes on Xq24. Mutations in CUL4B result in Cabezas syndrome (CS). Male CS patients present with dysmorphic, neuropsychiatric, genitourinary, and endocrine abnormalities. Heterozygous CS females are clinically asymptomatic. LAMP2 mutations cause Danon disease (DD). Cardiomyopathy is a dominant feature of DD present in both males and heterozygous females. No monogenic phenotypes have been associated with mutations in ATP1B4, TMEM255A, and ZBTB33 genes. To facilitate diagnostics and counseling in CS and DD families, we present a female DD patient with a de novo Alu-mediated Xq24 rearrangement causing a deletion encompassing CUL4B, LAMP2, and also the other three neighboring genes. Typical to females heterozygous for CUL4B mutations, the patient was CS asymptomatic, however, presented with extremely skewed X-chromosome inactivation (XCI) ratios in peripheral white blood cells. As a result of the likely selection against CUL4B deficient clones, only minimal populations (~3%) of LAMP2 deficient leukocytes were identified by flow cytometry. On the contrary, myocardial LAMP2 protein expression suggested random XCI. We demonstrate that contiguous CUL4B and LAMP2 loss-of-function

show abstract

LAMP2 exon‐copy number variations in Danon disease heterozygote female probands: Infrequent or underdetected?

Cited by 9 publications

References 20 publications

Review: Danon disease: Review of natural history and recent advances

Review: Danon disease: Review of natural history and recent advances

Danon disease is an underdiagnosed cause of advanced heart failure in young female patients: a LAMP2 flow cytometric study

Alu‐mediated Xq24 deletion encompassing CUL4B, LAMP2, ATP1B4, TMEM255A, and ZBTB33 genes causes Danon disease in a female patient

Contact Info

Product

Resources

About