Copy number variations in a population with prune belly syndrome

Iqbal, Nida S.; Jascur, Thomas; Harrison, Steven M.; Chen, Catherine; Arevalo, Michelle K.; Wong, Daniel; Sanchez, Emily; Grimsby, Gwen M.; Wilson, Kathleen; Baker, Linda A.

doi:10.1002/ajmg.a.40476

Cited by 8 publications

(6 citation statements)

References 31 publications

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“…Lastly, there have been 12 published multiplex pedigrees without causal genes identified in most [19][20][21][23][24][25][26][27][28][29][30][31]. More recently, five autosomal genes, including CHRM3, HNF1β, ACTA2, ACTG2 and STIM1, have been reported with potentially causal DNA variants, including structural, copy number, and single nucleotide variants, however these genes each only account for one or two PBS cases or one PBS multiplex consanguineous kindred [32][33][34][35][36][37][38]. Moreover, none of the currently suggested candidate genes fit an X-linked recessive mode of inheritance and functional data is lacking for many of these candidate genetic variants.…”

Section: Introductionmentioning

confidence: 99%

Prune belly syndrome in surviving males can be caused by Hemizygous missense mutations in the X-linked Filamin A gene

et al. 2020

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Background: Prune belly syndrome (PBS) is a rare, multi-system congenital myopathy primarily affecting males that is poorly described genetically. Phenotypically, its morbidity spans from mild to lethal, however, all isolated PBS cases manifest three cardinal pathological features: 1) wrinkled flaccid ventral abdominal wall with skeletal muscle deficiency, 2) urinary tract dilation with poorly contractile smooth muscle, and 3) intra-abdominal undescended testes. Despite evidence for a genetic basis, previously reported PBS autosomal candidate genes only account for one consanguineous family and single cases. Methods: We performed whole exome sequencing (WES) of two maternal adult half-brothers with syndromic PBS (PBS + Otopalatodigital spectrum disorder [OPDSD]) and two unrelated sporadic individuals with isolated PBS and further functionally validated the identified mutations. Results: We identified three unreported hemizygous missense point mutations in the X-chromosome gene Filamin ) in two related cases and two unrelated sporadic individuals. Two of the three PBS mutations map to the highly regulatory, stretch-sensing Ig19-21 region of FLNA and enhance binding to intracellular tails of the transmembrane receptor β-integrin 1 (ITGβ1). Conclusions: FLNA is a regulatory actin-crosslinking protein that functions in smooth muscle cells as a mechanosensing molecular scaffold, transmitting force signals from the actin-myosin motor units and cytoskeleton via binding partners to the extracellular matrix. This is the first evidence for an X-linked cause of PBS in multiple unrelated individuals and expands the phenotypic spectrum associated with FLNA in males surviving even into adulthood.

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Section: Introductionmentioning

confidence: 99%

Prune belly syndrome in surviving males can be caused by Hemizygous missense mutations in the X-linked Filamin A gene

et al. 2020

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“…At this point, most cases of PBS remain genetically undefined. In the last ten years, seven autosomal genes (MYOCD, CHRM3, HNF1β, ACTA2, ACTG2, STIM1 and MYH11) and one X-linked gene (FLNA) have been reported with potentially causal rare DNA variants, including structural variants, copy number variants, and single nucleotide variants 44 – 54 . Interestingly, FLNA, MYH11, ACTA2, and ACTG2 genes are involved in mechanosensation of the cell 55 – 58 .…”

Section: Discussionmentioning

confidence: 99%

PIEZO1 loss-of-function compound heterozygous mutations in the rare congenital human disorder Prune Belly Syndrome

Amado,

Nosyreva,

Thompson

et al. 2024

Nat Commun

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Prune belly syndrome (PBS), also known as Eagle-Barret syndrome, is a rare, multi-system congenital myopathy primarily affecting males. Phenotypically, PBS cases manifest three cardinal pathological features: urinary tract dilation with poorly contractile smooth muscle, wrinkled flaccid ventral abdominal wall with skeletal muscle deficiency, and intra-abdominal undescended testes. Genetically, PBS is poorly understood. After performing whole exome sequencing in PBS patients, we identify one compound heterozygous variant in the PIEZO1 gene. PIEZO1 is a cation-selective channel activated by various mechanical forces and widely expressed throughout the lower urinary tract. Here we conduct an extensive functional analysis of the PIEZO1 PBS variants that reveal loss-of-function characteristics in the pressure-induced normalized open probability (NPo) of the channel, while no change is observed in single-channel currents. Furthermore, Yoda1, a PIEZO1 activator, can rescue the NPo defect of the PBS mutant channels. Thus, PIEZO1 mutations may be causal for PBS and the in vitro cellular pathophysiological phenotype could be rescued by the small molecule, Yoda1. Activation of PIEZO1 might provide a promising means of treating PBS and other related bladder dysfunctional states.

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“…En un estudio de Iqbal y colaboradores se identificaron dos pacientes con desequilibrio en el cromosoma X, y uno con duplicación del gen AGTR2 ubicado en dicho cromosoma, el cual está implicado en el desarrollo del tracto urinario. 8 En otro estudio se identificaron tres mutaciones del gen FLNA, implicado en la producción de la proteína filamina A, la cual regula la reticulación de actina que funciona en las células del músculo liso. 9 Además, se han propuesto teorías que implican alteraciones en diversas proteínas de contractilidad muscular visceral como resultado de mutaciones genéticas, incluyendo los genes ACTA2, ACTG2, MYH11, MYLK, MYOCD y HNF1B.…”

Section: Discussionunclassified

“…Algunas incluyen el origen genético heterogéneo, con la implicación de diversas proteínas de contractilidad muscular visceral o de alteraciones de los receptores muscarínicos colinérgicos M3, 6,7 o bien, que el modo de herencia está ligado al cromosoma X. 8,9 Otra propuesta describe que hay alteración en el desarrollo del mesodermo, lo cual explicaría las alteraciones morfológicas a nivel genitourinario, gastrointestinal y de otros sistemas. 10 El diagnóstico puede realizarse durante la gestación, a través de una ecografía obstétrica con evidencia de contornos irregulares en el abdomen asociado con un aumento de su circunferencia, anomalías del tracto urinario, oligohidramnios, ascitis fetal y uraco permeable.…”

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