Sequencing of a Patient with Balanced Chromosome Abnormalities and Neurodevelopmental Disease Identifies Disruption of Multiple High Risk Loci by Structural Variation

Blake, Jonathon; Riddell, Andrew; Theiß, Susanne; Perez‐Gonzalez, Alexis; Haase, Bettina; Jauch, Anna; Janssen, Johannes W.G.; Ibberson, David; Pavlinić, Dinko; Moog, Ute; Beneš, Vladimír; Runz, Heiko

doi:10.1371/journal.pone.0090894

Cited by 21 publications

(14 citation statements)

References 33 publications

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“…Investigations of structural variants in other cancer projects have used three or more paired-end reads or mapping qualities (MAPQ) greater than 35 [41, 42]. We expanded the sensitivity of our filtering to identify structural variants with two paired-end reads, with a MAPQ greater than 20.…”

Section: Discussionmentioning

confidence: 99%

The genomic landscape of fibrolamellar hepatocellular carcinoma: whole genome sequencing of ten patients

et al. 2015

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Fibrolamellar hepatocellular carcinoma is a rare, malignant liver tumor that often arises in the otherwise normal liver of adolescents and young adults. Previous studies have focused on biomarkers and comparisons to traditional hepatocellular carcinoma, and have yielded little data on the underlying pathophysiology. We performed whole genome sequencing on paired tumor and normal samples from 10 patients to identify recurrent mutations and structural variations that could predispose to oncogenesis. There are relatively few coding, somatic mutations in this cancer, putting it on the low end of the mutational spectrum. Aside from a previously described heterozygous deletion on chromosome 19 that encodes for a functional, chimeric protein, there were no other recurrent structural variations that contribute to the tumor genotype. The lack of a second-hit mutation in the genomic landscape of fibrolamellar hepatocellular carcinoma makes the DNAJB1-PRKACA fusion protein the best target for diagnostic and therapeutic advancements. The mutations, altered pathways and structural variants that characterized fibrolamellar hepatocellular carcinoma were distinct from those in hepatocellular carcinoma, further defining it as a distinct carcinoma.

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Section: Discussionmentioning

confidence: 99%

The genomic landscape of fibrolamellar hepatocellular carcinoma: whole genome sequencing of ten patients

et al. 2015

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“…These inversions appear de novo in patients or are inherited mutations restricted to a given family, and thus they do not represent polymorphic variants segregating in human populations. Nevertheless, they have clinical importance and can contribute to the identification of genes underlying certain rare disorders [ 61 , 62 ]. In this sense, it is possible that the contribution of structural variants to disease is currently underestimated owing to the frequent use of exome sequencing to identify the causal genes, a strategy that fails to detect genes truncated by a breakpoint.…”

Section: Inversions As Simple Mutations Causing Diseasementioning

confidence: 99%

Human inversions and their functional consequences

Puig¹,

Casillas²,

Villatoro³

et al. 2015

Briefings in Functional Genomics

114

112

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Polymorphic inversions are a type of structural variants that are difficult to analyze owing to their balanced nature and the location of breakpoints within complex repeated regions. So far, only a handful of inversions have been studied in detail in humans and current knowledge about their possible functional effects is still limited. However, inversions have been related to phenotypic changes and adaptation in multiple species. In this review, we summarize the evidences of the functional impact of inversions in the human genome. First, given that inversions have been shown to inhibit recombination in heterokaryotes, chromosomes displaying different orientation are expected to evolve independently and this may lead to distinct gene-expression patterns. Second, inversions have a role as disease-causing mutations both by directly affecting gene structure or regulation in different ways, and by predisposing to other secondary arrangements in the offspring of inversion carriers. Finally, several inversions show signals of being selected during human evolution. These findings illustrate the potential of inversions to have phenotypic consequences also in humans and emphasize the importance of their inclusion in genome-wide association studies.

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“…60 In a subject with a balanced complex chromosomal aberration (reciprocal translocation and paracentric inversion), PSMD14 was considered a strong neurodevelopmental candidate gene. 61 As mentioned above, PSMD12 would need to directly interact with PSMD14 to acquire its active enzymatic conformation. 47,62 The second gene, PSMA7, encodes an alpha subunit of the 20S core complex.…”

Section: Congenital Malformationsmentioning

confidence: 99%

De Novo Disruption of the Proteasome Regulatory Subunit PSMD12 Causes a Syndromic Neurodevelopmental Disorder

Küry¹,

Besnard²,

Ebstein³

et al. 2017

The American Journal of Human Genetics

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Degradation of proteins by the ubiquitin-proteasome system (UPS) is an essential biological process in the development of eukaryotic organisms. Dysregulation of this mechanism leads to numerous human neurodegenerative or neurodevelopmental disorders. Through a multi-center collaboration, we identified six de novo genomic deletions and four de novo point mutations involving PSMD12, encoding the non-ATPase subunit PSMD12 (aka RPN5) of the 19S regulator of 26S proteasome complex, in unrelated individuals with intellectual disability, congenital malformations, ophthalmologic anomalies, feeding difficulties, deafness, and subtle dysmorphic facial features. We observed reduced PSMD12 levels and an accumulation of ubiquitinated proteins without any impairment of proteasome catalytic activity. Our PSMD12 loss-of-function zebrafish CRISPR/Cas9 model exhibited microcephaly, decreased convolution of the renal tubules, and abnormal craniofacial morphology. Our data support the biological importance of PSMD12 as a scaffolding subunit in proteasome function during development and neurogenesis in particular; they enable the definition of a neurodevelopmental disorder due to PSMD12 variants, expanding the phenotypic spectrum of UPS-dependent disorders.Proteolysis by the ubiquitin-proteasome system (UPS) is a tightly regulated biological process in eukaryotic cells and is crucial for their homeostasis, signaling, and fate determination. 1-3 Proteins subjected to degradation are typically marked by polyubiquitin chains to be hydrolyzed in a precise, rapid, timely, and ATP-dependent manner by the 19S regulatory subunit of the 26S proteasome. 3-6 UPS-dependent degradation essentially contributes to proteostasis and plays a key role in neuronal development and function 7,8 by regulating synaptic plasticity, 9,10

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Sequencing of a Patient with Balanced Chromosome Abnormalities and Neurodevelopmental Disease Identifies Disruption of Multiple High Risk Loci by Structural Variation

Cited by 21 publications

References 33 publications

The genomic landscape of fibrolamellar hepatocellular carcinoma: whole genome sequencing of ten patients

The genomic landscape of fibrolamellar hepatocellular carcinoma: whole genome sequencing of ten patients

Human inversions and their functional consequences

De Novo Disruption of the Proteasome Regulatory Subunit PSMD12 Causes a Syndromic Neurodevelopmental Disorder

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