Paediatrics (RCH) - Research Publications

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Author: van Bergen, Nicole ×

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    Integrated multi-omics for rapid rare disease diagnosis on a national scale
    Lunke, S ; Bouffler, SEE ; Patel, CVV ; Sandaradura, SAA ; Wilson, M ; Pinner, J ; Hunter, MFF ; Barnett, CPP ; Wallis, M ; Kamien, B ; Tan, TYY ; Freckmann, M-L ; Chong, B ; Phelan, D ; Francis, D ; Kassahn, KSS ; Ha, T ; Gao, S ; Arts, P ; Jackson, MRSR ; Scott, HSS ; Eggers, S ; Rowley, S ; Boggs, K ; Rakonjac, A ; Brett, GRR ; de Silva, MGG ; Springer, A ; Ward, M ; Stallard, K ; Simons, C ; Conway, T ; Halman, A ; Van Bergen, NJJ ; Sikora, T ; Semcesen, LNN ; Stroud, DAA ; Compton, AGG ; Thorburn, DRR ; Bell, KMM ; Sadedin, S ; North, KNN ; Christodoulou, J ; Stark, Z (NATURE PORTFOLIO, 2023-07)
    Critically ill infants and children with rare diseases need equitable access to rapid and accurate diagnosis to direct clinical management. Over 2 years, the Acute Care Genomics program provided whole-genome sequencing to 290 families whose critically ill infants and children were admitted to hospitals throughout Australia with suspected genetic conditions. The average time to result was 2.9 d and diagnostic yield was 47%. We performed additional bioinformatic analyses and transcriptome sequencing in all patients who remained undiagnosed. Long-read sequencing and functional assays, ranging from clinically accredited enzyme analysis to bespoke quantitative proteomics, were deployed in selected cases. This resulted in an additional 19 diagnoses and an overall diagnostic yield of 54%. Diagnostic variants ranged from structural chromosomal abnormalities through to an intronic retrotransposon, disrupting splicing. Critical care management changed in 120 diagnosed patients (77%). This included major impacts, such as informing precision treatments, surgical and transplant decisions and palliation, in 94 patients (60%). Our results provide preliminary evidence of the clinical utility of integrating multi-omic approaches into mainstream diagnostic practice to fully realize the potential of rare disease genomic testing in a timely manner.
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    De novo enhancer deletion of LMX1B produces a mild nail-patella clinical phenotype
    Francis, D ; Lall, P ; Ayres, S ; Van Bergen, NJ ; Christodoulou, J ; Brown, NJ ; Kalitsis, P (WILEY, 2024-02)
    Critical genes involved in embryonic development are often transcription factors, regulating many downstream genes. LMX1B is a homeobox gene that is involved in formation of the limbs, eyes and kidneys, heterozygous loss-of-function sequence variants and deletions cause Nail-Patella syndrome. Most of the reported variants are localised within the gene's coding sequence, however, approximately 5%-10% of affected individuals do not have a pathogenic variant identified within this region. In this study, we present a family with four affected individuals across two generations with a deletion spanning a conserved upstream LMX1B-binding sequence. This deletion is de novo in the mother of three affected children. Furthermore, in this family, the manifestations appear limited to the nails and limbs, and therefore may reflect an attenuated phenotype of the classic Nail-Patella phenotype that includes ophthalmological and renal manifestations.
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    Clinical and biochemical distinctions for a metabolite repair disorder caused by NAXD or NAXE deficiency
    Van Bergen, NJ ; Walvekar, AS ; Patraskaki, M ; Sikora, T ; Linster, CL ; Christodoulou, J (WILEY, 2022-11)
    The central cofactors NAD(P)H are prone to damage by hydration, resulting in formation of redox-inactive derivatives designated NAD(P)HX. The highly conserved enzymes NAD(P)HX dehydratase (NAXD) and NAD(P)HX epimerase (NAXE) function to repair intracellular NAD(P)HX. Recently, pathogenic variants in both the NAXD and NAXE genes were associated with rapid deterioration and death after an otherwise trivial fever, infection, or illness in young patients. As more patients are identified, distinct clinical features are emerging depending on the location of the pathogenic variant. In this review, we carefully catalogued the clinical features of all published NAXD deficiency patients and found distinct patterns in clinical presentations depending on which subcellular compartment is affected by the enzymatic deficiency. Exon 1 of NAXD contains a mitochondrial propeptide, and a unique cytosolic isoform is initiated from an alternative start codon in exon 2. NAXD deficiency patients with variants that affect both the cytosolic and mitochondrial isoforms present with neurological defects, seizures and skin lesions. Interestingly, patients with NAXD variants exclusively affecting the mitochondrial isoform present with myopathy, moderate neuropathy and a cardiac presentation, without the characteristic skin lesions, seizures or neurological degeneration. This suggests that cytosolic NAD(P)HX repair may protect from neurological damage, whereas muscle fibres may be more sensitive to mitochondrial NAD(P)HX damage. A deeper understanding of the clinical phenotype may facilitate rapid identification of new cases and allow earlier therapeutic intervention. Niacin-based therapies are promising, but advances in disease modelling for both NAXD and NAXE deficiency may identify more specific compounds as targeted treatments. In this review, we found distinct patterns in the clinical presentations of NAXD deficiency patients based on the location of the pathogenic variant, which determines the subcellular compartment that is affected by the enzymatic deficiency.
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    CDKL5 deficiency disorder: molecular insights and mechanisms of pathogenicity to fast-track therapeutic development
    Van Bergen, NJ ; Massey, S ; Quigley, A ; Rollo, B ; Harris, AR ; Kapsa, RMI ; Christodoulou, J (PORTLAND PRESS LTD, 2022-08)
    CDKL5 deficiency disorder (CDD) is an X-linked brain disorder of young children and is caused by pathogenic variants in the cyclin-dependent kinase-like 5 (CDKL5) gene. Individuals with CDD suffer infantile onset, drug-resistant seizures, severe neurodevelopmental impairment and profound lifelong disability. The CDKL5 protein is a kinase that regulates key phosphorylation events vital to the development of the complex neuronal network of the brain. Pathogenic variants identified in patients may either result in loss of CDKL5 catalytic activity or are hypomorphic leading to partial loss of function. Whilst the progressive nature of CDD provides an excellent opportunity for disease intervention, we cannot develop effective therapeutics without in-depth knowledge of CDKL5 function in human neurons. In this mini review, we summarize new findings on the function of CDKL5. These include CDKL5 phosphorylation targets and the consequence of disruptions on signaling pathways in the human brain. This new knowledge of CDKL5 biology may be leveraged to advance targeted drug discovery and rapid development of treatments for CDD. Continued development of effective humanized models will further propel our understanding of CDD biology and may permit the development and testing of therapies that will significantly alter CDD disease trajectory in young children.
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    Biallelic Variants in PYROXD2 Cause a Severe Infantile Metabolic Disorder Affecting Mitochondrial Function
    Van Bergen, NJ ; Hock, DH ; Spencer, L ; Massey, S ; Stait, T ; Stark, Z ; Lunke, S ; Roesley, A ; Peters, H ; Lee, JY ; Le Fevre, A ; Heath, O ; Mignone, C ; Yang, JY-M ; Ryan, MM ; D'Arcy, C ; Nash, M ; Smith, S ; Caruana, NJ ; Thorburn, DR ; Stroud, DA ; White, SM ; Christodoulou, J ; Brown, NJ (MDPI, 2022-01)
    Pyridine Nucleotide-Disulfide Oxidoreductase Domain 2 (PYROXD2; previously called YueF) is a mitochondrial inner membrane/matrix-residing protein and is reported to regulate mitochondrial function. The clinical importance of PYROXD2 has been unclear, and little is known of the protein's precise biological function. In the present paper, we report biallelic variants in PYROXD2 identified by genome sequencing in a patient with suspected mitochondrial disease. The child presented with acute neurological deterioration, unresponsive episodes, and extreme metabolic acidosis, and received rapid genomic testing. He died shortly after. Magnetic resonance imaging (MRI) brain imaging showed changes resembling Leigh syndrome, one of the more common childhood mitochondrial neurological diseases. Functional studies in patient fibroblasts showed a heightened sensitivity to mitochondrial metabolic stress and increased mitochondrial superoxide levels. Quantitative proteomic analysis demonstrated decreased levels of subunits of the mitochondrial respiratory chain complex I, and both the small and large subunits of the mitochondrial ribosome, suggesting a mitoribosomal defect. Our findings support the critical role of PYROXD2 in human cells, and suggest that the biallelic PYROXD2 variants are associated with mitochondrial dysfunction, and can plausibly explain the child's clinical presentation.
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    Mosaic MECP2 variants in males with classical Rett syndrome features, including stereotypical hand movements
    Schonewolf-Greulich, B ; Bisgaard, A-M ; Duno, M ; Jespersgaard, C ; Rokkjaer, M ; Hansen, LK ; Tsoutsou, E ; Sofokleous, C ; Topcu, M ; Kaur, S ; Van Bergen, NJ ; Brondum-Nielsen, K ; Larsen, MJ ; Sorensen, KP ; Christodoulou, J ; Fagerberg, CR ; Tumer, Z (WILEY, 2019-03)
    Rett syndrome is rarely suspected in males because of the X-linked dominant inheritance. In the literature, only six male patients have been reported with methyl-CpG-binding protein 2 (MECP2) mosaicism. Next-generation sequencing (NGS) methods have enabled better detection of somatic mosaicism compared to conventional Sanger sequencing; however, mosaics can still be difficult to detect. We present clinical and molecular findings in two males mosaic for a pathogenic MECP2 variant. Both have been reexamined using deep sequencing of DNA isolated from four different cell tissues (blood, muscle, fibroblasts and oral mucosa). Deep sequencing of the different tissues revealed that the variants were present in all tissues. In one patient, the molecular diagnosis could only be established by reexamination after a normal whole exome sequencing, and the other case is an example of reverse genetic diagnostics. Rett syndrome should be considered in males with neurodevelopmental delay and stereotypical hand movements. Subsequent to clinical diagnosis males should be investigated with NGS-based technologies of MECP2 with high read depth and a low threshold for variant calls. If the initial analysis on full blood derived DNA fails to confirm the suspicion, we recommend repeating the analysis on another tissue, preferentially fibroblasts to increase the diagnostic yield.
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    Clinician's guide to genes associated with Rett-like phenotypes-Investigation of a Danish cohort and review of the literature
    Schonewolf-Greulich, B ; Bisgaard, A-M ; Moller, RS ; Duno, M ; Brondum-Nielsen, K ; Kaur, S ; Van Bergen, NJ ; Lunke, S ; Eggers, S ; Jespersgaard, C ; Christodoulou, J ; Tumer, Z (WILEY, 2019-02)
    The differential diagnostics in Rett syndrome has evolved with the development of next generation sequencing-based techniques and many patients have been diagnosed with other syndromes or variants in newly described genes where the associated phenotype(s) is yet to be fully explored. The term Rett-like refers to phenotypes with distinct overlapping features of Rett syndrome where the clinical criteria are not completely fulfilled. In this study we have combined a review of Rett-like disorders with data from a Danish cohort of 35 patients with Rett-like phenotypes emphasizing the diagnostic overlap with Pitt-Hopkins syndrome, Cornelia de Lange syndrome with SMC1A variants, and epileptic encephalopathies, for example, due to STXBP1 variants. We also found a patient with a pathogenic variant in KCNB1, which has not been previously linked to a Rett-like phenotype. This study underlines the clinical and genetic heterogeneity of a Rett syndrome spectrum, and provides an overview of the Rett syndrome-related genes described to date, and hence serves as a guide for diagnosing patients with Rett-like phenotypes.
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    Abnormalities of mitochondrial dynamics and bioenergetics in neuronal cells from CDKL5 deficiency disorder
    Van Bergen, NJ ; Massey, S ; Stait, T ; Ellery, M ; Reljic, B ; Formosa, LE ; Quigley, A ; Dottori, M ; Thorburn, D ; Stroud, DA ; Christodoulou, J (ACADEMIC PRESS INC ELSEVIER SCIENCE, 2021-07)
    CDKL5 deficiency disorder (CDD) is a rare neurodevelopmental disorder caused by pathogenic variants in the Cyclin-dependent kinase-like 5 (CDKL5) gene, resulting in dysfunctional CDKL5 protein. It predominantly affects females and causes seizures in the first few months of life, ultimately resulting in severe intellectual disability. In the absence of targeted therapies, treatment is currently only symptomatic. CDKL5 is a serine/threonine kinase that is highly expressed in the brain, with a critical role in neuronal development. Evidence of mitochondrial dysfunction in CDD is gathering, but has not been studied extensively. We used human patient-derived induced pluripotent stem cells with a pathogenic truncating mutation (p.Arg59*) and CRISPR/Cas9 gene-corrected isogenic controls, differentiated into neurons, to investigate the impact of CDKL5 mutation on cellular function. Quantitative proteomics indicated mitochondrial defects in CDKL5 p.Arg59* neurons, and mitochondrial bioenergetics analysis confirmed decreased activity of mitochondrial respiratory chain complexes. Additionally, mitochondrial trafficking velocity was significantly impaired, and there was a higher percentage of stationary mitochondria. We propose mitochondrial dysfunction is contributing to CDD pathology, and should be a focus for development of targeted treatments for CDD.
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    Mutations in the exocyst component EXOC2 cause severe defects in human brain development
    Van Bergen, NJ ; Ahmed, SM ; Collins, F ; Cowley, M ; Vetro, A ; Dale, RC ; Hock, DH ; de Caestecker, C ; Menezes, M ; Massey, S ; Ho, G ; Pisano, T ; Glover, S ; Gusman, J ; Stroud, DA ; Dinger, M ; Guerrini, R ; Macara, IG ; Christodoulou, J (ROCKEFELLER UNIV PRESS, 2020-10)
    The exocyst, an octameric protein complex, is an essential component of the membrane transport machinery required for tethering and fusion of vesicles at the plasma membrane. We report pathogenic variants in an exocyst subunit, EXOC2 (Sec5). Affected individuals have severe developmental delay, dysmorphism, and brain abnormalities; variability associated with epilepsy; and poor motor skills. Family 1 had two offspring with a homozygous truncating variant in EXOC2 that leads to nonsense-mediated decay of EXOC2 transcript, a severe reduction in exocytosis and vesicle fusion, and undetectable levels of EXOC2 protein. The patient from Family 2 had a milder clinical phenotype and reduced exocytosis. Cells from both patients showed defective Arl13b localization to the primary cilium. The discovery of mutations that partially disable exocyst function provides valuable insight into this essential protein complex in neural development. Since EXOC2 and other exocyst complex subunits are critical to neuronal function, our findings suggest that EXOC2 variants are the cause of the patients' neurological disorders.
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    Expansion of the phenotypic spectrum of de novo missense variants in kinesin family member 1A (KIF1A)
    Kaur, S ; Van Bergen, NJ ; Verhey, KJ ; Nowell, CJ ; Budaitis, B ; Yue, Y ; Ellaway, C ; Brunetti-Pierri, N ; Cappuccio, G ; Bruno, I ; Boyle, L ; Nigro, V ; Torella, A ; Roscioli, T ; Cowley, MJ ; Massey, S ; Sonawane, R ; Burton, MD ; Schonewolf-Greulich, B ; Tumer, Z ; Chung, WK ; Gold, WA ; Christodoulou, J (WILEY-HINDAWI, 2020-10)
    Defects in the motor domain of kinesin family member 1A (KIF1A), a neuron-specific ATP-dependent anterograde axonal transporter of synaptic cargo, are well-recognized to cause a spectrum of neurological conditions, commonly known as KIF1A-associated neurological disorders (KAND). Here, we report one mutation-negative female with classic Rett syndrome (RTT) harboring a de novo heterozygous novel variant [NP_001230937.1:p.(Asp248Glu)] in the highly conserved motor domain of KIF1A. In addition, three individuals with severe neurodevelopmental disorder along with clinical features overlapping with KAND are also reported carrying de novo heterozygous novel [NP_001230937.1:p.(Cys92Arg) and p.(Pro305Leu)] or previously reported [NP_001230937.1:p.(Thr99Met)] variants in KIF1A. In silico tools predicted these variants to be likely pathogenic, and 3D molecular modeling predicted defective ATP hydrolysis and/or microtubule binding. Using the neurite tip accumulation assay, we demonstrated that all novel KIF1A variants significantly reduced the ability of the motor domain of KIF1A to accumulate along the neurite lengths of differentiated SH-SY5Y cells. In vitro microtubule gliding assays showed significantly reduced velocities for the variant p.(Asp248Glu) and reduced microtubule binding for the p.(Cys92Arg) and p.(Pro305Leu) variants, suggesting a decreased ability of KIF1A to move along microtubules. Thus, this study further expanded the phenotypic characteristics of KAND individuals with pathogenic variants in the KIF1A motor domain to include clinical features commonly seen in RTT individuals.