COL4A5 and LAMA5 variants co-inherited in familial hematuria: digenic inheritance or genetic modifier effect?

Voskarides, Konstantinos; Papagregoriou, Gregory; Hadjipanagi, Despina; Petrou, Ioanelli; Savva, Isavella; Elia, Avraam; Athanasiou, Yiannis; Androulla, Pastelli; Kkolou, Maria; Hadjigavriel, Michael; Stavrou, Christoforos; Pierides, Alkis; Deltas, Constantinos

doi:10.1186/s12882-018-0906-5

Cited by 39 publications

(33 citation statements)

References 37 publications

(31 reference statements)

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“…Mice with a double Lama5 knockout are fatal; however, mice with a hypomorphic Lama5 mutation (Lama5neo) that reduces laminin‐α5 expression, exhibit proteinuria, hematuria and cystic kidneys . It is probable, therefore, that although this might not represent true DI, the LAMA5 ‐p.Pro1243Leu variant behaves as a hypomorphic mutation that adds up to the Alport background…”

Section: True Non‐mendelian Digenic Inheritancementioning

confidence: 99%

“…52 Several reports on renal genetic studies using NGS have identified rare patients with 2 mutations in separate genes but it is not clear whether they act as modifiers to each other or they represent true DI of nephrotic syndrome. 53 In our setup we studied a family where 54 It is probable, therefore, that although this might not represent true DI, the LAMA5-p.Pro1243Leu variant behaves as a hypomorphic mutation that adds up to the Alport background 55 Evidence for true DI was published while this review was in press, in a Libyan patient with distal renal tubular acidosis (dRTA).…”

Section: Selected Recent Publications On True Digenic Inheritancementioning

confidence: 99%

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Digenic inheritance and genetic modifiers

Deltas

2018

Clinical Genetics

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Digenic inheritance (DI) concerns pathologies with the simplest form of multigenic etiology, implicating more than 1 gene (and perhaps the environment). True DI is when biallelic or even triallelic mutations in 2 distinct genes, in cis or in trans, are necessary and sufficient to cause pathology with a defined diagnosis. In true DI, a heterozygous mutation in each of 2 genes alone is not associated with a recognizable phenotype. Well-documented diseases with true DI are so far rare and follow non-Mendelian inheritance. DI is also encountered when by serendipity, pathogenic mutations responsible for 2 distinct disease entities are co-inherited, leading to a mixed phenotype. Also, we can consider many true monogenic Mendelian conditions, which show impressively broad spectrum of phenotypes due to pseudo-DI, as a result of co-inheriting genetic modifiers (GMs). I am herewith reviewing examples of GM and embark on presenting some recent notable examples of true DI, with wider discussion of the literature. Undeniably, the advent of high throughput sequencing is bound to unravel more patients suffering with true DI conditions and elucidate many important GM, thus impacting precision medicine.

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Section: True Non‐mendelian Digenic Inheritancementioning

confidence: 99%

Section: Selected Recent Publications On True Digenic Inheritancementioning

confidence: 99%

Digenic inheritance and genetic modifiers

Deltas

2018

Clinical Genetics

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“…Arrows point to the mutations. Family 7 has one novel mutation, c. 3,782 G > A researches and cases reported that AS patients with COL4A5 mutations who have coinherited with COL4A3/COL4A4, MYO1E and LAMA5 mutations could exacerbated phenotypes (Lennon et al, 2015;Voskarides et al, 2018). These clinical symptoms occur mostly in the late disease stages and are thought to be secondary changes caused by primary GBM defects resulting from abnormalities in the collagen reticular structure (Braunisch et al, 2018).…”

Section: F I G U R Ementioning

confidence: 99%

Genotype‐phenotype correlation and prognostic impact in Chinese patients with Alport Syndrome

Shang

Peng

Wang

et al. 2019

Molec Gen & Gen Med

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Background Alport Syndrome (AS) is a progressive hereditary glomerular disease. It is often accompanied by sensorineural hearing loss and ocular abnormalities and can sometimes develop into end stage renal disease (ESRD), which is caused by mutations in the genes encoding the collagen type IV family of proteins. Methods This study analyzed the association between the clinical data of seven AS families and genes and the disease progression of different mutation types, including COL4A3 (OMIM 120070)， COL4A4 (OMIM 120131), and COL4A5 (OMIM303630). Results A total of six new pathogenic mutation sites, one complex heterozygous mutation at COL4A3, and a combined mutation of COL4A5 and INF2 (OMIM 610982) were identified in this study. It was revealed that the clinical manifestations of X‐linked AS caused by mutations in the COL4A5 gene were more severe in males than in females. In addition, the difference in patient phenotype can be attributed to the location of gene mutations affecting the protein domain or functional domain. Our data suggested that the gene deletion and nonsense mutations had a high risk for progression to ESRD. Conclusion Our results revealed the spectrum of type IV collagen genes, which contribute to the enrichment of database resources and has important implications in the diagnosis, prognosis, and guiding treatment of AS.

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“…We looked for references in literature for the top suggested novel genes per disease by mantis-ml and have found supporting evidence for several genes. For instance, LAMA5 has been reported in the last two years to be co-inherited with COL4A5 in familial hematuria 21 and hosting variants that may affect pediatric nephrotic syndrome 22,23 . Moreover, NOS3 and NOS2-although not associated with CKD in OMIM -have already been implicated in Chronic Kidney Disease in a fair amount of studies 24, 25,26,27 , while MEF2C, a gene typically associated with mental disorders, has also been associated with estimated Glomerular Filtration Rate (eGFR) or proteinuria 28 .…”

Section: Application Of Mantis-ml Predictions To Triage Results From mentioning

confidence: 99%

Stochastic semi-supervised learning to prioritise genes from high-throughput genomic screens

Vitsios

Petrovski

2019

Preprint

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Access to large-scale genomics datasets has increased the utility of hypothesis-free genome-wide analyses that result in candidate lists of genes. Often these analyses highlight several gene signals that might contribute to pathogenesis but are insufficiently powered to reach experiment-wide significance. This often triggers a process of laborious evaluation of highly-ranked genes through manual inspection of various public knowledge resources to triage those considered sufficiently interesting for deeper investigation. Here, we introduce a novel multi-dimensional, multi-step machine learning framework to objectively and more holistically assess biological relevance of genes to disease studies, by relying on a plethora of gene-associated annotations. We developed mantis-ml to serve as an automated machine learning (AutoML) framework, following a stochastic semisupervised learning approach to rank known and novel disease-associated genes through iterative training and prediction sessions of random balanced datasets across the protein-coding exome (n=18,626 genes). We applied this framework on a range of disease-specific areas and as a generic disease likelihood estimator, achieving an average Area Under Curve (AUC) prediction performance of 0.85. Critically, to demonstrate applied utility on exome-wide association studies, we overlapped mantis-ml disease-specific predictions with data from published cohort-level association studies. We retrieved statistically significant enrichment of high mantis-ml predictions among the top-ranked genes from hypothesis-free cohort-level statistics (p<0.05), suggesting the capture of true prioritisation signals. We believe that mantis-ml is a novel easy-to-use tool to support objectively triaging gene discovery and overall enhancing our understanding of complex genotype-phenotype associations.

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COL4A5 and LAMA5 variants co-inherited in familial hematuria: digenic inheritance or genetic modifier effect?

Cited by 39 publications

References 37 publications

Digenic inheritance and genetic modifiers

Digenic inheritance and genetic modifiers

Genotype‐phenotype correlation and prognostic impact in Chinese patients with Alport Syndrome

Stochastic semi-supervised learning to prioritise genes from high-throughput genomic screens

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