Interpretation of mRNA splicing mutations in genetic disease: review of the literature and guidelines for information-theoretical analysis

Caminsky, Natasha; Mucaki, Eliseos J.

doi:10.12688/f1000research.5654.1

Cited by 85 publications

(79 citation statements)

References 244 publications

(384 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…ASSEDA is a web interface, which provides a tool to predict the effects of sequence changes that alter mRNA splicing in human disease. This tool is able to evaluate changes in splice site strength based on theory-based modelling of donor and acceptor splice sites [25]. …”

Section: Methodsmentioning

confidence: 99%

A targeted genome association study examining transient receptor potential ion channels, acetylcholine receptors, and adrenergic receptors in Chronic Fatigue Syndrome/Myalgic Encephalomyelitis

et al. 2016

View full text Add to dashboard Cite

BackgroundChronic Fatigue Syndrome, also known as Myalgic Encephalomyelitis (CFS/ME) is a debilitating condition of unknown aetiology. It is characterized by a range of physiological effects including neurological, sensory and motor disturbances. This study examined candidate genes for the above clinical manifestations to identify single nucleotide polymorphism (SNP) alleles associated with CFS/ME compared with healthy controls.MethodsDNA was extracted and whole genome genotyping was performed using the HumanOmniExpress BeadChip array. Gene families for transient receptor potential ion channels, acetylcholine receptors, and adrenergic receptors, and acetylcholinesterase were targeted. The frequency of each SNP and their association between CFS/ME and healthy controls was examined using Fisher’s exact test, and to adjust for multiple testing, False Detection Rate (FDR) and Bonferroni corrections were applied (p < 0.05).ResultsThe study included 172 participants, consisting of 95 Fukuda defined CFS/ME patients (45.8 ± 8.9; 69 % female) and 77 healthy controls (42.3 ± 10.3; 63 % female). A total of 950 SNPs were included for analysis. 60 significant SNPs were associated with CFS/ME compared with healthy controls. After applying FDR and Bonferroni corrections, SNP rs2322333 in adrenergic receptor α1 (ADRA1A) was higher in CFS/ME compared with healthy controls (45.3 % vs. 23.4 %; p = 0.059). The genotype class that was homozygous minor (AA) was substantially lower in CFS/ME compared with healthy controls (4.2 % vs. 24.7 %).ConclusionsThis study reports for the first time the identification of ADRA1A and a possible association between CFS/ME and genotype classes. Further examination of the functional role of this class of adrenergic receptors may elucidate the cause of particular clinical manifestations observed in CFS/ME.

show abstract

Section: Methodsmentioning

confidence: 99%

A targeted genome association study examining transient receptor potential ion channels, acetylcholine receptors, and adrenergic receptors in Chronic Fatigue Syndrome/Myalgic Encephalomyelitis

et al. 2016

View full text Add to dashboard Cite

show abstract

“…35 In the latter, a considerable amount of Spaghetti plot showing the increase of the area of reduced FAF in patients followed longitudinally. Note that even though most of group B had small areas of reduced FAF, they were comparatively younger than patients from group C, reflecting the earlier disease onset.…”

Section: Splicing Mutationsmentioning

confidence: 99%

Phenotype and Progression of Retinal Degeneration Associated With Nullizigosity of ABCA4

Fakin

Robson

Fujinami

et al. 2016

Invest. Ophthalmol. Vis. Sci.

View full text Add to dashboard Cite

show abstract

“…The combination of DNA and RNA-based analyses complement each other, serving as mutual controls for verifying potential findings [17] and increasing the sensitivity of variant detection, a feature especially important for analysis of low-purity tumours [25] . In particular, identification of variants affecting RNA processing, eventually leading to oncogenic isoforms (e.g., EGFR viii/ERBB2 ΔEx16), is close to impossible using genome-based analyses in isolation [26] , since the effect is only visible when considering the gene structure, as determined by RNAseq. Similarly, potential effects of RNA editing are inherently only detectable by RNA-based analyses.…”

Section: Is More More?mentioning

confidence: 99%

Cancer Precision Medicine: Why More Is More and DNA Is Not Enough

Schütte

Ogilvie

Rieke

et al. 2017

Public Health Genomics

View full text Add to dashboard Cite

Every tumour is different. They arise in patients with different genomes, from cells with different epigenetic modifications, and by random processes affecting the genome and/or epigenome of a somatic cell, allowing it to escape the usual controls on its growth. Tumours and patients therefore often respond very differently to the drugs they receive. Cancer precision medicine aims to characterise the tumour (and often also the patient) to be able to predict, with high accuracy, its response to different treatments, with options ranging from the selective characterisation of a few genomic variants considered particularly important to predict the response of the tumour to specific drugs, to deep genome analysis of both tumour and patient, combined with deep transcriptome analysis of the tumour. Here, we compare the expected results of carrying out such analyses at different levels, from different size panels to a comprehensive analysis incorporating both patient and tumour at the DNA and RNA levels. In doing so, we illustrate the additional power gained by this unusually deep analysis strategy, a potential basis for a future precision medicine first strategy in cancer drug therapy. However, this is only a step along the way of increasingly detailed molecular characterisation, which in our view will, in the future, introduce additional molecular characterisation techniques, including systematic analysis of proteins and protein modification states and different types of metabolites in the tumour, systematic analysis of circulating tumour cells and nucleic acids, the use of spatially resolved analysis techniques to address the problem of tumour heterogeneity as well as the deep analyses of the immune system of the patient to, e.g., predict the response of the patient to different types of immunotherapy. Such analyses will generate data sets of even greater complexity, requiring mechanistic modelling approaches to capture enough of the complex situation in the real patient to be able to accurately predict his/her responses to all available therapies.

show abstract

Interpretation of mRNA splicing mutations in genetic disease: review of the literature and guidelines for information-theoretical analysis

Cited by 85 publications

References 244 publications

A targeted genome association study examining transient receptor potential ion channels, acetylcholine receptors, and adrenergic receptors in Chronic Fatigue Syndrome/Myalgic Encephalomyelitis

A targeted genome association study examining transient receptor potential ion channels, acetylcholine receptors, and adrenergic receptors in Chronic Fatigue Syndrome/Myalgic Encephalomyelitis

Phenotype and Progression of Retinal Degeneration Associated With Nullizigosity of ABCA4

Cancer Precision Medicine: Why More Is More and DNA Is Not Enough

Contact Info

Product

Resources

About