Combinatorial clinically driven blood biomarker functional genomics significantly enhances genotype-phenotype resolution and diagnostics in neuromuscular disease

Chakravorty, Samya; Berger, Kiera; Rufibach, Laura; Gloster, Logan; Emmons, Sarah; Shenoy, Sreekala; Hegde, Madhuri; Dinasarapu, Ashok R.; Gibson, Greg

doi:10.1101/2021.01.14.21249850

Cited by 1 publication

(1 citation statement)

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“…In large cohorts, transcript abundance can also be used to analyze downstream effects of some pathogenic variants and characterize pathways involved in disease [ 48 , 49 ]. Even where a likely pathogenic variant is identified by DNA analysis, RNAseq can provide supporting evidence that the transcript is affected, and may be used to establish that both alleles are affected in trans by different mutations [ 50 , 51 ]. Although peripheral blood is a mixture of dozens of cell types, so long as the defect is observed in one or more of the major leukocyte or monocyte populations, bulk RNAseq should be a useful source of clinically actionable information.…”

Section: Introductionmentioning

confidence: 99%

Targeted RNAseq Improves Clinical Diagnosis of Very Early-Onset Pediatric Immune Dysregulation

Berger

Arafat

Chandrakasan

et al. 2022

JPM

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Despite increased use of whole exome sequencing (WES) for the clinical analysis of rare disease, overall diagnostic yield for most disorders hovers around 30%. Previous studies of mRNA have succeeded in increasing diagnoses for clearly defined disorders of monogenic inheritance. We asked if targeted RNA sequencing could provide similar benefits for primary immunodeficiencies (PIDs) and very early-onset inflammatory bowel disease (VEOIBD), both of which are difficult to diagnose due to high heterogeneity and variable severity. We performed targeted RNA sequencing of a panel of 260 immune-related genes for a cohort of 13 patients (seven suspected PID cases and six VEOIBD) and analyzed variants, splicing, and exon usage. Exonic variants were identified in seven cases, some of which had been previously prioritized by exome sequencing. For four cases, allele specific expression or lack thereof provided additional insights into possible disease mechanisms. In addition, we identified five instances of aberrant splicing associated with four variants. Three of these variants had been previously classified as benign in ClinVar based on population frequency. Digenic or oligogenic inheritance is suggested for at least two patients. In addition to validating the use of targeted RNA sequencing, our results show that rare disease research will benefit from incorporating contributing genetic factors into the diagnostic approach.

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