PhenoVar: a Phenotype-driven Approach in Clinical Genomics for the Diagnosis of Polymalformative Syndromes

Overview

Journal BMC Med Genomics

Publisher Biomed Central

Specialty Genetics

Date 2014 Jun 3

PMID 24884844

Citations 11

Authors

Yannis J Trakadis

Caroline Buote

Jean-Francois Therriault

Pierre-Etienne Jacques

Hugo Larochelle

Sebastien Levesque

Affiliations

Soon will be listed here.

Abstract

Background: We propose a phenotype-driven analysis of encrypted exome data to facilitate the widespread implementation of exome sequencing as a clinical genetic screening test.Twenty test-patients with varied syndromes were selected from the literature. For each patient, the mutation, phenotypic data, and genetic diagnosis were available. Next, control exome-files, each modified to include one of these twenty mutations, were assigned to the corresponding test-patients. These data were used by a geneticist blinded to the diagnoses to test the efficiency of our software, PhenoVar. The score assigned by PhenoVar to any genetic diagnosis listed in OMIM (Online Mendelian Inheritance in Man) took into consideration both the patient's phenotype and all variations present in the corresponding exome. The physician did not have access to the individual mutations. PhenoVar filtered the search using a cut-off phenotypic match threshold to prevent undesired discovery of incidental findings and ranked the OMIM entries according to diagnostic score.

Results: When assigning the same weight to all variants in the exome, PhenoVar predicted the correct diagnosis in 10/20 patients, while in 15/20 the correct diagnosis was among the 4 highest ranked diagnoses. When assigning a higher weight to variants known, or bioinformatically predicted, to cause disease, PhenoVar's yield increased to 14/20 (18/20 in top 4). No incidental findings were identified using our cut-off phenotypic threshold.

Conclusion: The phenotype-driven approach described could render widespread use of ES more practical, ethical and clinically useful. The implications about novel disease identification, advancement of complex diseases and personalized medicine are discussed.

Citing Articles

High-throughput Second-generation Sequencing Technology Assisted Diagnosis of Familial Partial Lipodystrophy (Type 2 Kobberling-Dunnigan Syndrome): A Case Report.

Deng M, Chen W, Qi Y Comb Chem High Throughput Screen. 2023; 27(2):346-351.

PMID: 37231758 DOI: 10.2174/1386207326666230523112454.

Individualised human phenotype ontology gene panels improve clinical whole exome and genome sequencing analytical efficacy in a cohort of developmental and epileptic encephalopathies.

Henry O, Stodberg T, Batelson S, Rasi C, Stranneheim H, Wedell A Mol Genet Genomic Med. 2023; 11(7):e2167.

PMID: 36967109 PMC: 10337286. DOI: 10.1002/mgg3.2167.

Phenotype-aware prioritisation of rare Mendelian disease variants.

Kelly C, Szabo A, Pontikos N, Arno G, Robinson P, Jacobsen J Trends Genet. 2022; 38(12):1271-1283.

PMID: 35934592 PMC: 9950798. DOI: 10.1016/j.tig.2022.07.002.

Diagnostic yield and clinical utility of whole exome sequencing using an automated variant prioritization system, EVIDENCE.

Seo G, Kim T, Choi I, Park J, Lee J, Kim S Clin Genet. 2020; 98(6):562-570.

PMID: 32901917 PMC: 7756481. DOI: 10.1111/cge.13848.

An Improved Phenotype-Driven Tool for Rare Mendelian Variant Prioritization: Benchmarking Exomiser on Real Patient Whole-Exome Data.

Cipriani V, Pontikos N, Arno G, Sergouniotis P, Lenassi E, Thawong P Genes (Basel). 2020; 11(4).

PMID: 32340307 PMC: 7230372. DOI: 10.3390/genes11040460.

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