Clinical phenome scanning

Nader Ghebranious; Catherine A. McCarty; Russell A. Wilke

doi:10.2217/17410541.4.2.175

Clinical phenome scanning

Nader Ghebranious, Catherine A. McCarty, Russell A. Wilke

Administration (DMED)

Research output: Contribution to journal › Article › peer-review

11 Scopus citations

Abstract

Large population-based cohorts are ideal for the study of common, complex disorders because they allow characterization of gene-gene and gene-environment interactions. We propose a clinical phenome scanning approach to genotype-phenotype association studies, as this approach acknowledges the heterogeneous nature of common diseases and takes advantage of the unprecedented density of phenotypic data available in population-based DNA biobanks. By analogy to genome-wide scanning, the construction of a clinical phenome scan includes a complete scan of all clinically available information (housed in electronic medical records). This is done on a subject-by-subject basis and the resulting phenomes can subsequently be interrogated for association with a single allele for any given gene. By prioritizing phenotype (rather than genotype), this approach allows investigators to ask the question "Which disease is associated with a given gene?" rather than "Which gene is associated with a given disease?".

Original language	English (US)
Pages (from-to)	175-182
Number of pages	8
Journal	Personalized Medicine
Volume	4
Issue number	2
DOIs	https://doi.org/10.2217/17410541.4.2.175
State	Published - May 2007

Keywords

Biobank
Clinical phenome scan
Common diseases
DNA
Phenomic markers
Pleiotropy

Access

10.2217/17410541.4.2.175

OpenUrl availability

Full text

Cite this

@article{b79af3235a8843faa50c326f261c58d5,

title = "Clinical phenome scanning",

abstract = "Large population-based cohorts are ideal for the study of common, complex disorders because they allow characterization of gene-gene and gene-environment interactions. We propose a clinical phenome scanning approach to genotype-phenotype association studies, as this approach acknowledges the heterogeneous nature of common diseases and takes advantage of the unprecedented density of phenotypic data available in population-based DNA biobanks. By analogy to genome-wide scanning, the construction of a clinical phenome scan includes a complete scan of all clinically available information (housed in electronic medical records). This is done on a subject-by-subject basis and the resulting phenomes can subsequently be interrogated for association with a single allele for any given gene. By prioritizing phenotype (rather than genotype), this approach allows investigators to ask the question {"}Which disease is associated with a given gene?{"} rather than {"}Which gene is associated with a given disease?{"}.",

keywords = "Biobank, Clinical phenome scan, Common diseases, DNA, Phenomic markers, Pleiotropy",

author = "Nader Ghebranious and McCarty, {Catherine A.} and Wilke, {Russell A.}",

year = "2007",

month = may,

doi = "10.2217/17410541.4.2.175",

language = "English (US)",

volume = "4",

pages = "175--182",

journal = "Personalized Medicine",

issn = "1741-0541",

publisher = "Future Medicine Ltd.",

number = "2",

}

TY - JOUR

T1 - Clinical phenome scanning

AU - Ghebranious, Nader

AU - McCarty, Catherine A.

AU - Wilke, Russell A.

PY - 2007/5

Y1 - 2007/5

N2 - Large population-based cohorts are ideal for the study of common, complex disorders because they allow characterization of gene-gene and gene-environment interactions. We propose a clinical phenome scanning approach to genotype-phenotype association studies, as this approach acknowledges the heterogeneous nature of common diseases and takes advantage of the unprecedented density of phenotypic data available in population-based DNA biobanks. By analogy to genome-wide scanning, the construction of a clinical phenome scan includes a complete scan of all clinically available information (housed in electronic medical records). This is done on a subject-by-subject basis and the resulting phenomes can subsequently be interrogated for association with a single allele for any given gene. By prioritizing phenotype (rather than genotype), this approach allows investigators to ask the question "Which disease is associated with a given gene?" rather than "Which gene is associated with a given disease?".

AB - Large population-based cohorts are ideal for the study of common, complex disorders because they allow characterization of gene-gene and gene-environment interactions. We propose a clinical phenome scanning approach to genotype-phenotype association studies, as this approach acknowledges the heterogeneous nature of common diseases and takes advantage of the unprecedented density of phenotypic data available in population-based DNA biobanks. By analogy to genome-wide scanning, the construction of a clinical phenome scan includes a complete scan of all clinically available information (housed in electronic medical records). This is done on a subject-by-subject basis and the resulting phenomes can subsequently be interrogated for association with a single allele for any given gene. By prioritizing phenotype (rather than genotype), this approach allows investigators to ask the question "Which disease is associated with a given gene?" rather than "Which gene is associated with a given disease?".

KW - Biobank

KW - Clinical phenome scan

KW - Common diseases

KW - DNA

KW - Phenomic markers

KW - Pleiotropy

UR - http://www.scopus.com/inward/record.url?scp=34249820776&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=34249820776&partnerID=8YFLogxK

U2 - 10.2217/17410541.4.2.175

DO - 10.2217/17410541.4.2.175

M3 - Article

AN - SCOPUS:34249820776

SN - 1741-0541

VL - 4

SP - 175

EP - 182

JO - Personalized Medicine

JF - Personalized Medicine

IS - 2

ER -

Clinical phenome scanning

Abstract

Keywords

Access

OpenUrl availability

Other files and links

Fingerprint

Cite this