Development and Evaluation of a Telephone Communication Protocol for the Delivery of Personalized Melanoma Genomic Risk to the General Population.

Fenton, GL; Smit, AK; Freeman, L; Badcock, C; Dunlop, K; Butow, PN; Kirk, J; Cust, AE

Development and Evaluation of a Telephone Communication Protocol for the Delivery of Personalized Melanoma Genomic Risk to the General Population.

Fenton, GL Smit, AK Freeman, L

Badcock, C Dunlop, K Butow, PN Kirk, J Cust, AE

Permalink

Publisher:: SPRINGER
Publication Type:: Journal Article
Citation:: J Genet Couns, 2018, 27, (2), pp. 370-380
Issue Date:: 2018-04

Closed Access

	Filename	Description	Size
	Journal of Genetic Counseling - 2017 - Fenton - Development and Evaluation of a Telephone Communication Protocol for the.pdf	Published version	562.35 kB		View/Open

Copyright Clearance Process

Recently Added
In Progress
Closed Access

This item is closed access and not available.

Full metadata record

Field	Value	Language
dc.contributor.author	Fenton, GL
dc.contributor.author	Smit, AK
dc.contributor.author	Freeman, L https://orcid.org/0000-0002-5814-3894
dc.contributor.author	Badcock, C
dc.contributor.author	Dunlop, K
dc.contributor.author	Butow, PN
dc.contributor.author	Kirk, J
dc.contributor.author	Cust, AE
dc.date.accessioned	2022-08-16T05:19:41Z
dc.date.available	2017-11-21
dc.date.available	2022-08-16T05:19:41Z
dc.date.issued	2018-04
dc.identifier.citation	J Genet Couns, 2018, 27, (2), pp. 370-380
dc.identifier.issn	1059-7700
dc.identifier.issn	1573-3599
dc.identifier.uri	http://hdl.handle.net/10453/160343
dc.description.abstract	Communicating personalized genomic risk results for common diseases to the general population as a form of tailored prevention is novel and may require alternative genetic counseling service delivery models. We describe the development and evaluation of a communication protocol for disclosing melanoma genomic risk information to the asymptomatic general population and assess participants' satisfaction and acceptability. Participants (n = 117) were aged 22-69 years, living in New South Wales, Australia and unselected for family history. They provided a saliva sample and had genomic testing for melanoma for low to moderate penetrant melanoma susceptibility variants in 21 genes. Participants could choose to receive their results from a genetic counselor via telephone, followed by a mailed booklet or to receive their risk result via mailed booklet only with a follow-up call for those at high risk. A follow-up questionnaire was completed by 85% of participants 3-months later. Most participants (80%) elected to receive their result via telephone. Participants were highly satisfied with the delivery of results (mean 3.4 out of 4, standard deviation 0.5), and this did not differ by delivery mode, risk category, age or sex. On follow-up, 75% accurately recalled their risk category, 6% indicated a preference for a different delivery mode, either electronic or face-to-face. The process of disclosing genomic risk results to the general population over the telephone with accompanying written material was feasible and acceptable, and may be useful for communicating polygenic risk for common diseases in the context of increasing demands for genomic testing.
dc.format	Print-Electronic
dc.language	eng
dc.publisher	SPRINGER
dc.relation.ispartof	J Genet Couns
dc.relation.isbasedon	10.1007/s10897-017-0183-7
dc.rights	info:eu-repo/semantics/closedAccess
dc.subject	1103 Clinical Sciences
dc.subject.classification	Genetics & Heredity
dc.subject.mesh	Adult
dc.subject.mesh	Aged
dc.subject.mesh	Communication
dc.subject.mesh	Female
dc.subject.mesh	Genome, Human
dc.subject.mesh	Humans
dc.subject.mesh	Male
dc.subject.mesh	Melanoma
dc.subject.mesh	Middle Aged
dc.subject.mesh	New South Wales
dc.subject.mesh	Precision Medicine
dc.subject.mesh	Program Evaluation
dc.subject.mesh	Risk Factors
dc.subject.mesh	Surveys and Questionnaires
dc.subject.mesh	Telephone
dc.subject.mesh	Young Adult
dc.subject.mesh	Humans
dc.subject.mesh	Melanoma
dc.subject.mesh	Risk Factors
dc.subject.mesh	Program Evaluation
dc.subject.mesh	Communication
dc.subject.mesh	Genome, Human
dc.subject.mesh	Telephone
dc.subject.mesh	Adult
dc.subject.mesh	Aged
dc.subject.mesh	Middle Aged
dc.subject.mesh	New South Wales
dc.subject.mesh	Female
dc.subject.mesh	Male
dc.subject.mesh	Young Adult
dc.subject.mesh	Surveys and Questionnaires
dc.subject.mesh	Precision Medicine
dc.title	Development and Evaluation of a Telephone Communication Protocol for the Delivery of Personalized Melanoma Genomic Risk to the General Population.
dc.type	Journal Article
utslib.citation.volume	27
utslib.location.activity	United States
utslib.for	1103 Clinical Sciences
pubs.organisational-group	/University of Technology Sydney
pubs.organisational-group	/University of Technology Sydney/Faculty of Health
utslib.copyright.status	closed_access	*
dc.date.updated	2022-08-16T05:19:39Z
pubs.issue	2
pubs.publication-status	Published
pubs.volume	27
utslib.citation.issue	2

Abstract:

Communicating personalized genomic risk results for common diseases to the general population as a form of tailored prevention is novel and may require alternative genetic counseling service delivery models. We describe the development and evaluation of a communication protocol for disclosing melanoma genomic risk information to the asymptomatic general population and assess participants' satisfaction and acceptability. Participants (n = 117) were aged 22-69 years, living in New South Wales, Australia and unselected for family history. They provided a saliva sample and had genomic testing for melanoma for low to moderate penetrant melanoma susceptibility variants in 21 genes. Participants could choose to receive their results from a genetic counselor via telephone, followed by a mailed booklet or to receive their risk result via mailed booklet only with a follow-up call for those at high risk. A follow-up questionnaire was completed by 85% of participants 3-months later. Most participants (80%) elected to receive their result via telephone. Participants were highly satisfied with the delivery of results (mean 3.4 out of 4, standard deviation 0.5), and this did not differ by delivery mode, risk category, age or sex. On follow-up, 75% accurately recalled their risk category, 6% indicated a preference for a different delivery mode, either electronic or face-to-face. The process of disclosing genomic risk results to the general population over the telephone with accompanying written material was feasible and acceptable, and may be useful for communicating polygenic risk for common diseases in the context of increasing demands for genomic testing.

Please use this identifier to cite or link to this item:

http://hdl.handle.net/10453/160343