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A Variant in a MicroRNA Complementary Site in the 3′UTR of the KIT Oncogene Increases Risk of Acral Melanoma

MicroRNAs are small ~22nt single stranded RNAs that negatively regulate protein expression by binding to partially complementary sequences in the 3′UTRs of target gene mRNAs. Recently, mutations have been identified in both microRNAs and target genes that disrupt regulatory relationships, contribute...

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Autores principales: Godshalk, Sirie E., Paranjape, Trupti, Nallur, Sunitha, Speed, William, Chan, Elcie, Molinaro, Annette M., Bacchiocchi, Antonella, Hoyt, Kathleen, Tworkoski, Kathryn, Stern, David F., Sznol, Mario, Ariyan, Stephan, Lazova, Rossitza, Halaban, Ruth, Kidd, Kenneth K., Weidhaas, Joanne, Slack, Frank J.
Formato: Texto
Lenguaje:English
Publicado: 2010
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3069149/
https://www.ncbi.nlm.nih.gov/pubmed/21119596
http://dx.doi.org/10.1038/onc.2010.536
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author Godshalk, Sirie E.
Paranjape, Trupti
Nallur, Sunitha
Speed, William
Chan, Elcie
Molinaro, Annette M.
Bacchiocchi, Antonella
Hoyt, Kathleen
Tworkoski, Kathryn
Stern, David F.
Sznol, Mario
Ariyan, Stephan
Lazova, Rossitza
Halaban, Ruth
Kidd, Kenneth K.
Weidhaas, Joanne
Slack, Frank J.
author_facet Godshalk, Sirie E.
Paranjape, Trupti
Nallur, Sunitha
Speed, William
Chan, Elcie
Molinaro, Annette M.
Bacchiocchi, Antonella
Hoyt, Kathleen
Tworkoski, Kathryn
Stern, David F.
Sznol, Mario
Ariyan, Stephan
Lazova, Rossitza
Halaban, Ruth
Kidd, Kenneth K.
Weidhaas, Joanne
Slack, Frank J.
author_sort Godshalk, Sirie E.
collection PubMed
description MicroRNAs are small ~22nt single stranded RNAs that negatively regulate protein expression by binding to partially complementary sequences in the 3′UTRs of target gene mRNAs. Recently, mutations have been identified in both microRNAs and target genes that disrupt regulatory relationships, contribute to oncogenesis and serve as biomarkers for cancer risk. KIT, an established oncogene with a multifaceted role in melanogenesis and melanoma pathogenesis, has recently been shown to be up-regulated in some melanomas, and is also a target of the microRNA miR-221. Here we describe a genetic variant in the 3′UTR of the KIT oncogene that correlates with a greater than fourfold increased risk of acral melanoma. This KIT variant results in a mismatch in the seed region of a miR-221 complementary site and reporter data suggests that this mismatch can result in increased expression of the KIT oncogene. Consistent with the hypothesis that this is a functional variant, KIT mRNA and protein levels are both increased in the majority of samples harboring the KIT variant. This work identifies a novel genetic marker for increased heritable risk of melanoma.
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spelling pubmed-30691492011-09-30 A Variant in a MicroRNA Complementary Site in the 3′UTR of the KIT Oncogene Increases Risk of Acral Melanoma Godshalk, Sirie E. Paranjape, Trupti Nallur, Sunitha Speed, William Chan, Elcie Molinaro, Annette M. Bacchiocchi, Antonella Hoyt, Kathleen Tworkoski, Kathryn Stern, David F. Sznol, Mario Ariyan, Stephan Lazova, Rossitza Halaban, Ruth Kidd, Kenneth K. Weidhaas, Joanne Slack, Frank J. Oncogene Article MicroRNAs are small ~22nt single stranded RNAs that negatively regulate protein expression by binding to partially complementary sequences in the 3′UTRs of target gene mRNAs. Recently, mutations have been identified in both microRNAs and target genes that disrupt regulatory relationships, contribute to oncogenesis and serve as biomarkers for cancer risk. KIT, an established oncogene with a multifaceted role in melanogenesis and melanoma pathogenesis, has recently been shown to be up-regulated in some melanomas, and is also a target of the microRNA miR-221. Here we describe a genetic variant in the 3′UTR of the KIT oncogene that correlates with a greater than fourfold increased risk of acral melanoma. This KIT variant results in a mismatch in the seed region of a miR-221 complementary site and reporter data suggests that this mismatch can result in increased expression of the KIT oncogene. Consistent with the hypothesis that this is a functional variant, KIT mRNA and protein levels are both increased in the majority of samples harboring the KIT variant. This work identifies a novel genetic marker for increased heritable risk of melanoma. 2010-11-29 2011-03-31 /pmc/articles/PMC3069149/ /pubmed/21119596 http://dx.doi.org/10.1038/onc.2010.536 Text en Users may view, print, copy, download and text and data- mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use: http://www.nature.com/authors/editorial_policies/license.html#terms
spellingShingle Article
Godshalk, Sirie E.
Paranjape, Trupti
Nallur, Sunitha
Speed, William
Chan, Elcie
Molinaro, Annette M.
Bacchiocchi, Antonella
Hoyt, Kathleen
Tworkoski, Kathryn
Stern, David F.
Sznol, Mario
Ariyan, Stephan
Lazova, Rossitza
Halaban, Ruth
Kidd, Kenneth K.
Weidhaas, Joanne
Slack, Frank J.
A Variant in a MicroRNA Complementary Site in the 3′UTR of the KIT Oncogene Increases Risk of Acral Melanoma
title A Variant in a MicroRNA Complementary Site in the 3′UTR of the KIT Oncogene Increases Risk of Acral Melanoma
title_full A Variant in a MicroRNA Complementary Site in the 3′UTR of the KIT Oncogene Increases Risk of Acral Melanoma
title_fullStr A Variant in a MicroRNA Complementary Site in the 3′UTR of the KIT Oncogene Increases Risk of Acral Melanoma
title_full_unstemmed A Variant in a MicroRNA Complementary Site in the 3′UTR of the KIT Oncogene Increases Risk of Acral Melanoma
title_short A Variant in a MicroRNA Complementary Site in the 3′UTR of the KIT Oncogene Increases Risk of Acral Melanoma
title_sort variant in a microrna complementary site in the 3′utr of the kit oncogene increases risk of acral melanoma
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3069149/
https://www.ncbi.nlm.nih.gov/pubmed/21119596
http://dx.doi.org/10.1038/onc.2010.536
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