Copy number loss of the interferon gene cluster in melanomas is linked to reduced T cell infiltrate and poor patient prognosis.

Copy number loss of the interferon gene cluster in melanomas is linked to reduced T cell infiltrate and poor patient prognosis.

While immunotherapies are rapidly becoming mainstays of cancer treatment, significant gaps remain in our understanding of how to optimally target them, alone or in combination. Here we describe a novel method to monitor levels of immune cells and pathways in expression data from solid tumors using p...

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Main Authors: Peter S Linsley, Cate Speake, Elizabeth Whalen, Damien Chaussabel
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2014-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC4196925?pdf=render
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spelling doaj-6cd845de85f24419ad969caf119d46952020-11-25T02:33:49ZengPublic Library of Science (PLoS)PLoS ONE1932-62032014-01-01910e10976010.1371/journal.pone.0109760Copy number loss of the interferon gene cluster in melanomas is linked to reduced T cell infiltrate and poor patient prognosis.Peter S LinsleyCate SpeakeElizabeth WhalenDamien ChaussabelWhile immunotherapies are rapidly becoming mainstays of cancer treatment, significant gaps remain in our understanding of how to optimally target them, alone or in combination. Here we describe a novel method to monitor levels of immune cells and pathways in expression data from solid tumors using pre-defined groups or modules of co-regulated immune genes. We show that expression of an interconnected sub-network of type I interferon-stimulated genes (ISGs) in melanomas at the time of diagnosis significantly predicted patient survival, as did, to a lesser extent, sub-networks of T helper/T regulatory and NK/T Cytotoxic cell genes. As a group, poor prognosis tumors with reduced ISG and immune gene levels exhibited significant copy number loss of the interferon gene cluster located at chromosome 9p21.3. Our studies demonstrate a link between type I interferon action and immune cell levels in melanomas, and suggest that therapeutic approaches augmenting both activities may be most beneficial.http://europepmc.org/articles/PMC4196925?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Peter S Linsley
Cate Speake
Elizabeth Whalen
Damien Chaussabel
spellingShingle Peter S Linsley
Cate Speake
Elizabeth Whalen
Damien Chaussabel
Copy number loss of the interferon gene cluster in melanomas is linked to reduced T cell infiltrate and poor patient prognosis.
PLoS ONE
author_facet Peter S Linsley
Cate Speake
Elizabeth Whalen
Damien Chaussabel
author_sort Peter S Linsley
title Copy number loss of the interferon gene cluster in melanomas is linked to reduced T cell infiltrate and poor patient prognosis.
title_short Copy number loss of the interferon gene cluster in melanomas is linked to reduced T cell infiltrate and poor patient prognosis.
title_full Copy number loss of the interferon gene cluster in melanomas is linked to reduced T cell infiltrate and poor patient prognosis.
title_fullStr Copy number loss of the interferon gene cluster in melanomas is linked to reduced T cell infiltrate and poor patient prognosis.
title_full_unstemmed Copy number loss of the interferon gene cluster in melanomas is linked to reduced T cell infiltrate and poor patient prognosis.
title_sort copy number loss of the interferon gene cluster in melanomas is linked to reduced t cell infiltrate and poor patient prognosis.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2014-01-01
description While immunotherapies are rapidly becoming mainstays of cancer treatment, significant gaps remain in our understanding of how to optimally target them, alone or in combination. Here we describe a novel method to monitor levels of immune cells and pathways in expression data from solid tumors using pre-defined groups or modules of co-regulated immune genes. We show that expression of an interconnected sub-network of type I interferon-stimulated genes (ISGs) in melanomas at the time of diagnosis significantly predicted patient survival, as did, to a lesser extent, sub-networks of T helper/T regulatory and NK/T Cytotoxic cell genes. As a group, poor prognosis tumors with reduced ISG and immune gene levels exhibited significant copy number loss of the interferon gene cluster located at chromosome 9p21.3. Our studies demonstrate a link between type I interferon action and immune cell levels in melanomas, and suggest that therapeutic approaches augmenting both activities may be most beneficial.
url http://europepmc.org/articles/PMC4196925?pdf=render
work_keys_str_mv AT peterslinsley copynumberlossoftheinterferongeneclusterinmelanomasislinkedtoreducedtcellinfiltrateandpoorpatientprognosis
AT catespeake copynumberlossoftheinterferongeneclusterinmelanomasislinkedtoreducedtcellinfiltrateandpoorpatientprognosis
AT elizabethwhalen copynumberlossoftheinterferongeneclusterinmelanomasislinkedtoreducedtcellinfiltrateandpoorpatientprognosis
AT damienchaussabel copynumberlossoftheinterferongeneclusterinmelanomasislinkedtoreducedtcellinfiltrateandpoorpatientprognosis
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