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Identification of mutations in the PYRIN-containing NLR genes (NLRP) in head and neck squamous cell carcinoma
Authors
A Mashberg
Ann Marie Egloff
+43 more
BK Davis
BW Neville
CB Moore
D Hanahan
E Elinav
E Meyer
E White
EA Collisson
GY Chen
HS van Monsjou
IC Allen
IC Allen
J Ahn
J Ferlay
Jennifer R. Grandis
JH Meurman
JP Ting
JP Ting
JP Ting
KK Ang
KV Woods
M Lamkanfi
MA O'Rorke
MH Zaki
MH Zaki
MH Zaki
MS Meyer
Muy-Teck Teh
N Agrawal
N Jounai
N Stransky
R Cooney
R Pries
R Slim
S Nik-Zainal
S Nik-Zainal
S Normand
T Strowig
V Brailo
Vivian W. Y. Lui
Y Lei
Y Lei
Yu Lei
Publication date
1 January 2014
Publisher
'Public Library of Science (PLoS)'
Doi
View
on
PubMed
Abstract
Head and Neck Squamous Cell Carcinoma (HNSCC) encompasses malignancies that arise in the mucosa of the upper aerodigestive tract. Recent high throughput DNA sequencing revealed HNSCC genes mutations that contribute to several cancer cell characteristics, including dysregulation of cell proliferation and death, intracellular proinflammatory signaling, and autophagy. The PYRIN-domain containing NLR (Nucleotide-binding domain, Leucine rich Repeats - containing) proteins have recently emerged as pivotal modulators of cell death, autophagy, inflammation, and metabolism. Their close physiologic association with cancer development prompted us to determine whether mutations within the NLRP (PYRIN-containing NLR ) gene family were associated with HNSCC genome instability and their clinicopathologic correlations. Catastrophic mutational events underlie cancer cell genome instability and mark a point-of-no-return in cancer cell development and generation of heterogeneity. The mutation profiles of 62 patients with primary conventional type HNSCC excluding other histologic variants were analyzed. Associations were tested using Fisher's Exact test or Mann-Whitney U test. Mutations in NLRP were associated with elevated genome instability as characterized by higher mutation rates. Clinically, NLRP mutations were more frequently found in HNSCC arising in the floor of mouth (50.0%) in comparison with HNSCC at other head and neck locations (14.8%). These mutations were clustered at the leucine rich repeats region of NLRP proteins, and affected NLRP genes were mostly localized at chromosomes 11p15.4 and 19q13.42-19q13.43. Twenty novel NLRP mutations were identified in HNSCC, and mutations in this group of genes were correlated with increased cancer cell genome mutation rates, and such features could be a potential molecular biomarker of HNSCC genome instability. © 2014 Lei et al
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