Gene expression analyses determine two different subpopulations in KIT-negative GIST-like (KNGL) patients
Author
Moura, David S.; Ramos, Rafael; Fernández-Serra, Antonio; Serrano, Teresa; Cruz, Julia; Álvarez-Alegret, Ramiro; Ortiz-Durán, Rosa; Vicioso, Luis; Gómez-Dorronsoro, María Luisa; Garcia del Muro, Xavier; Martínez-Trufero, Javier; Rubio-Casadevall, Jordi; Sevilla, Isabel; Laínez, Nuria; Gutiérrez, Antonio; Serrano, César; López-Álvarez, María; Hindi, Nadia; Tarón, Miguel; López Guerrero, José Antonio
Entity
UAM. Departamento de Biología MolecularPublisher
Impact JournalsDate
2018-04-03Citation
10.18632/oncotarget.24799
Oncotarget 9.25 (2018): 17576-17588
ISSN
1949-2553DOI
10.18632/oncotarget.24799Funded by
The project was funded by the Instituto de Salud Carlos III (ISCIII) - Fondo Europeo de Desarrollo Regional (FEDER), through a public competitive call (project reference PI15/01254; principal Investigator Javier Martín Broto), and the Spanish Group for Research on Sarcoma (GEIS)Project
Gobierno de España. PI15/01254Editor's Version
https://doi.org/10.18632/oncotarget.24799Subjects
KNGL; miRNA221/222 cluster; KIT; DOG1; IGF1R; Biología y Biomedicina / BiologíaRights
© 2018 Moura et al.Abstract
Introduction: There are limited findings available on KIT-negative GIST-like
(KNGL) population. Also, KIT expression may be post-transcriptionally regulated
by miRNA221 and miRNA222. Hence, the aim of this study is to characterize KNGL
population, by differential gene expression, and to analyze miRNA221/222 expression
and their prognostic value in KNGL patients.
Methods: KIT, PDGFRA, DOG1, IGF1R, MIR221 and MIR222 expression levels
were determined by qRT-PCR. We also analyzed KIT and PDGFRA mutations, DOG1
expression, by immunohistochemistry, along with clinical and pathological data.
Disease-free survival (DFS) and overall survival (OS) differences were calculated
using Log-rank test.
Results: Hierarchical cluster analyses from gene expression data identified
two groups: group I had KIT, DOG1 and PDGFRA overexpression and IGF1R
underexpression and group II had overexpression of IGF1R and low expression of
KIT, DOG1 and PDGFRA. Group II had a significant worse OS (p = 0.013) in all the
series, and showed a tendency for worse OS (p = 0.11), when analyzed only the
localized cases. MiRNA222 expression was significantly lower in a control subset of
KIT-positive GIST (p < 0.001). OS was significantly worse in KNGL cases with higher
expression of MIR221 (p = 0.028) or MIR222 (p = 0.014).
Conclusions: We identified two distinct KNGL subsets, with a different prognostic
value. Increased levels of miRNA221/222, which are associated with worse OS, could
explain the absence of KIT protein expression of most KNGL tumors
Files in this item
Google Scholar:Moura, David S.
-
Ramos, Rafael
-
Fernández-Serra, Antonio
-
Serrano, Teresa
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Cruz, Julia
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Álvarez-Alegret, Ramiro
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Ortiz-Durán, Rosa
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Vicioso, Luis
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Gómez-Dorronsoro, María Luisa
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Garcia del Muro, Xavier
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Martínez-Trufero, Javier
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Rubio-Casadevall, Jordi
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Sevilla, Isabel
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Laínez, Nuria
-
Gutiérrez, Antonio
-
Serrano, César
-
López-Álvarez, María
-
Hindi, Nadia
-
Tarón, Miguel
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López Guerrero, José Antonio
-
Martín-Broto, Javier
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