NOVA1 inhibition by miR-146b-5p in the remnant tissue microenvironment defines occult residual disease after gastric cancer removal

Occult residual disease in remnant tissues could be the cause of tumor relapse. To identify signal molecules and target cells that may be indicative of occult residual disease within a remnant microenvironment, proximal resection margin tissues of gastric cancers were used, as these correspond to th...

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Autores principales: Yoon, Sun Och, Kim, Eun Kyung, Lee, Mira, Jung, Woon Yong, Lee, Hyunjoo, Kang, Youngran, Jang, You-Jin, Hong, Soon Won, Choi, Seung Ho, Yang, Woo Ick
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2015
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4823049/
https://www.ncbi.nlm.nih.gov/pubmed/26673617
http://dx.doi.org/10.18632/oncotarget.6542
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author Yoon, Sun Och
Kim, Eun Kyung
Lee, Mira
Jung, Woon Yong
Lee, Hyunjoo
Kang, Youngran
Jang, You-Jin
Hong, Soon Won
Choi, Seung Ho
Yang, Woo Ick
author_facet Yoon, Sun Och
Kim, Eun Kyung
Lee, Mira
Jung, Woon Yong
Lee, Hyunjoo
Kang, Youngran
Jang, You-Jin
Hong, Soon Won
Choi, Seung Ho
Yang, Woo Ick
author_sort Yoon, Sun Och
collection PubMed
description Occult residual disease in remnant tissues could be the cause of tumor relapse. To identify signal molecules and target cells that may be indicative of occult residual disease within a remnant microenvironment, proximal resection margin tissues of gastric cancers were used, as these correspond to the nearest remnant tissues after gastrectomy. Increased miR-146b-5p in the remnant microenvironment was determined to be a strong risk factor for tumor relapse and poor survival rate. NOVA1, a target gene of miR-146b-5p, was decreased in remnant tissues of patients with a poor prognosis. NOVA1 was enriched in stromal spindle cells such as fibroblasts within normal tissues. In non-neoplastic inflammation, such as gastritis, NOVA1 was highly enriched in T lymphocytes and stromal spindle cells, while expression of this protein was frequently decreased in those types of cells within gastric cancer tissues. Particularly, decreased NOVA1 in T cells within the gastric cancer tissues was correlated with decreased FOXP3-positive regulatory T cells and was associated with poor patient prognosis. In vitro analysis showed that the NOVA1 gene was inhibited by miR-146b-5p. In immune cells as well as stromal spindle cells, decreased NOVA1, possibly inhibited by miR-146b-5p, is a candidate biomarker predicting poor prognosis of gastric cancer patients and is also a biomarker of occult residual disease in remnant tissues after gastric cancer removal.
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spelling pubmed-48230492016-05-03 NOVA1 inhibition by miR-146b-5p in the remnant tissue microenvironment defines occult residual disease after gastric cancer removal Yoon, Sun Och Kim, Eun Kyung Lee, Mira Jung, Woon Yong Lee, Hyunjoo Kang, Youngran Jang, You-Jin Hong, Soon Won Choi, Seung Ho Yang, Woo Ick Oncotarget Research Paper Occult residual disease in remnant tissues could be the cause of tumor relapse. To identify signal molecules and target cells that may be indicative of occult residual disease within a remnant microenvironment, proximal resection margin tissues of gastric cancers were used, as these correspond to the nearest remnant tissues after gastrectomy. Increased miR-146b-5p in the remnant microenvironment was determined to be a strong risk factor for tumor relapse and poor survival rate. NOVA1, a target gene of miR-146b-5p, was decreased in remnant tissues of patients with a poor prognosis. NOVA1 was enriched in stromal spindle cells such as fibroblasts within normal tissues. In non-neoplastic inflammation, such as gastritis, NOVA1 was highly enriched in T lymphocytes and stromal spindle cells, while expression of this protein was frequently decreased in those types of cells within gastric cancer tissues. Particularly, decreased NOVA1 in T cells within the gastric cancer tissues was correlated with decreased FOXP3-positive regulatory T cells and was associated with poor patient prognosis. In vitro analysis showed that the NOVA1 gene was inhibited by miR-146b-5p. In immune cells as well as stromal spindle cells, decreased NOVA1, possibly inhibited by miR-146b-5p, is a candidate biomarker predicting poor prognosis of gastric cancer patients and is also a biomarker of occult residual disease in remnant tissues after gastric cancer removal. Impact Journals LLC 2015-12-09 /pmc/articles/PMC4823049/ /pubmed/26673617 http://dx.doi.org/10.18632/oncotarget.6542 Text en Copyright: © 2016 Yoon et al. http://creativecommons.org/licenses/by/2.5/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Paper
Yoon, Sun Och
Kim, Eun Kyung
Lee, Mira
Jung, Woon Yong
Lee, Hyunjoo
Kang, Youngran
Jang, You-Jin
Hong, Soon Won
Choi, Seung Ho
Yang, Woo Ick
NOVA1 inhibition by miR-146b-5p in the remnant tissue microenvironment defines occult residual disease after gastric cancer removal
title NOVA1 inhibition by miR-146b-5p in the remnant tissue microenvironment defines occult residual disease after gastric cancer removal
title_full NOVA1 inhibition by miR-146b-5p in the remnant tissue microenvironment defines occult residual disease after gastric cancer removal
title_fullStr NOVA1 inhibition by miR-146b-5p in the remnant tissue microenvironment defines occult residual disease after gastric cancer removal
title_full_unstemmed NOVA1 inhibition by miR-146b-5p in the remnant tissue microenvironment defines occult residual disease after gastric cancer removal
title_short NOVA1 inhibition by miR-146b-5p in the remnant tissue microenvironment defines occult residual disease after gastric cancer removal
title_sort nova1 inhibition by mir-146b-5p in the remnant tissue microenvironment defines occult residual disease after gastric cancer removal
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4823049/
https://www.ncbi.nlm.nih.gov/pubmed/26673617
http://dx.doi.org/10.18632/oncotarget.6542
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