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Authors Zhang T, Han Z, Chandoo A, Huang X, Sun X, Ye L, Hu C, Xue X, Huang Y, Shen X, Chang W, Lin X
Received 28 May 2018
Accepted for publication 17 October 2018
Published 18 December 2018 Volume 2019:11 Pages 25—36
DOI https://doi.org/10.2147/CMAR.S175596
Checked for plagiarism Yes
Review by Single-blind
Peer reviewers approved by Dr Amy Norman
Peer reviewer comments 2
Editor who approved publication: Professor Kenan Onel
Background and aim: Periostin
is a protein from the Fascilin family. It is commonly present in normal tissues
and is responsible for cell adhesion. Evidence has emerged showing that changes
in periostin expression play an important role in tumor initiation,
development, and progression. This study aims to investigate the effect of
periostin in gastric cancer (GC) patients who underwent gastrectomy. Seven
hundred and forty-seven GC patients who underwent gastrectomy between December
2006 and July 2011 were included in this study.
Methods: Seven
hundred and forty-seven cancer tissues and 70 paired adjacent normal tissues
were collected. Periostin expression was evaluated by immunohistochemistry. The
Gene Expression Omnibus database was used to study the association between the
mRNA level and patient’s overall survival. The tumor microenvironment was also
studied.
Results: Periostin
expression in stroma was downregulated in tumor tissues but it was upregulated
in the epithelial cells. After dividing the tissues according to the Lauren
Classification, we found that periostin expression in stroma and epithelial
cells was higher in intestinal type than in diffuse type (P <0.001
and P =0.010,
respectively). Periostin was an independent predictor of lymph node (LN)
metastasis in GC patients. The study of CD163(+) tumor-associated macrophages
(TAMs) revealed that in diffuse type GC, periostin expression was associated
with CD163(+) TAMs.
Conclusion: We found
that the periostin expression can predict LN metastasis in patients undergoing
curative gastrectomy. Intestinal type GC patients with high periostin level had
both a favorable survival and lesser LN metastasis.
Keywords: lymph
node metastasis, tumor microenvironment, tissue microarray, cell adhesion,
Lauren Classification
