Lgr5 High /Dclk1 High Phenotype Is More Common in Early Stage and Intestinal Subtypes of Gastric Carcinomas

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Lgr5 High /Dclk1 High Phenotype Is More Common in Early Stage and Intestinal Subtypes of Gastric Carcinomas Publisher Pubmed

Kalantari E¹ ; Asadi Lari MH^{1, 2} ; Roudi R¹ ; Korourian A³ ; Madjd Z^{1, 3}

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1. Oncopathology Research Center, Iran University of Medical Sciences, Hemmat Street (Highway), Next to Milad Tower, Tehran, 14496-14530, Iran
2. Department of Cellular and Physiological Sciences, Faculty of Medicine, University of British Columbia, Vancouver, BC, Canada
3. Department of Molecular Medicine, Faculty of Advanced Technologies in Medicine, Iran University of Medical Sciences, Tehran, Iran

Source: Cancer Biomarkers Published:2017

Abstract

BACKGROUND: Gastric carcinoma is the third most common malignancy and is one of the main causes of cancer deaths worldwide. Cancer stem cells (CSCs) are a subpopulation of tumour cells capable of self-renewal and differentiation, likely responsible for the initiation, recurrence, metastasis and chemo/radio-resistance. OBJECTIVE: This study was conducted to evaluate the expression patterns and clinicopathologic significance of putative CSC markers, Lgr5 and DCLK1, in gastric carcinoma. METHOD: The expression levels of Lgr5 and DCLK1 were examined in a well-defined series of gastric carcinoma tissues, including 75 (80%) from intestinal and 19 (20%) from diffuse subtypes, using tissue microarray (TMA). In addition, the correlation of the expression of these markers with clinicopathological factors was explored. RESULTS: Higher expressions of Lgr5 and DCLK1 were mainly detected in intestinal subtypes of gastric carcinomas compared to diffuse subtypes (P= 0.005 and P= 0.050, respectively). We also found a higher expression of Lgr5 and DCLK1 more frequently in well-differentiated gastric carcinoma cases (P< 0.001 and P= 0.007). The combined analysis demonstrated that the co-expression of Lgr5 and DCLK1 (Lgr5High/DCLK1High) was more common in intestinal subtypes (P= 0.025) and well-differentiated gastric carcinoma samples (P< 0.001). Interestingly, there was a significant correlation between Lgr5High/DCLK1High phenotype and early-stage gastric carcinoma specimens (P= 0.045). CONCLUSION: Our findings indicated that the Lgr5High/DCLK1High expression pattern may be considered as a signature phenotype for intestinal subtypes of gastric carcinoma. © 2017 - IOS Press and the authors. All rights reserved.

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Style	Citing Format
MLA	Kalantari E, et al.. "Lgr5 High /Dclk1 High Phenotype Is More Common in Early Stage and Intestinal Subtypes of Gastric Carcinomas." Cancer Biomarkers, vol. 20, no. 4, 2017, pp. 563-573.
APA	Kalantari E, Asadi Lari MH, Roudi R, Korourian A, Madjd Z (2017). Lgr5 High /Dclk1 High Phenotype Is More Common in Early Stage and Intestinal Subtypes of Gastric Carcinomas. Cancer Biomarkers, 20(4), 563-573.
Chicago	Kalantari E, Asadi Lari MH, Roudi R, Korourian A, Madjd Z. "Lgr5 High /Dclk1 High Phenotype Is More Common in Early Stage and Intestinal Subtypes of Gastric Carcinomas." Cancer Biomarkers 20, no. 4 (2017): 563-573.
Harvard	Kalantari E et al. (2017) 'Lgr5 High /Dclk1 High Phenotype Is More Common in Early Stage and Intestinal Subtypes of Gastric Carcinomas', Cancer Biomarkers, 20(4), pp. 563-573.
Vancouver	Kalantari E, Asadi Lari MH, Roudi R, Korourian A, Madjd Z. Lgr5 High /Dclk1 High Phenotype Is More Common in Early Stage and Intestinal Subtypes of Gastric Carcinomas. Cancer Biomarkers. 2017;20(4):563-573.
BibTex	@article{ author = {Kalantari E and Asadi Lari MH and Roudi R and Korourian A and Madjd Z}, title = {Lgr5 High /Dclk1 High Phenotype Is More Common in Early Stage and Intestinal Subtypes of Gastric Carcinomas}, journal = {Cancer Biomarkers}, volume = {20}, number = {4}, pages = {563-573}, year = {2017} }
RIS	TY - JOUR AU - Kalantari E AU - Asadi Lari MH AU - Roudi R AU - Korourian A AU - Madjd Z TI - Lgr5 High /Dclk1 High Phenotype Is More Common in Early Stage and Intestinal Subtypes of Gastric Carcinomas JO - Cancer Biomarkers VL - 20 IS - 4 SP - 563 EP - 573 PY - 2017 ER -

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