The Clinicopathological Significance of miR-133a in Colorectal Cancer

This study determined the expression of microRNA-133a (MiR-133a) in colorectal cancer (CRC) and adjacent normal mucosa samples and evaluated its clinicopathological role in CRC. The expression of miR-133a in 125 pairs of tissue samples was analyzed by quantitative real-time polymerase chain reaction...

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Veröffentlicht in:Disease markers 2014-01, Vol.2014 (2014), p.1-8
Hauptverfasser: Ng, Lui, Lam, Colin Siu-Chi, Wan, Timothy Ming-Hun, Chow, Ariel Ka-Man, Wong, Sunny Kit-Man, Li, Hung-Sing, Man, Johnny Hon-Wai, Lo, Oswens Siu-Hung, Foo, Dominic, Cheung, Alvin, Yau, Thomas, Poon, Jensen Tung-Chung, Poon, Ronnie Tung-Ping, Law, Wai-Lun, Pang, Roberta Wen-Chi
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Sprache:eng
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Zusammenfassung:This study determined the expression of microRNA-133a (MiR-133a) in colorectal cancer (CRC) and adjacent normal mucosa samples and evaluated its clinicopathological role in CRC. The expression of miR-133a in 125 pairs of tissue samples was analyzed by quantitative real-time polymerase chain reaction (qRT-PCR) and correlated with patient’s clinicopathological data by statistical analysis. Endogenous expression levels of several potential target genes were determined by qRT-PCR and correlated using Pearson’s method. MiR-133a was downregulated in 83.2% of tumors compared to normal mucosal tissue. Higher miR-133a expression in tumor tissues was associated with development of distant metastasis, advanced Dukes and TNM staging, and poor survival. The unfavorable prognosis of higher miR-133a expression was accompanied by dysregulation of potential miR-133a target genes, LIM and SH3 domain protein 1 (LASP1), Caveolin-1 (CAV1), and Fascin-1 (FSCN1). LASP1 was found to possess a negative correlation (γ=-0.23), whereas CAV1 exhibited a significant positive correlation (γ=0.27), and a stronger correlation was found in patients who developed distant metastases (γ=0.42). In addition, a negative correlation of FSCN1 was only found in nonmetastatic patients. In conclusion, miR-133a was downregulated in CRC tissues, but its higher expression correlated with adverse clinical characteristics and poor prognosis.
ISSN:0278-0240
1875-8630
DOI:10.1155/2014/919283