Up-regulation of miR-224 promotes cancer cell proliferation and invasion and predicts relapse of colorectal cancer

Zhang, Guangjun; Zhou, He; Xiao, Hua-xu; Yu, Li; Zhou, Tong

doi:10.1186/1475-2867-13-104

Cited by 53 publications

(42 citation statements)

References 31 publications

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“…Smad4 contains two miR-224-binding sites in the 3′untranslated region and acts as a tumor suppressor role [21]. It was also reported that miR-224 acts as an oncogenic role in the cellular processes by targeting Smad4 in CRC [22]. The ectopic expressions of miRNAs may act as oncogenes which are closely related to the cancer development, and different signatures of miRNA expression distinguish the cancer cells from the normal ones [23].…”

Section: Mir-224 In Tumorigenesismentioning

confidence: 96%

MicroRNA-224: as a potential target for miR-based therapy of cancer

et al. 2015

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MicroRNAs (miRNAs) are small noncoding RNA molecules which regulate the target gene expression posttranscriptionally. Increasing studies have shown that microRNAs play important roles in multiple biological pathways. For instance, aberrant expression of microRNA-224 (miR-224) plays a vital role in tumor biology in various types of human cancer. Here, we aim to summarize the molecular mechanisms that lead to the overexpression of miR-224 in cancers, analyze the effect of miR-224 on tumor biology, and reveal the clinical significance of miR-224. MiR-224 regulates its targets by modulating messenger RNA (mRNA) stability and/or protein translation, and it would provide new insight into molecular targeting cancer treatment.

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Section: Mir-224 In Tumorigenesismentioning

confidence: 96%

MicroRNA-224: as a potential target for miR-based therapy of cancer

et al. 2015

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“…In terms of CRC, abnormal expression of several miRs such as miR-27b, miR-133b, miR-124 have been reported (Ye et al, 2013;Zhang et al, 2013b;Xiang and Li, 2014). Additionally, Zhang et al (2013a) found that ectopic expression of miR-224 promoted CRC tumor cell proliferation, migration, and invasion in vitro. Zheng et al (2014) indicated that downregulation of miR-132 in CRC was associated with tumor size, distant metastasis, and TNM stage.…”

Section: Introductionmentioning

confidence: 99%

Decreased expression of miR-874 and its tumor suppressive function in human colorectal cancer

Wang¹,

Xia²,

Bi³

2016

Genet. Mol. Res.

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ABSTRACT. Dysregulation of miRNAs is associated with cancer development and progression. For example, aberrant expression of miR-874 has been found in some types of cancer. However, miR-874 expression and its clinical significance in colorectal cancer (CRC) have not yet been explored. The aim of the current study was to explore the effects of miR-874 in CRC tumorigenesis and development. Quantitative reverse-transcription PCR was performed to evaluate miR-874 levels in CRC cell lines and in 135 pairs of primary human CRC specimens and adjacent noncancerous tissues. The association of miR-874 expression with clinicopathological factors and prognosis was also analyzed. Furthermore, the effects of miR-874 on the biological behavior of CRC cells in vitro were investigated. Our results revealed that miR-874 expression was significantly downregulated in CRC cancer tissues and cell lines. Decreased miR-874 expression was significantly associated with larger tumor size, deeper invasion depth, and advanced TNM stage in vivo. Additionally, low miR-874 expression in CRC was an independent predictor of poor survival. Moreover, overexpression of miR-874 inhibited cell proliferation, invasion, and migration, and promoted cell apoptosis of the SW620 CRC cell line in vitro. Taken together, these findings indicate that miR-874 may act as a tumor suppressor in CRC, and may serve as a novel therapeutic target for miR-based therapy.

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“…MiR-135a, b target APC gene to induce cell cycle progression and stimulate cell proliferation [48]. Zhang et al [49] reported that oncogenic miR-224 was significantly upregulated in CRC tissues and its overexpression in SW 480 cells promoted their proliferation. A tumor suppressor miR-185 (downregulated) inhibits division of CRC cells by targeting genes, RHOA (Ras Homolog Family Member A) and CDC42, involved in cell cycle progression; however, this mechanism appears to be cell-type specific [50].…”

Section: Mirna In the Pathogenesis Of Crcmentioning

confidence: 99%

“…Some of the upregulated miRNAs in CRC and their target genes miR-135/b APC Wnt-signaling pathway [54,95] miR-27 APC Promotes growth and metastasis [85] miR-221 RECK Stimulates invasion and metastasis [99] miR-210 RBM3 Promotes Angiogenesis [83,84] miR-21 CDC25A Cell cycle regulation [45] miR-31 RASA1 Promotes cell proliferation [47] miR-182 and miR-503 FBXW7 Tumor growth and progression [59] miR-200c ZEB1 and ZEB2 Metastasis [71] miR-224 PHLPP1, PHLPP1 Proliferation [49] miR-301a TGFBR2 Proliferation, migration [61] Some of downregulated miRNAs in CRC and their target genes miR-34a FRA-1 Invasion, migration [60] miR-137 Cdc-42,LSD-1 Tumor growth [133] miR-141 SIP1 Inhibits cell invasion and migration [134] miR-149 FOXM1 Proliferation, migration [62] miR-185 RHOA Cell cycle progression [50] miR-195 CARMA3 Promotes apoptosis [52] miR-215 TYMS,DTL Cell migration and proliferation [135] miR-330 CDC42 Cell proliferation [51] miR-339 --5p MDM2 Invasion, migration [64] miR-375 YAP1 Apoptosis [30] miR-455 RAF1 Proliferation [29] proliferation by targeting CARMA3 (Caspase Recruitment Domain Family, Member) and an inverse correlation is noted between miR-195 expression and CARMA3 protein expression [52].…”

Section: Identified Mirnamentioning

confidence: 99%