Dysregulated microRNA expression profiles in gastric cancer cells with high peritoneal metastatic potential

Yi, Feng; Bai, Feihu; You, Yanjie; Bai, Fangyun; Wu, Chuanxia; Xin, Ruijuan; Li, Xue; Nie, Yongzhan

doi:10.3892/etm.2018.6783

Cited by 11 publications

(14 citation statements)

References 32 publications

(19 reference statements)

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“…Cluster-2 included 2 miRNAs, miR-221-3p and miR-222-3p, which were both downregulated in UM patients with metastasis. In a recent study, miR-221-3p and miR-222-3p were also downregulated in gastric cancer cells with high metastatic potential [18].…”

Section: Figure 3: Boxplots Showing the Distribution Of The Mirna Expmentioning

confidence: 92%

“…miRNAs typically regulate Research Paper gene expression by altering mRNA stability or repressing translation of mRNA to protein. Several miRNAs play an important role (tumor suppressors or tumor promoters) in cancer development and progression including metastasis [15][16][17][18][19][20]. However, data are limited regarding the role of miRNAs in metastatic UM [21][22][23].…”

Section: Introductionmentioning

confidence: 99%

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Changes in microRNA expression associated with metastasis and survival in patients with uveal melanoma

2020

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Uveal melanoma (UM) is a major intraocular cancer that is molecularly distinct from cutaneous melanoma. Approximately half of patients with UM eventually develop metastasis. The prognosis of metastatic UM is poor, with a median overall survival (OS) of less than a year. In this study, we sought to identify microRNAs (miRNAs) associated with metastasis and OS in UM. We analyzed the miRNA expression and clinical outcomes data from The Cancer Genome Atlas (TCGA) dataset for UM. Differential expression analyses were conducted for each miRNA with respect everdevelopment of metastasis. Multiple survival analyses were done, using the Cox proportional hazards model, to evaluate interactions between miRNA expression, metastasis, and OS. A total of 22 miRNAs (3 upregulated and 19 downregulated) were differentially expressed between patients with vs. without metastatic UM. These 22 miRNAs could be grouped into four clusters based on similarities in expression patterns. Of the 22 miRNAs differentially expressed with respect to metastasis, 21 were significantly associated with OS. The expression of multiple miRNAs was significantly associated with metastasis and overall survival in patients with UM. Further investigation of these miRNAs as biomarkers and/or therapeutic targets is warranted in the push to improve outcomes for patients with metastatic UM.

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Section: Figure 3: Boxplots Showing the Distribution Of The Mirna Expmentioning

confidence: 92%

Section: Introductionmentioning

confidence: 99%

Changes in microRNA expression associated with metastasis and survival in patients with uveal melanoma

2020

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“…1 It is reported that abnormal expression of miRNA is associated with tumorigenesis. [1][2][3] Some miRNA molecules can induce tumorigenesis and promote tumor progression as tumor promoters; on the other hand, some miRNA molecules act as tumor suppressors and inhibit the growth of tumor cells or induce their apoptosis. Therefore, miRNA molecules are considered as novel tumor markers and can be used in the diagnosis, treatment and prognosis prediction of tumors.…”

Section: Introductionmentioning

confidence: 99%

<p>MicroRNA-497-5p Induces Cell Cycle Arrest Of Cervical Cancer Cells In S Phase By Targeting CBX4</p>

Chen

Wang

et al. 2019

OTT

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miR-497-5p can inhibit cervical cancer cell proliferation. However, the underlying mechanism remains to be elucidated. Methods: Bioinformatics was used to analyze the target genes of miR-497-5p. qRT-PCR and Western blot were used to analyze mRNA and protein expression, respectively. Dualluciferase reporter assay was used to analyze the direct binding between miR-497-5p and 3ʹ-untranslated region of CBX4. Cell viability was measured with MTT assay. Flow cytometry was performed to detect cell cycle distribution. Results: Here, using bioinformatics methods we firstly found that miR-497-5p regulated cervical carcinoma proliferation by targeting polycomb chromobox4 (CBX4). Expression of miR-497-5p in cervical carcinoma tissues was negatively correlated with CBX4. A binding region of miR-497-5p in 3ʹ-untranslated region of CBX4 was predicted. Further experiments confirmed that miR-497-5p directly targeted CBX4. Besides, RNA interference of CBX4 inhibited cervical cancer cell proliferation, arrested cells at S phase and reduced the expression of CDK2 and Cyclin A2 proteins. The use of miR-497-5p inhibitor compromised CBX4 interference RNAs induced cycle arrest of cervical cancer cells. Cells co-transfected with miR-497-5p inhibitors and CBX4 interference RNAs had a higher proliferation rate than CBX4 inference RNA-transfected cells. Conclusion: All together, the present study demonstrates that miR-497-5p inhibits cervical cancer cells proliferation by directly targeting CBX4.

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“…All differentially expressed miRNAs are listed according to tumor type in Supporting Table 4. [24][25][26][27][28][29][30][31][32][33][34][35][36][37] Investigation of these miRNAs within published data indicates their role in oncogenesis. 2A) We performed pathway analysis to determine the clinical significance and biologic functions of the differentially expressed miRNAs for each cancer type.…”

Section: Mirna Analysismentioning

confidence: 99%

“…AA miRNA expression data on TNBC were associated with an increase in the angiogenesis pathway, whereas miRNA expression data from AAs with non-TNBC tumor types were associated with a decrease in the angiogenesis pathway ( Table 2). In addition, all UCECs with dysregulated miRNA expression were of the EEA subtype; therefore, 25 Zhang 2017, 26 Sueta 2017 29 Shi 2017, 30 Meijer 2018 36 Duan 2016 37 Abbreviations: AA, African American; BRCA, breast cancer; KIRC, kidney renal clear cell carcinoma; miR, microRNA; NSCLC, non-small-cell lung cancer; PRAD, prostate adenocarcinoma; THCA, thyroid carcinoma; UCEC, uterine corpus endometrial carcinoma.…”

Section: Tumor Subtypingmentioning

confidence: 99%

Pan‐cancer clinical and molecular analysis of racial disparities

Lara

Wang

Asare

et al. 2019

Cancer

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Background Racial disparities in cancer outcomes are increasingly recognized, but comprehensive analyses, including molecular studies, are limited. The objective of the current study was to perform a pan‐cancer clinical and epigenetic molecular analysis of outcomes in African American (AA) and European American (EA) patients. Methods Cross‐platform analyses using cancer databases (the Surveillance, Epidemiology, and End Results program database and the National Cancer Data Base) and a molecular database (The Cancer Genome Ancestry Atlas) were performed to evaluate clinical and epigenetic molecular differences between AA and EA patients based on genetic ancestry. Results In the primary pan‐cancer survival analysis using the Surveillance, Epidemiology, and End Results database (2,045,839 patients; 87.5% EA and 12.5% AA), AA patients had higher mortality rates for 28 of 42 cancer types analyzed (hazard ratio, >1.0). AAs continued to have higher mortality in 13 cancer types after adjustment for socioeconomic variables using the National Cancer Database (5,150,023 patients; 11.6% AA and 88.4% EA). Then, molecular features of 5,283 tumors were analyzed in patients who had genetic ancestry data available (87.2% EA and 12.8% AA). Genes were identified with altered DNA methylation along with increased microRNA expression levels unique to AA patients that are associated with cancer drug resistance. Increased miRNAs (miR‐15a, miR‐17, miR‐130‐3p, miR‐181a) were noted in common among AAs with breast, kidney, thyroid, or prostate carcinomas. Conclusions The current results identified epigenetic features in AA patients who have cancer that may contribute to higher mortality rates compared with EA patients who have cancer. Therefore, a focus on molecular signatures unique to AAs may identify actionable molecular abnormalities.

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Dysregulated microRNA expression profiles in gastric cancer cells with high peritoneal metastatic potential

Cited by 11 publications

References 32 publications

Changes in microRNA expression associated with metastasis and survival in patients with uveal melanoma

Changes in microRNA expression associated with metastasis and survival in patients with uveal melanoma

<p>MicroRNA-497-5p Induces Cell Cycle Arrest Of Cervical Cancer Cells In S Phase By Targeting CBX4</p>

Pan‐cancer clinical and molecular analysis of racial disparities

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