2014
DOI: 10.1007/s13277-014-2771-6
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MicroRNA-93 suppress colorectal cancer development via Wnt/β-catenin pathway downregulating

Abstract: MicroRNA-93 (miR-93) is involved in several carcinoma progressions. It has been reported that miR-93 acts as a promoter or suppressor in different tumors. However, till now, the role of miR-93 in colon cancer is unclear. Herein, we have found that expression of miR-93 was lower in human colon cancer tissue and colorectal carcinoma cell lines compared with normal colon mucosa. Forced expression of miR-93 in colon cancer cells inhibits colon cancer invasion, migration, and proliferation. Furthermore, miR-93 may … Show more

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Cited by 85 publications
(68 citation statements)
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“…The prognosis of CRC largely results from the presence of distal metastases or not, since in situ cancer and cancer with invasion of lymph nodes are both highly treatable [1][2][3]. However, distal metastases of CRC to the liver, lungs, or other organs cause difficulties for treatments, leading to poor therapeutic outcome [4][5][6][7].…”
Section: Introductionmentioning
confidence: 99%
“…The prognosis of CRC largely results from the presence of distal metastases or not, since in situ cancer and cancer with invasion of lymph nodes are both highly treatable [1][2][3]. However, distal metastases of CRC to the liver, lungs, or other organs cause difficulties for treatments, leading to poor therapeutic outcome [4][5][6][7].…”
Section: Introductionmentioning
confidence: 99%
“…*P < 0.05 vs. sham group; # P < 0.05 vs. I/R + miR control group Until now, studies of miR-93 have been focused mainly on its involvement in many types of human cancers, such as glioblastoma, gastric cancer, breast carcinoma, and others. miR-93 is overexpressed in a number of types of human cancers and functions as an oncogene by targeting important cancer-related genes [25][26][27][28][29], whereas, in some types of cancers miR-93 was down-regulated and repressed proliferation paradoxically [30,31]. However, the present study is the first to investigate its role in ischemia-induced cerebral injury.…”
Section: Mir-93 Antagomir Induced Ho-1 Expression Through Nrf2mentioning
confidence: 66%
“…Member(s) of the hsa-miR-18114 and hsa-miR-29 families15 exhibit both anticancer and pro-cancer regulation under different clinical conditions, while members of hsa-miR-12616, hsa-miR-12917, hsa-miR-13618, hsa-miR-20419, hsa-miR-66320, hsa-miR-9921, hsa-miR-37822, hsa-miR-9223, and hsa-miR-40924 families are recognized as having anticancer properties under different clinical conditions. Families that contained at least one miRNA found in hAMSC-CM-derived exosomes reportedly exhibit antagonistic roles in numerous cancer types and include hsa-miR-48625, hsa-miR-10026, hsa-miR-10127, hsa-miR-12428, hsa-miR-128529, hsa-miR-13430, hsa-miR-13831, hsa-miR-13932, hsa-miR-14333, hsa-miR-18634, hsa-miR-19335, hsa-miR-20536, hsa-miR-22237, hsa-miR-33838, hsa-miR-33939, hsa-miR-42440, hsa-miR-12741, hsa-miR-2642, hsa-miR-10343, hsa-miR-10744, hsa-miR-12845, hsa-miR-14046, hsa-miR-14447, hsa-miR-15348, hsa-miR-19249, hsa-miR-21250, hsa-miR-21851, hsa-miR-2352, hsa-miR-2553, hsa-miR-37054, hsa-miR-37555, hsa-miR-38156, hsa-miR-41057, hsa-miR-4158, and hsa-miR-9359. These NGS data revealed an enriched miRNA population in hAMSC-CM-derived exosomes that are likely involved in the regulation of different types of cancer.…”
Section: Resultsmentioning
confidence: 99%
“…Exceptionally, hAMSC-CM derived exosomal miRNAs demonstrated outstanding diversity, which encompasses numerous anti-cancer miRNAs891011121314151617181920212223242526272829303132333435363738394041424344454647484950515253545556575859, as well as new and poorly investigated miRNAs. In contrast, miRNAs, which are frequently detected in different cancers exosomes (include hsa-miR-105, hsa-miR-214, hsa-miR-92, hsa-miR-21, hsa-miR-29, hsa-miR-9, hsa-miR-222)6364, were either absent or showed very nominal expression in hAMSC-CM derived exosomes.…”
Section: Discussionmentioning
confidence: 99%