CCL19 suppresses angiogenesis through promoting miR-206 and inhibiting Met/ERK/Elk-1/HIF-1α/VEGF-A pathway in colorectal cancer

Xu, Zhuoqing; Zhu, Congcong; Chen, Chun; Zong, Yaping; Feng, Hao; Liu, Di; Feng, Wenqing; Zhao, Jingkun; Liu, Aiguo

doi:10.1038/s41419-018-1010-2

Cited by 121 publications

(101 citation statements)

References 50 publications

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“…Our results revealed that cell lines transfected with miR-206 mimics experienced a significant down regulation of VEGF. Similar behavior has been reported previously in renal carcinoma [32], colorectal [33] and lung cancers [34]. These key findings indicate that miR-206 can suppress VEGF-mediated invasion and angiogenesis in TNBC.…”

Section: Discussionsupporting

confidence: 89%

VEGF and KRAS are Potential Targets of miR-206 Modulation in Triple Negative Breast Cancer

Feky¹,

Ibrahim²,

Nassar³

et al. 2019

JCRT

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Triple negative is a subtype of breast cancer characterized by lack of expression of hormone receptors (ER, PR and Her2/neu). Due to the limited treatment options, the search for novel treatment targets continues. The aim of this study was to assess the differential expression of miR-206, VEGF and KRAS in TNBC and non-TNBC tissues and cell lines and to evaluate the modulatory effect of miR-206 on the key oncogenic targets VEGF and KRAS. The expression of miR-206, VEGF and KRAS was quantified using real time PCR in both paraffin embedded breast cancer and adjacent tissues as well as in MDA-MB-231 and MCF-7 cell lines. Cell lines were transfected with different concentrations of miR-206 mimic and their viability were assessed using MTT assay. Our results indicated that miR-206 was significantly downregulated in cancerous compared to non-cancerous tissues with a more pronounced downregulation in TNBC than non-TNBC tissues. VEGF and KRAS were significantly upregulated in TNBC compared to non-TNBC and their expression was negatively correlated to miR-206 expression. Transfection of TNBC and non-TNBC cell lines with miR-206 mimic resulted in a dose dependent reduction in cell viability as well as a significant reduction in VEGF and KRAS expression. In conclusion, based on our combined human tissues and cell line-based investigations we can suggest that VEGF and KRAS may be potential targets for miR-206-mediated regulation and that their targeting by miR-206 can be a highly efficient therapeutic strategy in TNBC.

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Section: Discussionsupporting

confidence: 89%

VEGF and KRAS are Potential Targets of miR-206 Modulation in Triple Negative Breast Cancer

Feky¹,

Ibrahim²,

Nassar³

et al. 2019

JCRT

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“…19,31 Inhibition of MET gene expression by miR-206 has been suggested to limit the development of various types of cancers. 9,11,[31][32][33][34][35] We found that miR-206 mimic transfection signicantly reduced c-Met protein level in patient-derived HCC cells, and restoring c-Met protein level by transient overexpression could partially restore the malignancy of HCC cells that were reduced by miR-206 mimic transfection in vitro, suggesting that inhibiting c-Met protein expression is implicated in the HCC-suppressive role of miR-206. We observed no signicant inuence on EGFR or IGF1R protein level in HCC cells by miR-206 mimic transfection (data not shown), although several previous reports have described the inhibition of EGFR gene expression by miR-206 via mRNA targeting in lung squamous cell carcinoma, 36 head and neck squamous cell carcinoma 37 and ovarian carcinoma cells.…”

Section: Discussionmentioning

confidence: 72%

“…7,8 MiR-206 is a cancer-suppressive microRNA in colorectal cancer, non-small-cell lung cancer, ovarian cancer and neck squamous cell carcinoma by suppressing the activation of PI3K-Akt and MAPK signaling pathways. [9][10][11][12][13] MiR-206 has also been described as a tumor-suppressive microRNA in HCC: miR-206 was found downregulated in HCC in association with advance in tumor stage and patients' worsened outcome, 14 and the antiproliferative/pro-apoptotic effects of overexpressing miR-206 in HCC cells in vitro were also reported. [14][15][16] However, molecular mechanisms underlying the HCC-suppressive role of miR-206 remain largely underexplored.…”

Section: Introductionmentioning

confidence: 99%

Retracted Article: MiR-206 reduced the malignancy of hepatocellular carcinoma cells in vitro by inhibiting MET and CTNNB1 gene expressions

2019

RSC Adv.

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“…However, when the expression of miR-206 was inhibited, the impaired migration ability of MSCs was partially alleviated (P < 0:001 compared to the H 2 O 2 group), whereas supplementation of levamisole significantly blocked such positive effects (Figures 6(a) and 6(b)). Further, to explore the paracrine function of rat MSCs, we cocultured HUVEC cells with the supernatants of MSCs in different groups for 24 hours and then performed tube formation assay as described previously [22]. As shown in Figures 6(c)-6(e), compared to the NC group, both the meshes numbers and tube lengths in the H 2 O 2 group showed a dramatic decrease (P < 0:01).…”

Section: Alpl Was a Target Gene Of Mir-206 As Depicted Inmentioning

confidence: 94%

“…Moreover, the HUVEC angiogenesis in the miR-206 inhibitor group was even superior to that in the NC group. Similarly, an in vitro study observed that CCL19 high-expressed SW1116 supernatant was able to inhibit the angiogenesis of HUVEC through promoting miR-206, whereas CCL19 low-expressed SW620 supernatant can promote HUVEC angiogenesis [22]. Besides, Wang et al have reported that amphiregulin enhanced VEGF-A production in human chondrosarcoma cells and promoted angiogenesis by inhibiting miR-206 via the FAK/c-Src/PKCd pathway [39].…”

Section: Oxidative Medicine and Cellular Longevitymentioning

confidence: 97%

Downregulation of MicroRNA-206 Alleviates the Sublethal Oxidative Stress-Induced Premature Senescence and Dysfunction in Mesenchymal Stem Cells via Targeting Alpl

Yang

Meng

et al. 2020

Oxidative Medicine and Cellular Longevity

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Bone marrow-derived mesenchymal stem cells (MSCs) have shown great promise in tissue engineering and regenerative medicine; however, the regenerative capacity of senescent MSCs is greatly reduced, thus exhibiting limited therapy potential. Previous studies uncovered that microRNA-206 (miR-206) could largely regulate cell functions, including cell proliferation, survival, and apoptosis, but whether miR-206 is involved in the senescent process of MSCs remains unknown. In this study, we mainly elucidated the effects of miR-206 on MSC senescence and the underlying mechanism. We discovered that miR-206 was upregulated in the senescent MSCs induced by H2O2, and abrogation of miR-206 could alleviate this tendency. Besides, we determined that by targeting Alpl, miR-206 could ameliorate the impaired migration and paracrine function in MSCs reduced by H2O2. In vivo study, we revealed that inhibition of miR-206 in senescent MSCs could effectively protect their potential for myocardial infarction treatment in a rat MI model. In summary, we examined that inhibition of miR-206 in MSCs can alleviate H2O2-induced senescence and dysfunction, thus protecting its therapeutic potential.

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CCL19 suppresses angiogenesis through promoting miR-206 and inhibiting Met/ERK/Elk-1/HIF-1α/VEGF-A pathway in colorectal cancer

Cited by 121 publications

References 50 publications

VEGF and KRAS are Potential Targets of miR-206 Modulation in Triple Negative Breast Cancer

VEGF and KRAS are Potential Targets of miR-206 Modulation in Triple Negative Breast Cancer

Retracted Article: MiR-206 reduced the malignancy of hepatocellular carcinoma cells in vitro by inhibiting MET and CTNNB1 gene expressions

Downregulation of MicroRNA-206 Alleviates the Sublethal Oxidative Stress-Induced Premature Senescence and Dysfunction in Mesenchymal Stem Cells via Targeting Alpl

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