XIST sponges miR-320d to promote chordoma progression by regulating ARF6

Wang, Yonggang; Tang, Zhouzhou; Guo, Weichun

doi:10.1016/j.jbo.2022.100447

Cited by 1 publication

(9 citation statements)

References 36 publications

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“…[126,127] The same sponging mechanism on has-miR-320d, for example by a competitive endogenous RNA, resulting in the loss of tumor suppression effects of has-miR-320d, as the key mediation of tumorigenesis and development, was demonstrated in research reports like on lung cancer [122] and on chordoma. [126,127] All these results indicated that hsa-miR-320d was a novel promising biomarker or target for early diagnosis, prognosis assessment and therapy, including chemoradiotherapy sensitivity assessment, in the relative tumor patients. [114,[117][118][119][120][121][122][123][124]126,127]…”

Section: The Potential Values Of Exosomal Hsa-mir-320d In Ecmentioning

confidence: 74%

“…All the research reports mentioned above on the effects of hsa-miR-320d on the relative cancers showed that the relative effects of hsa-miR-320d were altogether negatively oncogenic, as hsa-miR-320d was a potential tumor suppressor. [114,117–127] The expression of hsa-miR-320d was significantly decreased in the cancer tissue and/or the peripheral serum of patients, [114,117–119,123,124,126] which was a loss of negative effect of hsa-miR-320d as a potential tumor suppressor. A lower expression level of hsa-miR-320d, either in cancer tissue or in peripheral serum, was positively correlated with the related tumorigenesis and development, adverse tumor phenotypes or prognosis, like bigger tumor size, advanced clinic stages, lymph node metastasis, chemoresistance, recurrence, or shorter overall and disease-free survival, etc.…”

Section: Discussionmentioning

confidence: 99%

“…As to hsa-miR-320d in cancers, there have been several special research reports, like on colorectal cancer, [117][118][119][120][121] on lung cancer, [122] on HCC, [114] on ovarian cancer, [123,124] on prostate cancer [10,125] and on chordoma. [126,127] But, until now, there is not any special research report on the potential values of exosomal hsa-miR-320d in the EC clinic and the relative research.…”

Section: The Potential Values Of Exosomal Hsa-mir-320d In Ecmentioning

confidence: 99%

“…[121] The related target genes of hsa-miR-320d, here, could be TUSC3 (an oncogene) [117] or c-Myc (an oncogenic transcription factor), [121] BMI1 (an oncogene), [114] KIF3C-mRNA (an oncogene) [125] or ARF6 (an oncogene). [127] The related signaling pathways or routes could be Rap1 signaling pathway like in colorectal cancer, [119] exosomal lncRNA LINC00662/has-miR-320d/E2F1 axis like in lung cancer [122] and either LncRNA NONHSAT114552/hsa-miR-320d/NRP1 axis or XIST/has-miR-320d/ARF6 axis [127] like in chordoma. [126,127] The same sponging mechanism on has-miR-320d, for example by a competitive endogenous RNA, resulting in the loss of tumor suppression effects of has-miR-320d, as the key mediation of tumorigenesis and development, was demonstrated in research reports like on lung cancer [122] and on chordoma.…”

Section: The Potential Values Of Exosomal Hsa-mir-320d In Ecmentioning

confidence: 99%

“…[127] The related signaling pathways or routes could be Rap1 signaling pathway like in colorectal cancer, [119] exosomal lncRNA LINC00662/has-miR-320d/E2F1 axis like in lung cancer [122] and either LncRNA NONHSAT114552/hsa-miR-320d/NRP1 axis or XIST/has-miR-320d/ARF6 axis [127] like in chordoma. [126,127] The same sponging mechanism on has-miR-320d, for example by a competitive endogenous RNA, resulting in the loss of tumor suppression effects of has-miR-320d, as the key mediation of tumorigenesis and development, was demonstrated in research reports like on lung cancer [122] and on chordoma. [126,127] All these results indicated that hsa-miR-320d was a novel promising biomarker or target for early diagnosis, prognosis assessment and therapy, including chemoradiotherapy sensitivity assessment, in the relative tumor patients.…”

Section: The Potential Values Of Exosomal Hsa-mir-320d In Ecmentioning

confidence: 99%

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Four differentially expressed exosomal miRNAs as prognostic biomarkers and therapy targets in endometrial cancer: Bioinformatic analysis

Yao,

Shi,

Zhu

2023

Medicine

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Endometrial cancer (EC) is one of the most common gynecological malignancies worldwide. Accumulated evidence has demonstrated exosomes of cancer cells carry microRNAs (miRNAs) to nonmalignant cells to induce metastasis. Our study aimed to find possible biomarkers of EC. Data for miRNA expression related with exosome from EC patients were downloaded from The Cancer Genome Atlas database, and the miRNA expression profiles associated with exosomes of EC were downloaded from the National Center for Biotechnology Information. We used different algorithms to analyze the differential miRNA expression, infer the relative proportion of immune infiltrating cells, predict chemotherapy sensitivity, and comprehensively score each gene set to evaluate the potential biological function changes of different samples. The gene ontology analysis and Kyoto encyclopedia of genome genomics pathway analysis were performed for specific genes. A total of 13 differential miRNAs were identified, of which 4 were up-regulated. The 4 miRNAs, that is hsa-miR-17-3p, hsa-miR-99b-3p, hsa-miR-193a-5p, and hsa-miR-320d, were the hub exosomal miRNAs that were all closely related to the clinic phenotypes and prognosis of patients. This study preliminarily indicates that the 4 hub exosomal miRNAs (hsa-miR-17-3p, hsa-miR-99b-3p, hsa-miR-193a-5p, and hsa-miR-320d) could be used as prognostic biomarkers or therapy targets in EC. Further studies are required to make sure of their real feasibility and values in the EC clinic and the relative research.

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