4.5 Article

Exosomal miR-122-5p is Related to the Degree of Myelosuppression Caused by Chemotherapy in Patients with Colorectal Cancer

Journal

CANCER MANAGEMENT AND RESEARCH
Volume 13, Issue -, Pages 8329-8339

Publisher

DOVE MEDICAL PRESS LTD
DOI: 10.2147/CMAR.S332384

Keywords

colorectal cancer; chemotherapy; myelosuppression; miR-122-5p

Categories

Funding

  1. Independent Innovation Project in Putuo District [ptkwws201701]
  2. Clinical Specialized Disease Construction Project of Shanghai Putuo District Municipal Health Commission [2020tszb03]
  3. National Nature Science Foundation of China [81873137]
  4. Natural Science Foundation of Shanghai [20ZR1450500]
  5. Putuo District Health system [ptkwws201905]
  6. Hospital Scientific Research Project [2020366A]

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This study utilized small RNA sequencing and RT-qPCR techniques to find that the expression level of exosomal miR122-5p correlates with the severity of myelosuppression after chemotherapy, and this miRNA can inhibit the cell cycle by targeting CDK4.
Purpose: As rapidly dividing cells are usually the target of anticancer chemotherapy, it is inevitable that rapidly dividing normal cells become damaged, with myelosuppressive effects being a serious side effect of this therapy. Many recent studies have found that exosomal microRNAs (miRNAs) are related to the occurrence of some diseases. Patients and Methods: Small RNA sequencing was used to investigate differential exosomal miRNAs with the same expression trend between groups after chemotherapy: MildA (before chemotherapy in patients with mild myelosuppression) and MildB (after chemotherapy in patients with mild myelosuppression); SevereA (before chemotherapy in patients with severe myelosuppression) and SevereB (after chemotherapy in patients with severe myelosuppression). A Venn diagram was generated to screen exosomal miRNAs related to chemotherapy. Small RNA sequencing was also used to investigate differentially expressed exosomal miRNAs among these groups, and exosomal miRNAs related to myelosuppression after chemotherapy was explored using a Venn diagram. RT-qPCR was applied to further verify the sequencing results. We performed target gene prediction and functional analysis for candidate exosomal miRNAs. Results: Compared with that in the MildA or SevereA group, an increase in exosomal miR122-5p was found in the MildB or SevereB group, and the expression level was lower in the SevereB group than in the MildB group. However, we found no notable difference in its expression level between the MildA and SevereA groups. Similar results were not obtained for the remaining miRNAs. RT-qPCR confirmed the screening results. Further analyses indicated that exosomal miR-122-5p targets CDK4 to inhibit the cell cycle. Conclusion: The expression level of exosomal miR-122-5p in the serum of patients with colorectal cancer correlates with the severity of myelosuppression caused by chemotherapy, and miR-122-5p targets CDK4 to inhibit cell cycle progression.

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