Exosomal Circ_FMN2 Derived from the Serum of Colorectal Cancer Patients Promotes Cancer Progression by miR-338-3p/MSI1 Axis

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作者
Qiyao Yu
Yi Zhang
Yanming Tian
Ale Peng
Xiujing Cui
Boyue Ding
Lei Yang
Yabin Liu
Yingchao Ju
Chao Gao
机构
[1] The Fourth Hospital of Hebei Medical University,Department of Research
[2] Hebei Medical University,Department of Physiology
[3] The Fourth Hospital of Hebei Medical University,Department of Radiation Oncology
[4] The Fourth Hospital of Hebei Medical University,Department of Surgery
[5] The Fourth Hospital of Hebei Medical University,Department of experimental animal center
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Colorectal cancer; Exosome; Circ_FMN2; miR-338-3p; MSI1;
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摘要
Background: Colorectal cancer (CRC) is a common malignancy of the gastrointestinal tract with high incidence and mortality. Exosomal circular RNA (circRNA) has been shown to be associated with the malignant progression of cancers, including CRC. Circ_0005100 (named as circ_FMN2) has been shown to promote CRC cell proliferation and migration. However, whether exosomal circ_FMN2 participated in CRC progression remains unclear. Methods: Exosomes were isolated from the serum of CRC patients and then identified using transmission electron microscope. Western blot assay was used to test the protein levels of exosome markers, proliferation-related marker, metastasis-related markers and musashi-1 (MSI1). The expression levels of circ_FMN2, microRNA (miR)-338-3p and MSI1 were detected by qPCR. Flow cytometry, colony formation assay, MTT assay, and transwell assay were employed to measure cell cycle, apoptosis, colony formation ability, viability, migration and invasion. Dual-luciferase reporter assay was performed to assess the interaction between miR-338-3p and circ_FMN2 or MSI1. BALB/c nude mice was used to conduct animal experiments. Results: Circ_FMN2 was overexpressed in the exosomes of CRC patient’s serums and CRC cells. Overexpressed exosomal circ_FMN2 could promote CRC cell proliferation, metastasis, and suppress apoptosis. Circ_FMN2 acted as miR-338-3p sponge. MiR-338-3p overexpression reversed the promotion effect of circ_FMN2 on CRC progression. MSI1 was found to be a target of miR-338-3p, and its overexpression revoked the inhibitory effect of miR-338-3p on CRC progression. Furthermore, exosomal circ_FMN2 overexpression also could facilitate CRC tumor growth in vivo. Conclusion: Exosomal circ_FMN2 accelerated CRC progression through miR-338-3p/MSI1 axis, revealing that exosomal circ_FMN2 might be a target for CRC treatment.
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页码:7322 / 7337
页数:15
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