Hypoxic Non-Small-Cell Lung Cancer Cell-Secreted Exosomal microRNA-582-3p Drives Cancer Cell Malignant Phenotypes by Targeting Secreted Frizzled-Related Protein 1

Jian Wang; Jia Zhao; Jinsong Zhu; Shengli Zhang

摘要

Background: Hypoxic environment and exosomes (exos)-mediated intercellular communication are crucial for cancer invasion and metastasis, but the mechanisms are not yet fully understood. In this study, we investigated the regulatory effect of hypoxic tumor cell-secreted exosomal miR-582-3p on non-small-cell lung cancer (NSCLC) cell malignant phenotypes. Methods: The concentration and diameters of exos were evaluated by nanosight particle tracking analysis. microRNA-582-3p (miR-582-3p) expression was detected by quantitative real-time PCR. The fluorescent dye PKH26 was used to label exos. The direct interaction between miR-582-3p and secreted frizzled-related protein 1 (SFRP1) was determined by dual-luciferase activity assay. NSCLC cell proliferation, migration, and invasion abilities were assessed by cell count kit-8 assay, wound healing assay, and transwell migration and invasion assay. Western blot analysis was performed to detect the protein expression level. Results: Hypoxic NSCLC cell-derived exos promoted the proliferation, migration, and invasion of normoxic NSCLC cells. miR-582-3p expression was upregulated in hypoxic NSCLC cells and hypoxic NSCLC cell-secreted exos. Hypoxic NSCLC cell-derived exos transmitted miR-582-3p to normoxic NSCLC cells. Hypoxic NSCLC cell-secreted exosomal miR-582-3p promoted the proliferation, migration, and invasion of normoxic NSCLC cells. miR-582-3p inhibited the expression of SFRP1 protein by binding to its 3?-UTR. In addition, enforced expression of SFRP1 restrained malignant phenotypes of normoxic NSCLC cells, which was abrogated by hypoxic NSCLC cell-secreted exosomal miR-582-3p. Conclusion: Hypoxic NSCLC cell-secreted exosomal miR-582-3p drives cancer cell malignant phenotypes by targeting SFRP1, which provides a better understanding of cancer metastasis and may facilitate the development of therapeutics against human NSCLC.

机译：背景：缺氧环境和外泌体（EXOS）介导的细胞间通信对癌症侵袭和转移至关重要，但尚未完全理解机制。在这项研究中，我们研究了缺氧肿瘤细胞分泌的外泌体miR-582-3p对非小细胞肺癌（NSCLC）细胞恶性表型的调节作用。方法：通过纳米颗粒跟踪分析评估外壳的浓度和直径。通过定量实时PCR检测MicroRNA-582-3P（miR-582-3P）表达。荧光染料PKH26用于标记外壳。通过双荧光素酶活性测定法测定miR-582-3p和分泌细胞分泌的混浊相关蛋白1（sfrp1）之间的直接相互作用。通过细胞计数试剂盒测定，伤口愈合测定和Transwell迁移和侵袭测定评估NSCLC细胞增殖，迁移和侵袭能力。进行蛋白质印迹分析以检测蛋白质表达水平。结果：缺氧NSCLC细胞衍生的外壳促进常氧NSCLC细胞的增殖，迁移和侵袭。 MiR-582-3P表达在缺氧NMSCLC细胞和缺氧NMSCLC细胞分泌的外部上调。缺氧NSCLC细胞衍生的外部透射MiR-582-3P至常氧NSCLC细胞。缺氧NMSCLC细胞分泌的外泌体MIR-582-3P促进了常氧NSCLC细胞的增殖，迁移和侵袭。 MiR-582-3P通过与其3〜-UTR结合来抑制SFRP1蛋白的表达。此外，由缺氧NMSCLC细胞分泌的外泌体MIR-582-3P脱氧，强制表达SFRP1受限制的常氧NMSCLC细胞的恶性表型。结论：缺氧NMSCLC细胞分泌的外泌体MIR-582-3P通过靶向SFRP1驱动癌细胞恶性表型，这为癌症转移提供了更好的理解，并可促进对人NSCLC的治疗学的发展。

Hypoxic Non-Small-Cell Lung Cancer Cell-Secreted Exosomal microRNA-582-3p Drives Cancer Cell Malignant Phenotypes by Targeting Secreted Frizzled-Related Protein 1

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