Abstract
BackgroundAngiogenesis provides essential nutrients and oxygen for tumor growth and has become the main mechanism of tumor invasion and metastasis. Exosomes are nanoscale membrane vesicles containing proteins, lipids, mRNA and microRNA (miRNA), which mediate intercellular communication and play an important role in tumor progression. Accumulated evidence indicates that tumor-derived exosomal miRNAs participate in the tumor microenvironment and promote angiogenesis.MethodsBioinformatic target prediction and dual luciferase reporter assays were performed to identify the binding site between miR-663b and the 3′-UTR of vinculin (VCL). VCL overexpression lentivirus and miR-663b overexpression/inhibition lentivirus were used to create a VCL overexpression model and miR-663b overexpression/inhibition model in-vitro. Immunohistochemistry (IHC) assays and western blot assays were used to detect protein expression. Exosome-cell cocultures, wound healing assays, tube formation assays and transwell assays were used to measure the migration and tube formation ability of vascular endothelial cells [human umbilical vein endothelial cells (HUVECs)]. siRNA targeted VCL was used to knockdown VCL.ResultsIn the present study, we found that miR-663b was elevated in cervical cancer tissue and exosomes. miR-663b could bind the 3′-UTR of VCL and inhibit its expression. VCL is downregulated in cervical cancer, and decreased VCL has a negative correlation with a high level of miR-663b. Further studies demonstrated that exosomes secreted by cervical cancer cells can deliver miR-663b to HUVECs and inhibit the expression of VCL, thereby promoting angiogenesis and tumor growth.ConclusionsmiR-663b derived from cancer cell exosomes acts as a driving factor for angiogenesis and a potential target of antiangiogenic therapy in cervical cancer. Our findings illustrated a new signaling pathway, including exosomes, miRNAs and target genes, which provides potential targets for antiangiogenic therapy.
Highlights
Cervical cancer remains an important cancer worldwide and was responsible for an estimated 570,000 cases and 311,000 deaths in 2018 worldwide, making it the fourth most frequently diagnosed cancer and the fourth leading cause of cancer death in women [1]
VCL is downregulated in cervical cancer We explored the expression of VCL in cervical cancer from clinical samples
WB and PCR results showed that the protein and mRNA levels of VCL in cervical cancer tissue were significantly lower than those in normal cervix (Fig. 1A, B)
Summary
Cervical cancer remains an important cancer worldwide and was responsible for an estimated 570,000 cases and 311,000 deaths in 2018 worldwide, making it the fourth most frequently diagnosed cancer and the fourth leading cause of cancer death in women [1]. Previous studies have shown that tumor growth will not exceed 1–2 mm or metastasize to other organs due to insufficient oxygen and nutrient supply if there is no new blood vessel formation [3, 4]. Angiogenesis is essential for tumor proliferation, migration and invasion and is a very common phenomenon in cervical cancer [5, 6]. It is essential to suppress the progression of cervical cancer by exploring new antiangiogenic molecular mechanisms of angiogenesis. Angiogenesis provides essential nutrients and oxygen for tumor growth and has become the main mechanism of tumor invasion and metastasis. Exosomes are nanoscale membrane vesicles containing proteins, lipids, mRNA and microRNA (miRNA), which mediate intercellular communication and play an important role in tumor progression. Accumulated evidence indicates that tumor-derived exosomal miRNAs participate in the tumor microenvironment and promote angiogenesis
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