Abstract
BackgroundTo investigate effect of microRNA-325-3p (miR-325-3p) on bone metastasis of colorectal cancer (CRC) and the precise role on osteoclastogenesis.MethodsCT-26 cells were injected into tibias to establish bone metastatic model of CRC in vivo. AgomiR-325-3p or antagomir-325-3p were injected in tail-veins of Balb/c mice to interfere the osteoclastogenesis and bone metastasis of CRC. Safranin O and Fast Green staining examined the changes of trabecular area and TRAP staining examined the osteoclast number in bone metastasis of CRC. Real-time PCR was conducted to test the RNA level of miR-325-3p and mRNA levels of TRAP and Cathepsin K in osteoclast precursors (OCPs). Dual-luciferase reporter system was utilized to identify the direct target of miR-325-3p. Conditioned medium from CT-26 cells was collected to stimulate the OCPs during osteoclastogenesis induced by RANKL and M-CSF in vitro. Western blot analysis was performed to examine the protein level of S100A4 in OCPs after interfered by agomiR-325-3p or antagomir-325-3p cultured in CM or not.ResultsmiR-325-3p downregulated in OCPs in CRC microenvironment both in vivo and in vitro. By luciferase activity assay, S100A4 was the target gene of miR-325-3p and the protein level of S100A4 in OCPs upregulated in CRC microenvironment. Overexpression of miR-325-3p inhibited the osteoclastogenesis of OCPs and it can be reversed after transfection with plasmid containing S100A4. Treatment with miR-325-3p can preserve trabecular area in bone metastasis of CRC.ConclusionmiR-325-3p can prevent osteoclast formation through targeting S100A4 in OCPs. Overexpression of miR-325-3p efficiently decreased the osteoclast number and attenuated bone resorption in bone metastasis of CRC.
Highlights
Bone is one of metastatic sites in colorectal cancer (CRC)
Results miR‐325‐3p downregulates in osteoclast precursors in bone metastasis of CRCSafranin O and Fast Green staining showed comparing with samples collected at 0 days post injection (0 d.p.i), trabecular area significantly decreased in samples collected at 14 d.p.i (Fig. 1a, b)
To investigate whether CT-26 cells downregulate the expression of miR-325-3p in osteoclast precursors (OCPs), conditioned medium (CM) collected from CT-26 cells were used to stimulate OCPs, the result showed the expression of miR-325-3p downregulated in CM treated OCPs (Fig. 1f )
Summary
Bone is one of metastatic sites in colorectal cancer (CRC). Complications, including bone-associated pain, pathological fractures, can influence quality of life (QoL) in patients with CRC significantly. Radiation and pathologic fractures can affect 45% and 10% patients with bone metastasis of CRC, respectively (Santini et al 2012). Preventing or attenuating the progression of bone metastasis is critical to improve QoL and prognosis of patients with bone metastasis of CRC. Due to relative lower incidence (Katoh et al 1995), the underlying mechanisms regulating bone metastasis of CRC are still elusive. To investigate effect of microRNA-325-3p (miR-325-3p) on bone metastasis of colorectal cancer (CRC) and the precise role on osteoclastogenesis
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