We previously reported that IGFBP7 plays a role in maintaining mRNA stability of oncogenic lncRNA UBE2CP3 by RNA-RNA interaction in gastric cancer (GC). Clinical cohort studies had implied an oncogenic role of IGFBP7 in GC. However, the molecular mechanism of IGFBP7 in GC progression remains unknown. In this study, clinical analysis based on two independent cohorts showed that IGFBP7 was positively associated with poor prognosis and macrophage infiltration in GC. Loss-of-function studies confirmed the oncogenic properties of IGFBP7 in regulating GC cell proliferation and invasion. Mechanismly, IGFBP7 was highly expressed in cancer-associated fibroblasts (CAF) and mesenchymal cells, and was induced by epithelial-to-mesenchymal transition (EMT) signaling, since its expression was increased by TGF-beta treatment and reduced by overexpression of OVOL2 in GC. RNA sequencing, qRT-PCR, ELISA assay showed that IGFBP7 positively regulated FGF2 expression and secretion in GC. Transcriptome analysis revealed that FGFR1 was downregulated in M1 polarization but upregulated in M2 polarization. Exogenous recombinant IGFBP7 treatment in macrophages and GC cells further identified that IGFBP7 promotes tumor associated macrophage (TAM) polarization via FGF2/FGFR1/PI3K/AKT axis. Our finding here represented the first evidence that IGFBP7 promotes GC by enhancing TAM/M2 macrophage polarization through FGF2/FGFR1/PI3K/AKT axis.
BackgroundThe dysregulated genes and miRNAs in tumor progression can be used as biomarkers for tumor diagnosis and prognosis. However, the biomarkers for predicting the clinical outcome of gastrointestinal cancer (GIC) are still scarce.MethodsGenome-wide association studies were performed to screen optimal prognostic miRNA biomarkers. RNA-seq, Ago-HITS-CLIP-seq, western blotting and qRT-PCR assays were conducted to identify target genes of miR-194. Genome-wide CRISPR-cas9 proliferation screening analysis were conducted to distinguish passenger gene and driver gene.ResultsA total of 9 prognostic miRNAs for GIC were identified by global microRNA expression analysis. Among them, miR-194 was the only one miRNA that significantly associated with overall survival, disease-specific survival and progress-free interval in both gastric, colorectal and liver cancers, indicating miR-194 was an optimal prognostic biomarker for GIC. RNA-seq analysis confirmed 18 conservative target genes of miR-194. Four of them, including ATP6V1F, PPP1R14B, BTF3L4 and SLC7A5, were directly targeted by miR-194 and required for cell proliferation. Cell proliferation assay validated that miR-194 inhibits cell proliferation by targeting ATP6V1F, PPP1R14B, BTF3L4 and SLC7A5 in GIC.ConclusionIn summary, miR-194 is an optimal biomarker for predicting the outcome of GIC. Our finding highlights that miR-194 exerts a tumor-suppressive role in digestive system cancers by targeting ATP6V1F, PPP1R14B, BTF3L4 and SLC7A5.
Serine proteases has been considered to be closely associated with the inflammatory response and tumor progression. As a novel serine protease, the biological function of PRSS23 is rarely studied in cancers. In this study, the prognostic significance of PRSS23 was analyzed in two-independent gastric cancer (GC) cohorts. PRSS23 overexpression was clinically correlated with poor prognosis and macrophage infiltration of GC patients. Loss-of-function study verified that PRSS23 plays oncogenic role in GC. RNA-seq, qRT-PCR, western blotting and ELISA assay confirmed that serine protease PRSS23 positively regulated FGF2 expression and secretion. Single-cell analysis and gene expression correlation analysis showed that PRSS23 and FGF2 were high expressed in fibroblasts, and highly co-expressed with the biomarkers of tumor associated macrophages (TAMs), cancer-associated fibroblasts (CAFs) and mesenchymal cells. Functional analysis confirmed PRSS23/FGF2 was required for TAM infiltration. Rescue assay further verified that PRSS23 promotes GC progression and TAM infiltration through FGF2. Survival analysis showed that high infiltration of M1-macrophage predicted favorable prognosis, while high infiltration level of M2-macrophage predicted poor prognosis in GC. Our finding highlights that PRSS23 promotes TAM infiltration through regulating FGF2 expression and secretion, thereby resulting in a poor prognosis.
Summary
In this paper, simple and consistent open boundary conditions are presented for the numerical simulation of viscous incompressible laminar flows. The present approach is based on an arbitrary Lagrangian‐Eulerian particle method using upwind interpolation. Three kinds of inlet/outlet boundary conditions are proposed for particle methods, a pressure specified inlet/outlet condition, a velocity profile specified inlet/outlet condition, and a fully developed flow outlet condition. These inlet/outlet conditions are realized by using boundary particles and modification to the physical value such as velocity. Poiseuille flows, flows over a backward‐facing step, and flows in a T‐shape branch are calculated. The results are compared with those of mesh‐based methods such as the finite volume method. The method presented herein exhibits accuracy and numerical stability.
In the process of high flow rate fracture and high gas production, the sealing performance of the premium connection decreases due to the dynamic load and vibration of downhole tubing strings, which may cause accidents. Existing static analysis methods cannot effectively explain this phenomenon. The main objective of this paper is to propose a novel analytical method for evaluating the sealing performance of a premium connection. In this paper, a dynamic model of sealing surfaces of the premium connection is established based on the vibration equation of elastic rod, and the hysteresis characteristics and energy dissipation mechanism of sealing surfaces are analyzed. Considering the influence of spherical radius, internal pressure, axial cyclic load amplitude, and modal vibration, a spherical-conical premium connection finite element model is established to analyze the influence laws of the connection’s energy dissipation and sealing performance. The results show that the sealing performance of the premium connection under dynamic load can be effectively analyzed by using energy dissipation theory compared with traditional static contact analysis. Compared with the vibration of the tubing string, the dynamic loads caused by the change of fluid pressure and flow rate in the tubing string have a significant influence on the connection’s sealing performance. When the internal pressure and axial cyclic loads are 80 MPa, 400 kN, or 60 MPa and 500 kN respectively, serious plastic deformation occurs in the thread and sealing surfaces, and the energy dissipation of the sealing surfaces increases significantly, which could lead to sealing failure.
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