Project description:Our Prior research has shown that 6-hydroxygenistein (6-OHG) alleviates hypobaric hypoxia induced brain injury (HHBI) achieved by its powerful antioxidant, anti-inflammatory, and anti-apoptotic capabilities, but its mechanism still requires additional investigation. The objective of this study was to uncover the protective mechanism of 6-OHG against HHBI based on transcriptomics analysis and experimental validation.The RNA-Seq analysis revealed 1585 differentially expressed genes (DEGs) between the Con and Mod groups, with 460 upregulated and 1125 downregulated. Between the 6-OHG and Mod groups, there were 679 DEGs, including 348 upregulated and 331 downregulated genes. Go and KEGG function analyses highlighted the PI3K/AKT signaling pathway as a crucial regulatory mechanism. Western blot analysis showed that HH exposure caused a decrease in the ratios of p-PI3K/PI3K and p-AKT/AKT in the mouse brain, but this effect was reversed by 6-OHG treatment, indicating that 6-OHG activates the PI3K/AKT signaling pathway. Furthermore, LY294002, a selective PI3K inhibitor, effectively blocked this activation and also abolished the protective effects of 6-OHG on histopathological damage, as well as its antioxidant, anti-inflammatory, and anti-apoptotic activities in HHBI mice. In summary, 6-OHG mitigates HHBI by activating the PI3K/AKT signaling pathway, suggesting its potential therapeutic application for HHBI treatment.

Project description:E3 ubiquitin ligase RNF11 protects against liver ischemia reperfusion injury through HINT1 degradation-mediated PI3K/AKT activation

Project description:Protein post-translational modifications (PTMs) participate in important bioactive regulatory processes and therefore can help elucidate the pathogenesis of Metabolic dysfunction-associated steatotic liver disease (MASLD). Ubiquitination modification plays a vital role in regulating the inflammatory response and fibrosis in MASLD process. Here, we performed multi-omics analysis to demonstated that TRIM46 binds directedly with SGPL1, promoting SGPL1 degradation via K48-linked polyubiquitination which subsequently suppresses the activation of downstream lipophagy signaling cascades in MASLD progression.

Project description:Background and Aims: Ischemia/reperfusion injury (IRI), considered one of the most important causes of liver organ rejection in acute and chronic phases, generates an inflammatory environment leading to compromised allograft functionality and rejection. In the last ten years, iRhom2 emerged as an essential regulator of tumor necrosis factor (TNFα) release by controlling the activity of TNFα converting enzyme (TACE), thus implying its involvement in several inflammatory diseases. Our goal was to investigate iRhom2 function in IRI since no data have been described yet on its potential role in the insurgence of the injury. Methods: We analyzed iRhom2 expression in a cohort of 48 patients undergoing liver transplants (OT). We then study iRhom2 function via siRNA and CRISPR/Cas9 technology in macrophages subjected to in vitro IRI model. We used proteomics and cell biology assays to determine iRhom2 function during in vitro IRI. Finally, we used a novel in vitro IRI protocol to study the effects of iRhom2-ablated macrophages co-culture with hepatocytes. Results: We demonstrated that iRhom2 is involved in liver IRI progression in transplanted patients, and its downregulation modulates the secretion of pro-inflammatory cytokines, including HMGB1, in M1-like primary macrophages. Our findings showed that HMGB1 is secreted in an iRhom2-dependent manner and in a TACE-independent fashion, thus inducing IRI-associated senescence phenotype on injured hepatocytes. Conclusions: Our results show that HMGB1 iRhom2-dependent secretion is required to induce IRI-associated senescence phenotype on IRI-cultured hepatocytes. Thus, iRhom2 inhibition during IRI might represent a promising target to improve recovery from the damage and may prevent the development of late-onset allograft rejection by tackling the damage from two different aspects: TNF-dependent inflammation and HMGB1-dependent hepatocyte senescence.

Project description:Neuroblastoma is a pediatric tumor of the peripheral sympathetic nervous system with a highly variable prognosis. Activation of the PI3K/AKT pathway in neuroblastoma is correlated with poor patient prognosis, but the precise downstream effectors mediating this effect have not been determined. Here, we identify the forkhead transcription factor FOXO3a as a key target of the PI3K/AKT pathway in neuroblastoma. FOXO3a expression was elevated in low stage neuroblastoma tumors and normal embryonal neuroblasts, but reduced in late stage neuroblastoma. Inactivation of FOXO3a by AKT was essential for neuroblastoma cell survival. Treatment of neuroblastoma cells with the dual PI3K/mTOR inhibitor PI-103 activated FOXO3a and triggered apoptosis. This effect was rescued by FOXO3a silencing. Conversely, apoptosis induced by PI-103 or the AKT inhibitor MK-2206 was potentiated by FOXO3a overexpression. Further, levels of total or phosphorylated FOXO3a correlated closely with apoptotic sensitivity to MK-2206. In clinical specimens, there was an inverse relationship between gene expression signatures regulated by PI3K signaling and FOXO3a transcriptional activity. Moreover, high PI3K activity and low FOXO3a activity were each associated with an extremely poor prognosis. Our work indicates that expression of FOXO3a and its targets offer useful prognostic markers as well as biomarkers for PI3K/AKT inhibitor efficacy in neuroblastoma. Affymetrix U133 Plus 2.0 profiling of SY5Y-TetR-FOXO3A cells treated with doxycycline and/or the PI3K/mTOR inhibitor PI-103. Each condition profiled in triplicate.

Project description:Pulmonary ischemia–reperfusion injury (IRI) is characterized by excessive inflammation, oxidative stress, and mitochondrial dysfunction, leading to severe lung damage. To elucidate the molecular mechanisms underlying the protective effects of a macrophage membrane-coated mesoporous polydopamine nanoparticle system loaded with Ginsenoside Rg3 (Rg3@PACVs) combined with near-infrared (NIR) irradiation, we performed transcriptome sequencing of rat lung tissues. Differential gene expression profiles were compared between IRI and IRI + Rg3@PACVs + NIR groups. A total of 209 upregulated and 332 downregulated genes were identified in the treatment group relative to IRI controls. Functional enrichment analyses revealed that Rg3@PACVs + NIR pretreatment enhanced pathways related to endoplasmic reticulum stress response, PI3K-AKT signaling, oxygen transport, protein folding, hypoxia response, TCA cycle activity, ATP-dependent processes, and cell cycle progression. In contrast, inflammation-associated pathways including TLR/NF-κB signaling, cytokine binding, cell adhesion molecules, neutrophil extracellular trap formation, IL-1β production, and leukocyte trans-endothelial migration were significantly suppressed. GSEA further demonstrated reduced oxidative stress (cytochrome P450 activity) and enhanced FOXO signaling. These findings indicate that Rg3@PACVs + NIR mitigates pulmonary IRI by coordinately suppressing inflammatory responses, alleviating oxidative stress, and restoring mitochondrial homeostasis, thereby promoting lung tissue repair.

Project description:The expression changes of secretory proteins under the inhibition of PI3K were studied, including AML12-DEX-DMSO and AML12-DEX-PI3K.

Project description:TRAIP suppresses bladder cancer progression by catalyzing K48-linked polyubiquitination of MYC

Project description:E2F1 has been shown to induce both proliferation and apoptosis. We now show that PI3K/Akt signaling regulates the balance of these events by specifically blocking expression of genes in the E2F1 apoptotic program but not the proliferative program. Experiment Overall Design: 11 samples total, two replicates each (except Sample 1 which is represented once)

Project description:Purpose The aim of this study was to investigate the effects of baicalin on septic cardiomyopathy and to elucidate the underlying mechanisms involved. Specifically, this study sought to determine the effects of baicalin on septic cardiomyopathy induced by AC16 cells and LPS in C57BL/6J mice and its underlying mechanisms. Methods: Echocardiography, histological staining, immunoblotting, qPCR, ELISA, RNA-seq, network pharmacology and molecular docking were performed. Changes in cardiomyocytes after LPS injection in mice were observed. The targets of baicalein in septic cardiomyopathy were screened using molecular docking and molecular dynamics, and the pathway of baicalein action was further elucidated by using RNA-seq and network pharmacology. Results: LPS stimulation induced apoptosis, an inflammatory response and oxidative stress in cardiomyocytes. In vivo experiments revealed that baicalin treatment attenuated septic myocardial injury, as evidenced by enhanced cardiac functional parameters, preservation of myocardial structure, and reduced inflammatory/apoptotic responses, and RNA-seq analyses revealed that the Pi3k/AKT signaling pathway was activated after the administration of baicalin, which was verified both in vitro and in vivo; this indicated that the protective effects of baicalin were related to the findings in vitro and in vivo, suggesting that the protective effect of baicalin is related to the activation of the PI3K/AKT pathway. Molecular docking studies revealed that baicalin inhibited cardiomyocyte inflammation and cardiomyocyte apoptosis, thereby ameliorating sepsis-induced cardiac injury, which may be related to the PI3K/Akt pathway. Conclusion: Baicalin activates the PI3K/AKT pathway and protects against sepsis-induced cardiac injury by binding with AKT.