文獻引用產(chǎn)品：

bs-12028R | GPR105 Rabbit pAb | WB

作者單位：中國藥科大學(xué)

Background and Aims

Venous thromboembolism (VTE) is a disease related to high mortality and complications. Neutrophil extracellular trap (NET) formation promotes thrombo-inflammatory responses, exacerbating VTE. P2Y₁₄ receptor (P2Y₁₄R), which is highly expressed on neutrophils mediates NET formation, but its role and mechanism in VTE are unclear. This study aims to explore the role and mechanism of P2Y₁₄R in VTE and to investigate the feasibility of P2Y₁₄R-targeting therapy for VTE.

Methods

Venous blood of VTE patients was collected to detect the expression of P2Y₁₄R. Deep vein thrombosis and disseminated intravascular coagulation models were developed to detect thrombus and NET formation in wild-type and neutrophil P2Y₁₄R deficiency mice. Transcriptomics, phosphorylated proteomics, and immunofluorescence were performed to investigate the mechanisms. A high-throughput Glide docking pipeline was performed to find potent P2Y₁₄R antagonists from repurposing drug library.

Results

Neutrophil P2Y₁₄R of VTE patients was significantly increased. Neutrophil-specific P2Y₁₄R deficiency alleviated venous thrombosis and NET formation in mice. Mechanistically, neutrophil P2Y₁₄R deletion promotes PKA-induced AKAP13 phosphorylation, thereby inhibiting RhoA activation and cytoskeleton rearrangement, resulting in reduced neutrophil-platelet aggregates and NET release. Interestingly, proglumide was identified as a potent P2Y₁₄R antagonist with excellent P2Y₁₄R antagonistic activity and binding affinity, of which the pharmacodynamic effect and mechanism on thrombosis and NET formation were verified.

Conclusions

Neutrophil P2Y₁₄R deficiency regulates PKA/AKAP13/RhoA pathway to inhibit neutrophil-platelet aggregate, thereby reducing NET release and venous thrombosis. This indicates that P2Y₁₄R may be a potential therapeutic target for the intervention of VTE using P2Y₁₄R antagonists, including proglumide.

文獻引用產(chǎn)品：

bs-1035R | CD86 Rabbit pAb | IF

作者單位：西安交通大學(xué)第二附屬醫(yī)院

摘要：Intrauterine adhesions (IUA) are characterized by fibrotic repair and partial or complete occlusion of the uterine cavity, resulting from endometrial damage. The occurrence of IUA can adversely affect the reproductive and physiological health of women. Developing a delivery platform capable of loading various bioactive agents to achieve personalized treatment strategies can significantly enhance IUA therapy. In this study, cryopolymerization is employed to fabricate an antifouling porous scaffold (GNP) with shape memory properties, serving as a delivery vehicle for bioactive agents. Both in vitro and in vivo experiments demonstrate that GNP can incorporate multiple bioactive agents (penicillin-streptomycin (PS), stem cell exosomes (Ex) and N-acetylcysteine (NAC)), and promote their sustained retention. Based on the core factors of adhesion formation, the antioxidant NAC is chosen as a model agent combined with GNP. In the rat IUA model, NAC-loaded GNP (P150N) modulates the endometrial microenvironment through its antioxidant, anti-inflammatory, and anti-fibrotic actions. P150N effectively facilitates endometrial regeneration, reduces adhesion formation, and significantly increases embryo implantation rates. Additionally, proteomics analysis reveals that the P150N significantly downregulates proteins associated with inflammation, oxidative stress, and fibrosis, while upregulating those involved in cell proliferation. Overall, this work presents a versatile platform, offering a potential personalized therapeutic strategy for IUA prevention.

文獻引用產(chǎn)品：

作者單位：廣州醫(yī)科大學(xué)附屬醫(yī)院