The transcriptomic profile shows the protective effects of celecoxib on cirrhotic splenomegaly.

IF 2.9 4区 医学 Q3 IMMUNOLOGY Immunopharmacology and Immunotoxicology Pub Date : 2024-02-01 Epub Date: 2024-01-21 DOI:10.1080/08923973.2023.2281282
Yanting Ye, Shihang Tang, Yang Tai, Chong Zhao, Chengwei Tang, Zhiyin Huang, Jinhang Gao
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Abstract

Background: Splenomegaly can exacerbate liver cirrhosis and portal hypertension. We have previously demonstrated that cyclooxygenase-2 (COX-2) inhibitor can attenuate cirrhotic splenomegaly. However, the mechanism of cirrhotic splenomegaly remains unclear, thus becoming the focus of the present study.

Materials and methods: Thioacetamide (TAA) intraperitoneal injection was used to induce cirrhotic splenomegaly. Rats were randomized into the control, TAA and TAA + celecoxib groups. Histological analysis and high-throughput RNA sequencing of the spleen were conducted. Splenic collagen III, α-SMA, Ki-67, and VEGF were quantified.

Results: A total of 1461 differentially expressed genes (DEGs) were identified in the spleens of the TAA group compared to the control group. The immune response and immune cell activation might be the major signaling pathways involved in the pathogenesis of cirrhotic splenomegaly. With its immunoregulatory effect, celecoxib presents to ameliorate cirrhotic splenomegaly and liver cirrhosis. Furthermore, 304 coexisting DEGs were obtained between TAA vs. control and TAA + celecoxib vs. TAA. Gene ontology (GO) and KEGG analyses collectively indicated that celecoxib may attenuate cirrhotic splenomegaly through the suppression of splenic immune cell proliferation, inflammation, immune regulation, and fibrogenesis. The impacts on these factors were subsequently validated by the decreased splenic Ki-67-positive cells, macrophages, fibrotic areas, and mRNA levels of collagen III and α-SMA.

Conclusions: Celecoxib attenuates cirrhotic splenomegaly by inhibiting splenic immune cell proliferation, inflammation, and fibrogenesis. The current study sheds light on the therapeutic strategy of liver cirrhosis by targeting splenic abnormalities and provides COX-2 inhibitors as a novel medical treatment for cirrhotic splenomegaly.

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转录组学分析显示塞来昔布对肝硬化脾肿大的保护作用。
背景:脾肿大可加重肝硬化和门静脉高压症。我们之前已经证明环氧化酶-2 (COX-2)抑制剂可以减轻肝硬化脾肿大。然而,肝硬化脾肿大的发病机制尚不清楚,因此成为本研究的重点。材料与方法:采用硫乙酰胺(TAA)腹腔注射诱导肝硬化脾大。将大鼠随机分为对照组、TAA组和TAA +塞来昔布组。对脾脏进行组织学分析和高通量RNA测序。定量脾III型胶原、α-SMA、Ki-67、VEGF。结果:与对照组相比,TAA组小鼠脾脏共鉴定出1461个差异表达基因(DEGs)。免疫应答和免疫细胞活化可能是肝硬化脾肿大发病的主要信号通路。塞来昔布具有改善肝硬化脾肿大和肝硬化的免疫调节作用。此外,TAA与对照组、TAA +塞来昔布与TAA之间共存在304个deg。基因本体论(GO)和KEGG分析共同表明,塞来昔布可能通过抑制脾免疫细胞增殖、炎症、免疫调节和纤维化来减轻肝硬化脾肿大。对这些因素的影响随后通过脾脏ki -67阳性细胞、巨噬细胞、纤维化区域以及III型胶原和α-SMA mRNA水平的降低来验证。结论:塞来昔布通过抑制脾免疫细胞增殖、炎症和纤维化减轻肝硬化脾肿大。目前的研究揭示了针对脾脏异常的肝硬化治疗策略,并提供了COX-2抑制剂作为肝硬化脾肿大的一种新的药物治疗方法。
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来源期刊
CiteScore
5.40
自引率
0.00%
发文量
133
审稿时长
4-8 weeks
期刊介绍: The journal Immunopharmacology and Immunotoxicology is devoted to pre-clinical and clinical drug discovery and development targeting the immune system. Research related to the immunoregulatory effects of various compounds, including small-molecule drugs and biologics, on immunocompetent cells and immune responses, as well as the immunotoxicity exerted by xenobiotics and drugs. Only research that describe the mechanisms of specific compounds (not extracts) is of interest to the journal. The journal will prioritise preclinical and clinical studies on immunotherapy of disorders such as chronic inflammation, allergy, autoimmunity, cancer etc. The effects of small-drugs, vaccines and biologics against central immunological targets as well as cell-based therapy, including dendritic cell therapy, T cell adoptive transfer and stem cell therapy, are topics of particular interest. Publications pointing towards potential new drug targets within the immune system or novel technology for immunopharmacological drug development are also welcome. With an immunoscience focus on drug development, immunotherapy and toxicology, the journal will cover areas such as infection, allergy, inflammation, tumor immunology, degenerative disorders, immunodeficiencies, neurology, atherosclerosis and more. Immunopharmacology and Immunotoxicology will accept original manuscripts, brief communications, commentaries, mini-reviews, reviews, clinical trials and clinical cases, on the condition that the results reported are based on original, clinical, or basic research that has not been published elsewhere in any journal in any language (except in abstract form relating to paper communicated to scientific meetings and symposiums).
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