Inhibition of RIPK1-driven necroptosis ameliorates inflammatory hyperalgesia caused by lipopolysaccharide: involvement of TLR-, NLRP3-, and caspase-11-mediated signaling pathways.

IF 1.5 4区生物学 Q4 BIOCHEMISTRY & MOLECULAR BIOLOGY

Cellular and molecular biology Pub Date : 2025-01-12 DOI:10.14715/cmb/2024.70.12.7

Seda Kurt, Sefika Pinar Senol, Dilsah Ezgi Yilmaz, Omer Bahceli, Beyza Ozgen, Zainab Sabrie, Muhammed Ahmed-Reda Elosman, Bahar Tunctan

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引用次数: 0

Abstract

Increasing evidence suggests that inhibition of receptor-interacting serine/threonine-protein kinase (RIPK) 1/RIPK3/mixed lineage kinase domain-like pseudokinase (MLKL) necrosome has protective effects in vivo models of painful conditions seen in humans associated with inflammation and demyelination in the central nervous system. However, the contribution of RIPK1-driven necroptosis to inflammatory pain remains unknown. Therefore, this study aims to determine the effect of necrostatin (Nec) -1s, a selective RIPK1 inhibitor, on lipopolysaccharide (LPS)-induced inflammatory pain and related underlying mechanisms. In the saline-, LPS-, and/or Nec-1s-injected male mice, thermal hyperalgesia was evaluated by hot plate test. Alterations in the expression of proteins involved in the RIPK1, toll-like receptor (TLR) 4, myeloid differentiation factor (MyD) 88/toll-interleukin (IL)-1 receptor domain-containing adapter-inducing interferon-β (TRIF)/nuclear factor (NF)-kB, nucleotide-binding oligomerization domain, leucine-rich repeat and pyrin domain containing (NLRP) 3/apoptosis-associated speck-like protein containing a caspase recruitment domain (ASC)/pro-caspase-1, and caspase-11/gasdermin D (GSDMD) signaling pathways, as well as proteins related to demyelination and remyelination in the brain and spinal cord were determined by the immunoblotting method. The LPS-induced alleviation of thermal hyperalgesia was prevented by necrostatin-1s. Necrostatin-1s reversed (1) increased activity of RIPK1, RIPK3, MLKL, and NF-kB p65, (2) enhanced expression of TLR4, MyD88, TRIF, NF-kB p65, HMGB1, NLRP3, ASC, caspase-1 p20, IL-1β, caspase-11 p20, p30-GSDMD, and semaphorin 3A, and (3) diminished myelin PLP expression induced by LPS. These findings suggest that the use of RIPK1 inhibitors could be a therapeutic approach in the management of inflammatory pain associated with necroptosis, pyroptosis, and demyelination.

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抑制ripk1驱动的坏死性下垂可改善脂多糖引起的炎症性痛觉过敏：参与TLR-、NLRP3-和caspase-11介导的信号通路。

越来越多的证据表明，受体相互作用丝氨酸/苏氨酸蛋白激酶（RIPK） 1/RIPK3/混合谱系激酶结构域样伪激酶（MLKL）坏死体的抑制在与中枢神经系统炎症和脱髓鞘相关的人类疼痛疾病的体内模型中具有保护作用。然而，ripk1驱动的坏死性上睑下垂在炎症性疼痛中的作用尚不清楚。因此，本研究旨在确定选择性RIPK1抑制剂坏死性他汀(Nec) -1对脂多糖（LPS）诱导的炎症性疼痛的影响及其相关机制。在生理盐水、LPS和/或nec -1s注射的雄性小鼠中，通过热板试验评估热痛觉过敏。RIPK1、toll样受体（TLR） 4、髓样分化因子（MyD） 88/toll-白细胞介素(IL)-1受体结构域(TRIF)/核因子(NF)-kB、核苷酸结合寡聚化结构域、富含亮氨酸的重复序列和pyrin结构域（NLRP） 3/含有caspase募集结构域(ASC)/ caspase-1前的凋亡相关斑点样蛋白表达的改变。免疫印迹法检测大鼠脑和脊髓中caspase-11/gasdermin D （GSDMD）信号通路，以及与脱髓鞘和再髓鞘形成相关的蛋白。脂多糖诱导的热痛觉过敏缓解被坏死他汀-1阻止。坏死他汀-1逆转了(1)RIPK1、RIPK3、MLKL和NF-kB p65活性的升高，(2)TLR4、MyD88、TRIF、NF-kB p65、HMGB1、NLRP3、ASC、caspase-1 p20、IL-1β、caspase-11 p20、p30-GSDMD和信号蛋白3A的表达增强，(3)LPS诱导的髓磷脂PLP表达降低。这些发现表明，使用RIPK1抑制剂可能是治疗坏死下垂、焦下垂和脱髓鞘相关炎症性疼痛的一种治疗方法。

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来源期刊

Cellular and molecular biology 生物-生化与分子生物学

CiteScore

1.60

自引率

12.50%

发文量

331

期刊介绍： Cellular and Molecular Biology publishes original articles, reviews, short communications, methods, meta-analysis notes, letters to editor and comments in the interdisciplinary science of Cellular and Molecular Biology linking and integrating molecular biology, biophysics, biochemistry, enzymology, physiology and biotechnology in a dynamic cell and tissue biology environment, applied to human, animals, plants tissues as well to microbial and viral cells. The journal Cellular and Molecular Biology is therefore open to intense interdisciplinary exchanges in medical, dental, veterinary, pharmacological, botanical and biological researches for the demonstration of these multiple links.