吗啡使用诱导胃微生物失调,通过 TLR2 信号转导驱动胃炎症,质子泵抑制可减弱该信号转导。
Morphine use induces gastric microbial dysbiosis driving gastric inflammation through TLR2 signalling which is attenuated by proton pump inhibition.
机构信息
Department of Surgery, Miller School of Medicine, University of Miami, Miami, Florida, USA.
Sylvester Comprehensive Cancer Center, Miami, Florida, USA.
出版信息
Br J Pharmacol. 2023 Jun;180(12):1582-1596. doi: 10.1111/bph.16025. Epub 2023 Jan 24.
BACKGROUND AND PURPOSE
Opioids are the standard drug for pain management; however, their effects on gastric dysfunction are relatively understudied. Opioid users have a higher incidence of gastric pathology leading to increased hospitalization. Herein, we investigated the consequences of morphine use on gastric pathology and the underlying mechanisms. We further investigated the therapeutic benefit of proton pump inhibition to overcome morphine-mediated gastric inflammation.
EXPERIMENTAL APPROACH
Mice were implanted with 25 mg slow-release morphine and placebo pellets. Gastric microbiome analyses were performed. Gastric damage was assayed. Gastric pH was measured. Germ-free and TLR2KO mice were used to investigate the mechanisms. Gastroprotective studies were performed with the proton pump inhibitor (PPI) omeprazole.
KEY RESULTS
Chronic morphine treatment alters gastric microbial composition and induces preferential expansion of pathogenic bacterial communities such as Streptococcus and Pseudomonas. Morphine causes disruption of the gastric mucosal layer, increases apoptosis, and elevates inflammatory cytokines. Moreover, morphine-mediated gastric pathology was significantly attenuated in germ-free mice, and reconstitution of morphine gastric microbiome in germ-free mice resulted gastric inflammation. In addition, morphine-mediated gastric inflammation was attenuated in TLR2KO mice. Morphine causes a decrease in gastric pH, which contributes to gastric dysbiosis leads to gastric inflammation. Omeprazole treatment inhibits gastric acidity, rescuing morphine-induced gastric dysbiosis and preventing inflammation.
CONCLUSION AND IMPLICATIONS
This study attributes morphine-induced gastric acidity as a driver of gastric dysbiosis and pathology and proposes the therapeutic use of PPI as an inexpensive approach for the clinical management of morphine-associated pathophysiology.
背景和目的
阿片类药物是疼痛管理的标准药物;然而,它们对胃功能障碍的影响相对研究较少。阿片类药物使用者胃病理发生率较高,导致住院率增加。本文研究了吗啡使用对胃病理的影响及其潜在机制。我们进一步研究了质子泵抑制剂治疗以克服吗啡介导的胃炎症的治疗益处。
实验方法
给小鼠植入 25mg 缓释吗啡和安慰剂丸。进行胃微生物组分析。测定胃损伤。测量胃 pH 值。使用无菌和 TLR2KO 小鼠研究机制。进行质子泵抑制剂(PPI)奥美拉唑的胃保护研究。
主要结果
慢性吗啡治疗改变了胃微生物组成,并诱导了致病性细菌群落(如链球菌和假单胞菌)的优先扩张。吗啡引起胃黏膜层破坏、增加细胞凋亡和升高炎症细胞因子。此外,无菌小鼠中吗啡介导的胃病理明显减轻,并且无菌小鼠中吗啡胃微生物组的重建导致胃炎症。此外,TLR2KO 小鼠中吗啡介导的胃炎症减轻。吗啡引起胃酸度降低,导致胃菌群失调导致胃炎症。奥美拉唑治疗抑制胃酸,挽救吗啡诱导的胃菌群失调并预防炎症。
结论和意义
本研究将吗啡引起的胃酸作为胃菌群失调和病理的驱动因素,并提出使用 PPI 的治疗方法作为治疗吗啡相关病理生理的一种廉价方法。
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