Chronic DSS-Induced Colitis Exacerbates Parkinson’s Disease Phenotype and Its Pathological Features Following Intragastric Rotenone Exposure

IF 4.9 Q1 CHEMISTRY, MEDICINAL

ACS Pharmacology and Translational Science Pub Date : 2025-01-24 DOI:10.1021/acsptsci.4c0028610.1021/acsptsci.4c00286

Nishant Sharma, Monika Sharma, Disha Thakkar, Hemant Kumar, Sona Smetanova, Lucie Buresova, Petr Andrla and Amit Khairnar*,

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Abstract

Background: Parkinson’s disease (PD) is intricately linked to gastrointestinal inflammation and the presence of neurotoxins in the gut, integrating α-syn pathologic alterations and subsequent neurodegeneration into the brain. Objectives: This study aimed to explore the enduring impact of dextran sodium sulfate (DSS)-mediated colitis on the vulnerability of central dopaminergic neurons to subsequent rotenone exposure. Methods: To induce chronic colitis, 10-month-old C57BL/6 mice were pre-exposed to 3 cycles of 1 week of 1% (w/v) DSS administration in drinking water followed by 2 weeks of regular drinking water. After colitis induction, animals received a low dose of intragastric rotenone for the next 8 weeks, followed by testing for Parkinsonian behavior and GI phenotypes of inflammation. At the end of the 17th week, colon, brain stem, and midbrain tissue were isolated and analyzed for α-syn, inflammatory markers, and dopaminergic neuronal loss. Gut microbial composition was assessed by 16S rRNA sequencing analysis. Results: We found that chronic rotenone administration in the presence of preexisting colitis led to a further increase in colonic pro-inflammatory mediator expressions, α-syn expression, and reduced colonic tight junction protein expressions. We also found early impairment of GI functions and worsened grip strength in rotenone-exposed colitic mice. Furthermore, α-syn pathology specific to the colitic mice exposed to rotenone showed dopaminergic neurons degeneration and astroglial activation in substantia nigra and striatum, including regions of the brain stem, i.e., dorsal motor of the vagus and locus coeruleus. Finally, the result of 16S rRNA gene sequencing analysis indicated that colitic mice, after being exposed to rotenone, exhibited a discernible trend in their microbiota composition (Catenibacterium, Turicibactor, and clostridium sensue stricto 1), linking it to the development of PD. Conclusions: These findings indicate that prolonged low-dose rotenone exposure, combined with an early inflammatory intestinal milieu, provides a preconditioning effect on α-syn pathology and exerts neurodegeneration in the intragastric rotenone PD mouse model.

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慢性dss诱导的结肠炎在胃内暴露鱼藤酮后会加剧帕金森病的表型及其病理特征

背景：帕金森病（PD）与胃肠道炎症和肠道神经毒素的存在有着复杂的联系，将α-syn病理改变和随后的神经变性整合到大脑中。目的：本研究旨在探讨葡聚糖硫酸钠（DSS）介导的结肠炎对中枢多巴胺能神经元对后续鱼藤酮暴露的脆弱性的持久影响。方法：为诱导慢性结肠炎，将10月龄C57BL/6小鼠预先暴露于1% (w/v) DSS给药1周的3个周期的饮用水中，然后再正常饮水2周。结肠炎诱导后，动物在接下来的8周内接受低剂量的鱼藤酮灌胃，随后进行帕金森行为和GI表型炎症的检测。17周末，分离结肠、脑干和中脑组织，分析α-syn、炎症标志物和多巴胺能神经元损失。采用16S rRNA测序法测定肠道微生物组成。结果：我们发现，在既往存在结肠炎的情况下，慢性鱼藤酮可导致结肠促炎介质表达和α-syn表达进一步增加，结肠紧密连接蛋白表达降低。我们还发现鱼藤酮暴露的结肠炎小鼠早期胃肠道功能受损和握力恶化。此外，暴露于鱼藤酮的结肠炎小鼠的α-syn病理表现为黑质和纹状体的多巴胺能神经元变性和星形胶质细胞活化，包括脑干区域，即迷走神经背侧运动和蓝斑。最后，16S rRNA基因测序分析结果表明，暴露于鱼藤酮后，结肠炎小鼠的微生物群组成（Catenibacterium, Turicibactor, clostridium sensue stricto 1）呈现出明显的变化趋势，与PD的发生有关。结论：这些结果表明，长期低剂量鱼藤酮暴露，结合早期肠道炎症环境，对鱼藤酮腹腔PD小鼠模型的α-syn病理和神经变性提供了预调节作用。

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来源期刊

ACS Pharmacology and Translational Science Medicine-Pharmacology (medical)

CiteScore

10.00

自引率

3.30%

发文量

133

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