Departamento de Bioquímica Clínica, Facultad de Ciencias Químicas, Universidad Nacional de Córdoba, Córdoba, Argentina.
Centro de Investigaciones en Bioquímica Clínica e Inmunología (CIBICI), Consejo Nacional de Investigaciones Científicas y Técnicas (CONICET), Córdoba, Argentina.
Front Immunol. 2024 Jan 12;14:1267641. doi: 10.3389/fimmu.2023.1267641. eCollection 2023.
Chagas disease causes a cardiac illness characterized by immunoinflammatory reactions leading to myocardial fibrosis and remodeling. The development of Chronic Chagas Cardiomyopathy (CCC) in some patients while others remain asymptomatic is not fully understood, but dysregulated inflammatory responses are implicated. The Aryl hydrocarbon receptor (AhR) plays a crucial role in regulating inflammation. Certain tryptophan (Trp) metabolites have been identified as AhR ligands with regulatory functions.
We investigated AhR expression, agonist response, ligand production, and AhR-dependent responses, such as IDO activation and regulatory T (Treg) cells induction, in two T. cruzi-infected mouse strains (B6 and Balb/c) showing different polymorphisms in AhR. Furthermore, we assessed the metabolic profile of Trp catabolites and AhR agonistic activity levels in plasma samples from patients with chronic Chagas disease (CCD) and healthy donors (HD) using a luciferase reporter assay and liquid chromatography-mass spectrophotometry (LC-MS) analysis. T. cruzi-infected B6 mice showed impaired AhR-dependent responses compared to Balb/c mice, including reduced IDO activity, kynurenine levels, Treg cell induction, CYP1A1 up-regulation, and AhR expression following agonist activation. Additionally, B6 mice exhibited no detectable AhR agonist activity in plasma and displayed lower CYP1A1 up-regulation and AhR expression upon agonist activation. Similarly, CCC patients had decreased AhR agonistic activity in plasma compared to HD patients and exhibited dysregulation in Trp metabolic pathways, resulting in altered plasma metabolite profiles. Notably, patients with severe CCC specifically showed increased N-acetylserotonin levels in their plasma. The methods and findings presented here contribute to a better understanding of CCC development mechanisms and may identify potential specific biomarkers for T. cruzi infection and the severity of associated heart disease. These insights could be valuable in designing new therapeutic strategies. Ultimately, this research aims to establish the AhR agonistic activity and Trp metabolic profile in plasma as an innovative, non-invasive predictor of prognosis for chronic Chagas disease.
恰加斯病可导致一种心脏疾病,其特征为免疫炎症反应导致心肌纤维化和重构。在一些患者中会发展为慢性恰加斯心肌病(CCC),而另一些患者则无症状,但炎症反应失调被认为与此相关。芳香烃受体(AhR)在调节炎症中起着至关重要的作用。某些色氨酸(Trp)代谢物已被确定为具有调节功能的 AhR 配体。
我们研究了在两种感染了 T. cruzi 的小鼠品系(B6 和 Balb/c)中 AhR 的表达、激动剂反应、配体产生以及 AhR 依赖性反应,如 IDO 激活和调节性 T(Treg)细胞诱导,这两种品系在 AhR 上存在不同的多态性。此外,我们使用荧光素酶报告基因检测和液相色谱-质谱联用(LC-MS)分析评估了慢性恰加斯病(CCD)患者和健康供体(HD)血浆样本中的 Trp 代谢物谱和 AhR 激动活性水平。与 Balb/c 小鼠相比,感染了 T. cruzi 的 B6 小鼠显示出 AhR 依赖性反应受损,包括 IDO 活性、犬尿氨酸水平、Treg 细胞诱导、CYP1A1 上调以及激动剂激活后的 AhR 表达减少。此外,B6 小鼠的血浆中检测不到 AhR 激动活性,并且在激动剂激活时,CYP1A1 的上调和 AhR 的表达减少。同样,与 HD 患者相比,CCD 患者的血浆中 AhR 激动活性降低,并且 Trp 代谢途径失调,导致血浆代谢物谱改变。值得注意的是,患有严重 CCC 的患者的血浆中 N-乙酰血清素水平升高。本文提出的方法和研究结果有助于更好地了解 CCC 发病机制,并可能为 T. cruzi 感染和相关心脏病严重程度确定潜在的特异性生物标志物。这些见解对于设计新的治疗策略具有重要意义。最终,本研究旨在将血浆中的 AhR 激动活性和 Trp 代谢谱确立为慢性恰加斯病预后的一种创新的、非侵入性预测指标。
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