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犬尿氨酸酸对大鼠主动脉缺血再灌注模型的影响:药理学特征和蛋白质组学分析。

Effects of Kynurenic Acid on the Rat Aorta Ischemia-Reperfusion Model: Pharmacological Characterization and Proteomic Profiling.

机构信息

Laboratório Multidisciplinar em Pesquisa, Universidade São Francisco, 12916-900 Bragança Paulista, Brazil.

Laboratório de Bioquímica e Biofísica, Instituto Butantan, 05503-900 São Paulo, Brazil.

出版信息

Molecules. 2021 May 11;26(10):2845. doi: 10.3390/molecules26102845.

Abstract

Kynurenic acid (KYNA) is derived from tryptophan, formed by the kynurenic pathway. KYNA is being widely studied as a biomarker for neurological and cardiovascular diseases, as it is found in ischemic conditions as a protective agent; however, little is known about its effect after ischemia-reperfusion in the vascular system. We induced ischemia for 30 min followed by 5 min reperfusion (I/R) in the rat aorta for KYNA evaluation using functional assays combined with proteomics. KYNA recovered the exacerbated contraction induced by phenylephrine and relaxation induced by acetylcholine or sodium nitroprussiate in the I/R aorta, with vessel responses returning to values observed without I/R. The functional recovery can be related to the antioxidant activity of KYNA, which may be acting on the endothelium-injury prevention, especially during reperfusion, and to proteins that regulate neurotransmission and cell repair/growth, expressed after the KYNA treatment. These proteins interacted in a network, confirming a protein profile expression for endothelium and neuron repair after I/R. Thus, the KYNA treatment had the ability to recover the functionality of injured ischemic-reperfusion aorta, by tissue repairing and control of neurotransmitter release, which reinforces its role in the post-ischemic condition, and can be useful in the treatment of such disease.

摘要

犬尿酸(KYNA)来源于色氨酸,由犬尿氨酸途径形成。KYNA 作为神经和心血管疾病的生物标志物正在被广泛研究,因为它在缺血条件下作为一种保护剂存在;然而,关于其在血管系统缺血再灌注后的作用知之甚少。我们通过功能测定结合蛋白质组学方法,在大鼠主动脉中诱导缺血 30 分钟,再灌注 5 分钟(I/R),以评估 KYNA。KYNA 恢复了 I/R 主动脉中由苯肾上腺素引起的加剧收缩和由乙酰胆碱或硝普酸钠引起的舒张,血管反应恢复到没有 I/R 时的水平。功能恢复可能与 KYNA 的抗氧化活性有关,KYNA 可能作用于内皮损伤预防,特别是在再灌注期间,以及调节神经递质释放和细胞修复/生长的蛋白质,这些蛋白质在 KYNA 处理后表达。这些蛋白质相互作用形成一个网络,证实了 I/R 后内皮和神经元修复的蛋白质谱表达。因此,KYNA 治疗能够恢复损伤的缺血再灌注主动脉的功能,通过组织修复和控制神经递质释放,这加强了其在缺血后条件下的作用,并可用于治疗此类疾病。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1883/8150825/ee0ee8a14fd9/molecules-26-02845-g001.jpg

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