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没食子酸在对乙酰氨基酚(APAP)诱导的急性肝衰竭中的应用前景。

Prospective Application of Tannic Acid in Acetaminophen (APAP)-Induced Acute Liver Failure.

机构信息

Department of Biomechatronics Engineering, National Taiwan University, No. 1, Sec. 4, Roosevelt Road, Taipei 10617, Taiwan.

出版信息

Int J Mol Sci. 2023 Dec 25;25(1):317. doi: 10.3390/ijms25010317.

Abstract

This study investigated the effect of tannic acid (TA), a natural plant-derived polyphenol, on hepatocyte viability and function, focusing on both hepatoprotective and hepatocurative aspects within liver failure models. In an in vitro prevention model, the TA-containing group exhibited 1.5-fold and 59-fold higher relative cell viability and albumin synthesis, respectively, in injured mature hepatocytes (MHs) and 1.14-fold and 1.10-fold higher values in injured small hepatocytes (SHs), compared with the TA-free group. In the in vitro curative model, the TA-containing group exhibited 3.25-fold and 113-fold higher relative cell viability and albumin synthesis, respectively, in injured MHs and 0.36-fold and 3.55-fold higher values in injured SHs, compared with the TA-free group. In the in vivo disease model, the administration of 300 μL of 1 μg/mL TA significantly mitigated acute liver failure damage and post-APAP toxicity in mice. This was evident in serum analysis, where the levels of alanine transaminase, aspartate aminotransferase, and total bilirubin notably decreased, in agreement with histological observations. The study findings reveal that TA can enhance hepatic function at specific additive concentrations. Furthermore, even when injured by APAP, hepatocytes could revert to their preinjury state after additional TA supplementation. Additionally, pretreating hepatocytes with TA can alleviate subsequent damage. Thus, TA holds clinical potential in the treatment of APAP-induced liver failure.

摘要

本研究探讨了单宁酸(TA)对肝细胞活力和功能的影响,重点关注肝衰竭模型中的肝保护和肝修复两个方面。在体外预防模型中,与不含 TA 的组相比,含 TA 的组中受损成熟肝细胞(MHs)的相对细胞活力和白蛋白合成分别提高了 1.5 倍和 59 倍,受损小肝细胞(SHs)的相对细胞活力和白蛋白合成分别提高了 1.14 倍和 1.10 倍。在体外治疗模型中,与不含 TA 的组相比,含 TA 的组中受损 MHs 的相对细胞活力和白蛋白合成分别提高了 3.25 倍和 113 倍,受损 SHs 的相对细胞活力和白蛋白合成分别提高了 0.36 倍和 3.55 倍。在体内疾病模型中,给予 300μL 浓度为 1μg/mL 的 TA 显著减轻了急性肝衰竭和 APAP 后毒性对小鼠的损伤。这在血清分析中表现明显,其中丙氨酸转氨酶、天冬氨酸转氨酶和总胆红素水平显著降低,与组织学观察结果一致。研究结果表明,TA 可以在特定的附加浓度下增强肝功能。此外,即使肝细胞受到 APAP 损伤,在补充额外的 TA 后也可以恢复到损伤前的状态。此外,预先用 TA 处理肝细胞可以减轻随后的损伤。因此,TA 在治疗 APAP 诱导的肝衰竭方面具有临床潜力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e28b/10778794/036b3d64b02f/ijms-25-00317-g001.jpg

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