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黄芩苷可保护小鼠免受肠出血性细菌的致死性感染。

Baicalin Protects Mice from Lethal Infection by Enterohemorrhagic .

作者信息

Zhang Yong, Qi Zhimin, Liu Yan, He Wenqi, Yang Cheng, Wang Quan, Dong Jing, Deng Xuming

机构信息

The First Hospital and Institute of Infection and Immunity, Jilin UniversityChangchun, China; Key Laboratory of Zoonosis, Ministry of Education, Institute of Zoonosis, College of Veterinary Medicine, Jilin UniversityChangchun, China.

Key Laboratory of Zoonosis, Ministry of Education, Institute of Zoonosis, College of Veterinary Medicine, Jilin University Changchun, China.

出版信息

Front Microbiol. 2017 Mar 9;8:395. doi: 10.3389/fmicb.2017.00395. eCollection 2017.

Abstract

Shiga-like toxin-producing (STEC) O157:H7 poses grave challenges to public health by its ability to cause severe colonic diseases and renal failure in both human and animals. Shiga-like toxins are the major pathogenic factor for some highly virulent expecially Shiga-like toxin 2. Conventional treatments such as antibiotics can facilitate the release of the toxin thus potentially exacerbate the diseases. Small molecule inhibitors and antibodies capable of neutralizing the toxins are the two major venues for the development of therapeutics against enterohemorrhagic serotype infection. While promising and potentially effective at clinical settings, these approaches need to overcome obstacles such as the limited routes of administration, responses from the host immune system, which are known to differ greatly among individuals. Our previous studies demonstrate that Baicalin (BAI), a flavonoid compound isolated from protects against rStx2-induced cell cytotoxicity and also protects mice from lethal rStx2 challenges by inducing Stx2 to form inactive oligomers. In this manuscript, we present some exciting work showing that baicalin is an effective agent for therapeutic treatment of STEC O157:H7 infection.

摘要

产志贺毒素大肠杆菌(STEC)O157:H7因其能够在人和动物中引起严重的结肠疾病和肾衰竭,对公共卫生构成了严峻挑战。志贺样毒素是一些高毒力菌株的主要致病因素,尤其是志贺样毒素2。抗生素等传统治疗方法会促使毒素释放,从而可能加重病情。能够中和毒素的小分子抑制剂和抗体是开发抗肠出血性血清型感染治疗药物的两个主要途径。虽然这些方法在临床环境中有前景且可能有效,但它们需要克服诸如给药途径有限、宿主免疫系统反应等障碍,而众所周知,这些反应在个体之间差异很大。我们之前的研究表明,从黄芩中分离出的黄酮类化合物黄芩苷(BAI)可保护细胞免受重组志贺样毒素2(rStx2)诱导的细胞毒性,并通过诱导Stx2形成无活性寡聚体来保护小鼠免受致死性rStx2攻击。在本论文中,我们展示了一些令人兴奋的工作,表明黄芩苷是治疗STEC O157:H7感染的有效药物。

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