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抑制百日咳毒素的新策略。

Novel Strategies to Inhibit Pertussis Toxin.

机构信息

Institute of Pharmacology and Toxicology, Ulm University Medical Center, 89081 Ulm, Germany.

出版信息

Toxins (Basel). 2022 Mar 3;14(3):187. doi: 10.3390/toxins14030187.

Abstract

Pertussis, also known as whooping cough, is a respiratory disease caused by infection with , which releases several virulence factors, including the AB-type pertussis toxin (PT). The characteristic symptom is severe, long-lasting paroxysmal coughing. Especially in newborns and infants, pertussis symptoms, such as leukocytosis, can become life-threatening. Despite an available vaccination, increasing case numbers have been reported worldwide, including Western countries such as Germany and the USA. Antibiotic treatment is available and important to prevent further transmission. However, antibiotics only reduce symptoms if administered in early stages, which rarely occurs due to a late diagnosis. Thus, no causative treatments against symptoms of whooping cough are currently available. The AB-type protein toxin PT is a main virulence factor and consists of a binding subunit that facilitates transport of an enzyme subunit into the cytosol of target cells. There, the enzyme subunit ADP-ribosylates inhibitory α-subunits of G-protein coupled receptors resulting in disturbed cAMP signaling. As an important virulence factor associated with severe symptoms, such as leukocytosis, and poor outcomes, PT represents an attractive drug target to develop novel therapeutic strategies. In this review, chaperone inhibitors, human peptides, small molecule inhibitors, and humanized antibodies are discussed as novel strategies to inhibit PT.

摘要

百日咳,又称“天哮呛”,是一种由 感染引起的呼吸道疾病,会释放多种毒力因子,包括 AB 型百日咳毒素(PT)。其特征性症状是严重且持久的阵发性咳嗽。尤其是在新生儿和婴儿中,百日咳的症状(如白细胞增多症)可能会危及生命。尽管有可用的疫苗,但全世界包括德国和美国等西方国家在内的百日咳病例数量都在不断增加。抗生素治疗可用于预防进一步传播,这非常重要。然而,抗生素只有在早期使用才能减轻症状,但由于诊断较晚,这种情况很少发生。因此,目前尚无针对百日咳症状的特效治疗方法。AB 型蛋白毒素 PT 是一种主要的毒力因子,由促进酶亚基进入靶细胞胞质溶胶的结合亚基组成。在那里,酶亚基 ADP-核糖基化 G 蛋白偶联受体的抑制性 α 亚基,导致 cAMP 信号转导紊乱。作为与白细胞增多症和不良预后等严重症状相关的重要毒力因子,PT 代表了开发新型治疗策略的有吸引力的药物靶点。在这篇综述中,讨论了伴侣蛋白抑制剂、人类肽、小分子抑制剂和人源化抗体等作为抑制 PT 的新型策略。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/79ed/8951090/5c4b937a62fa/toxins-14-00187-g001.jpg

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