Emerging challenges in innate immunity: Staphylococcus aureus and healthcare-associated infection

Muhammadul-Awwal Irodatullah Bisola , Gbolahan Olatunji , Emmanuel Kokori , Abdulhafeez Ayodele Mustapha , Godfred Yawson Scott , Ikponmwosa Jude Ogieuh , Nathnael Abera Woldehana , Anthony Chidera Stanley , Oyakhire Aizenosa Olohita , Ayedun Samuel Abiola , David B. Olawade , Nicholas Aderinto
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Abstract

Staphylococcus aureus, a prominent human pathogen, exhibits a remarkable ability to interact with host proteins involved in crucial physiological pathways, such as the complement system, coagulation cascade, and fibrinolysis cascade. This paper explores the ability of this notable bacteria to successfully manipulate and evade the host innate system, expatiating on the strategies that enhance its pathogenicity leading to implications on the healthcare system such as the propagation of diverse nosocomial infections. The investigation focuses on key S. aureus proteins, including Coagulase (Coa), von Willebrand factor-binding protein (vWbp), and Staphylokinase (SAK), which play pivotal roles in blood coagulation, fibrinolysis, and evasion of host antibacterial peptides. Notably, these proteins contribute to the formation of fibrin networks, protecting the bacterium from immune clearance and promoting lethal bloodstream infections in murine models. Additionally, the debate surrounding the role of SAK as a critical virulence factor is addressed, emphasizing its impact on biofilm formation, invasion of internal organs, and bacterial loads in sepsis studies. Furthermore, the interaction of S. aureus with matrix metalloproteinases and the secretion of superantigen-like proteins (SSL1 and SSL5) are explored as additional mechanisms employed by the bacterium to impede immune responses. In addressing emerging challenges in innate immunity, the paper discusses the escalating antibiotic resistance in S. aureus, with a specific focus on methicillin-resistant strains (MRSA) and its capacity to instigate healthcare-associated infections as an effect.

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先天性免疫的新挑战:金黄色葡萄球菌与医疗相关感染
金黄色葡萄球菌是一种常见的人类病原体,具有与参与补体系统、凝血级联和纤维蛋白溶解级联等关键生理途径的宿主蛋白质相互作用的卓越能力。本文探讨了这种著名细菌成功操纵和躲避宿主先天系统的能力,阐述了增强其致病性的策略,这些策略对医疗保健系统产生了影响,如传播各种鼻腔感染。研究重点是金黄色葡萄球菌的关键蛋白,包括凝固酶(Coa)、冯-威廉因子结合蛋白(vWbp)和葡萄球菌激酶(SAK),它们在血液凝固、纤维蛋白溶解和逃避宿主抗菌肽方面发挥着关键作用。值得注意的是,这些蛋白质有助于纤维蛋白网络的形成,保护细菌不被免疫清除,并促进小鼠模型中致命的血液感染。此外,还讨论了围绕 SAK 作为关键毒力因子的作用的争论,强调了它对生物膜形成、内脏器官入侵和败血症研究中细菌负荷的影响。此外,还探讨了金黄色葡萄球菌与基质金属蛋白酶的相互作用以及超抗原样蛋白(SSL1 和 SSL5)的分泌,这些都是金黄色葡萄球菌阻碍免疫反应的额外机制。在探讨先天性免疫方面新出现的挑战时,论文讨论了金黄色葡萄球菌不断升级的抗生素耐药性,并特别关注耐甲氧西林菌株(MRSA)及其引发医疗相关感染的能力。
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