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用于研究与急性风湿热/风湿性心脏病相关的自身免疫并发症疾病机制的可靠动物模型的要求。

Requirements for a Robust Animal Model to Investigate the Disease Mechanism of Autoimmune Complications Associated With ARF/RHD.

作者信息

Rafeek Rukshan A M, Sikder Suchandan, Hamlin Adam S, Andronicos Nicholas M, McMillan David J, Sriprakash Kadaba S, Ketheesan Natkunam

机构信息

School of Science and Technology, University of New England, Armidale, NSW, Australia.

Department of Medicine and Surgery, Chattogram Veterinary and Animal Sciences University, Chattogram, Bangladesh.

出版信息

Front Cardiovasc Med. 2021 May 5;8:675339. doi: 10.3389/fcvm.2021.675339. eCollection 2021.

Abstract

The pathogenesis of Acute Rheumatic Fever/Rheumatic Heart Disease (ARF/RHD) and associated neurobehavioral complications including Sydenham's chorea (SC) is complex. Disease complications triggered by Group A streptococcal (GAS) infection are confined to human and determining the early events leading to pathology requires a robust animal model that reflects the hallmark features of the disease. However, modeling these conditions in a laboratory animal, of a uniquely human disease is challenging. Animal models including cattle, sheep, pig, dog, cat, guinea pigs rats and mice have been used extensively to dissect molecular mechanisms of the autoimmune inflammatory responses in ARF/RHD. Despite the characteristic limitations of some animal models, several rodent models have significantly contributed to better understanding of the fundamental mechanisms underpinning features of ARF/RHD. In the Lewis rat autoimmune valvulitis model the development of myocarditis and valvulitis with the infiltration of mononuclear cells along with generation of antibodies that cross-react with cardiac tissue proteins following exposure to GAS antigens were found to be similar to ARF/RHD. We have recently shown that Lewis rats injected with recombinant GAS antigens simultaneously developed cardiac and neurobehavioral changes. Since ARF/RHD is multifactorial in origin, an animal model which exhibit the characteristics of several of the cardinal diagnostic criteria observed in ARF/RHD, would be advantageous to determine the early immune responses to facilitate biomarker discovery as well as provide a suitable model to evaluate treatment options, safety and efficacy of vaccine candidates. This review focuses on some of the common small animals and their advantages and limitations.

摘要

急性风湿热/风湿性心脏病(ARF/RHD)及其相关神经行为并发症(包括 Sydenham 舞蹈病(SC))的发病机制很复杂。A 组链球菌(GAS)感染引发的疾病并发症仅限于人类,确定导致病理变化的早期事件需要一个能反映该疾病标志性特征的强大动物模型。然而,在实验室动物中模拟这种独特的人类疾病情况具有挑战性。包括牛、羊、猪、狗、猫、豚鼠、大鼠和小鼠在内的动物模型已被广泛用于剖析 ARF/RHD 中自身免疫炎症反应的分子机制。尽管一些动物模型存在典型局限性,但几种啮齿动物模型对更好地理解 ARF/RHD 特征背后的基本机制做出了重大贡献。在 Lewis 大鼠自身免疫性心内膜炎模型中,发现暴露于 GAS 抗原后,心肌炎和心内膜炎的发展伴有单核细胞浸润以及与心脏组织蛋白发生交叉反应的抗体产生,这与 ARF/RHD 相似。我们最近发现,注射重组 GAS 抗原的 Lewis 大鼠同时出现了心脏和神经行为变化。由于 ARF/RHD 起源是多因素的,一个能展现出 ARF/RHD 中观察到的几个主要诊断标准特征的动物模型,将有利于确定早期免疫反应以促进生物标志物的发现,以及提供一个合适的模型来评估治疗方案、候选疫苗的安全性和有效性。本综述重点关注一些常见的小动物及其优缺点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/36c8/8131511/048d8aa375c5/fcvm-08-675339-g0001.jpg

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