RSV A 和 RSV B 亚群之间的差异及其对药物预防措施的影响。

IF 4.7 3区 医学 Q1 INFECTIOUS DISEASES Infectious Diseases and Therapy Pub Date : 2024-08-01 Epub Date: 2024-07-06 DOI:10.1007/s40121-024-01012-2
Charles Nuttens, Juliette Moyersoen, Daniel Curcio, Zuleika Aponte-Torres, Marc Baay, Hilde Vroling, Bradford D Gessner, Elizabeth Begier
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引用次数: 0

摘要

导言:了解呼吸道合胞病毒(RSV)A 和 B 亚群之间的差异有助于制定预防策略和公共卫生干预措施。我们旨在描述 RSV 亚群的结构差异、流行病学和基因组多样性。我们还调查了相关的免疫反应和临床严重程度的差异:方法:从 PubMed 和 Google Scholar(1985-2023 年)上进行文献综述,并通过滚雪球的方法从获取的出版物中的参考文献中进行扩展:结果:RSV 有两个主要的抗原亚群:A 和 B,由 G 糖蛋白定义。预融合构象中的 RSV F 融合糖蛋白是病毒中和抗体的主要靶标,RSV A 和 RSV B 的表面暴露区域不同。这两个亚群每年都在共同传播,但对于临床严重程度是否会受感染 RSV 株系亚群的影响还存在很大争议。据观察,报告 RSV 亚群对临床严重性影响的研究之间存在很大差异。疾病严重程度较高的趋势可能归因于 RSV A,但对于感染其中一个亚群是否会导致更严重的后果,目前尚未达成共识。在过去二十年中,RSV 基因型的多样性有所减少,自 2014 年以来,ON 和 BA 已成为 RSV A 和 RSV B 的唯一检测到的血系。2014 年后获得数据的研究均未报告这两个亚组之间疾病严重程度的差异。RSV F 相对保守,与 RSV A 和 B 高度相似,但氨基酸序列发生了变化。接种后第二季的初步结果表明,对于基于 RSV PreF 的单价疫苗,RSV B 的特异性疗效比 RSV A 减弱得更快:结论:RSV A 和 RSV B 都是造成全球 RSV 负担的主要原因。这两种 RSV 亚群都会导致严重的疾病,迄今为止,没有任何现有证据表明这两个亚群的临床严重程度存在差异。因此,必须采取有效措施预防 RSV A 和 RSV B 导致的疾病,以确保公共卫生干预措施的影响力。需要进行超时监测,以评估抗体水平下降对特定亚群疗效的影响。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Differences Between RSV A and RSV B Subgroups and Implications for Pharmaceutical Preventive Measures.

Introduction: Understanding the differences between respiratory syncytial virus (RSV) subgroups A and B provides insights for the development of prevention strategies and public health interventions. We aimed to describe the structural differences of RSV subgroups, their epidemiology, and genomic diversity. The associated immune response and differences in clinical severity were also investigated.

Methods: A literature review from PubMed and Google Scholar (1985-2023) was performed and extended using snowballing from references in captured publications.

Results: RSV has two major antigenic subgroups, A and B, defined by the G glycoprotein. The RSV F fusion glycoprotein in the prefusion conformation is a major target of virus neutralizing antibodies and differs in surface exposed regions between RSV A and RSV B. The subgroups co-circulate annually, but there is considerable debate as to whether clinical severity is impacted by the subgroup of the infecting RSV strain. Large variations between the studies reporting RSV subgroup impact on clinical severity were observed. A tendency for higher disease severity may be attributed to RSV A but no consensus could be reached as to whether infection by one of the subgroup caused more severe outcomes. RSV genotype diversity decreased over the last two decades, and ON and BA have become the sole lineages detected for RSV A and RSV B, since 2014. No studies with data obtained after 2014 reported a difference in disease severity between the two subgroups. RSV F is relatively well conserved and highly similar between RSV A and B, but changes in the amino acid sequence have been observed. Some of these changes led to differences in F antigenic sites compared to reference F sequences (e.g., RSV/A Long strain), which are more pronounced in antigenic sites of the prefusion conformation of RSV B. Initial results from the second season after vaccination suggest specific RSV B efficacy wanes more rapidly than RSV A for RSV PreF-based monovalent vaccines.

Conclusions: RSV A and RSV B both contribute substantially to the global RSV burden. Both RSV subgroups cause severe disease and none of the available evidence to date suggests any differences in clinical severity between the subgroups. Therefore, it is important to implement measures effective at preventing disease due to both RSV A and RSV B to ensure impactful public health interventions. Monitoring overtime will be needed to assess the impact of waning antibody levels on subgroup-specific efficacy.

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来源期刊
Infectious Diseases and Therapy
Infectious Diseases and Therapy Medicine-Microbiology (medical)
CiteScore
8.60
自引率
1.90%
发文量
136
审稿时长
6 weeks
期刊介绍: Infectious Diseases and Therapy is an international, open access, peer-reviewed, rapid publication journal dedicated to the publication of high-quality clinical (all phases), observational, real-world, and health outcomes research around the discovery, development, and use of infectious disease therapies and interventions, including vaccines and devices. Studies relating to diagnostic products and diagnosis, pharmacoeconomics, public health, epidemiology, quality of life, and patient care, management, and education are also encouraged. Areas of focus include, but are not limited to, bacterial and fungal infections, viral infections (including HIV/AIDS and hepatitis), parasitological diseases, tuberculosis and other mycobacterial diseases, vaccinations and other interventions, and drug-resistance, chronic infections, epidemiology and tropical, emergent, pediatric, dermal and sexually-transmitted diseases.
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