Institute for Virology, University Medicine Essen, University of Duisburg-Essen, Essen, Germany.
Department of Infectious Diseases, West German Centre of Infectious Diseases, University Medicine Essen, Essen, Germany.
Front Cell Infect Microbiol. 2022 Oct 17;12:949036. doi: 10.3389/fcimb.2022.949036. eCollection 2022.
Type I interferons (IFNs) present the first line of defense against viral infections, providing antiviral, immunomodulatory and antiproliferative effects. The type I IFN family contains 12 IFNα subtypes and IFNβ, and although they share the same receptor, they are classified as non-redundant, capable to induce a variety of different IFN-stimulated genes. However, the biological impact of individual subtypes remains controversial. Recent data propose a subtype-specificity of type I IFNs revealing unique effector functions for different viruses and thus expanding the implications for IFNα-based antiviral immunotherapies. Despite extensive research, drug-resistant infections with herpes simplex virus type 1 (HSV-1), which is the common agent of recurrent orogenital lesions, are still lacking a protective or curing therapeutic. However, due to the risk of generalized infections in immunocompromised hosts as well as the increasing incidence of resistance to conventional antiherpetic agents, HSV infections raise major health concerns. Based on their pleiotropic effector functions, the application of type I IFNs represents a promising approach to inhibit HSV-1 replication, to improve host immunity and to further elucidate their qualitative differences. Here, selective IFNα subtypes and IFNβ were evaluated for their therapeutic potential in genital HSV-1 infections. Respective studies in mice revealed subtype-specific differences in the reduction of local viral loads. IFNβ had the strongest antiviral efficacy against genital HSV-1 infection in mice, whereas IFNα1, IFNα4, and IFNα11 had no impact on viral loads. Based on flow cytometric analyses of underlying immune responses at local and peripheral sites, these differences could be further assigned to specific modulations of the antiviral immunity early during HSV-1 infection. IFNβ led to enhanced systemic cytokine secretion and elevated cytotoxic responses, which negatively correlated with viral loads in the vaginal tract. These data provide further insights into the diversity of type I IFN effector functions and their impact on the immunological control of HSV-1 infections.
I 型干扰素 (IFN) 是抵御病毒感染的第一道防线,具有抗病毒、免疫调节和抗增殖作用。I 型 IFN 家族包含 12 种 IFNα 亚型和 IFNβ,尽管它们具有相同的受体,但它们被归类为非冗余的,能够诱导多种不同的 IFN 刺激基因。然而,个别亚型的生物学影响仍存在争议。最近的数据表明 I 型 IFN 具有亚型特异性,揭示了不同病毒的独特效应功能,从而扩大了基于 IFNα 的抗病毒免疫疗法的应用。尽管进行了广泛的研究,但单纯疱疹病毒 1 型(HSV-1)的耐药感染仍然缺乏保护性或治愈性治疗,HSV-1 是复发性或生殖器病变的常见病原体。然而,由于免疫功能低下宿主发生全身性感染的风险以及对传统抗疱疹药物的耐药性不断增加,HSV 感染引起了重大的健康问题。基于其多效性的效应功能,应用 I 型 IFN 代表了抑制 HSV-1 复制、改善宿主免疫和进一步阐明其定性差异的有前途的方法。在这里,评估了选择性 IFNα 亚型和 IFNβ 在生殖器 HSV-1 感染中的治疗潜力。在小鼠中的相应研究表明,在降低局部病毒载量方面存在亚型特异性差异。IFNβ 对小鼠生殖器 HSV-1 感染具有最强的抗病毒功效,而 IFNα1、IFNα4 和 IFNα11 对病毒载量没有影响。基于对局部和外周部位潜在免疫反应的流式细胞术分析,这些差异可以进一步归因于 HSV-1 感染早期抗病毒免疫的特异性调节。IFNβ 导致全身细胞因子分泌增加和细胞毒性反应增强,这与阴道部位的病毒载量呈负相关。这些数据为 I 型 IFN 效应功能的多样性及其对 HSV-1 感染免疫控制的影响提供了进一步的见解。
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