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尽管存在 IFN-λ 受体表达,但血液免疫细胞(而非角质形成细胞或黑素细胞)对 III 型干扰素的反应受损:这对这些细胞因子的治疗应用有影响。

Despite IFN-lambda receptor expression, blood immune cells, but not keratinocytes or melanocytes, have an impaired response to type III interferons: implications for therapeutic applications of these cytokines.

机构信息

Interdisciplinary Group of Molecular Immunopathology, Dermatology/Medical Immunology, University Hospital Charité, Berlin, Germany.

出版信息

Genes Immun. 2009 Dec;10(8):702-14. doi: 10.1038/gene.2009.72. Epub 2009 Oct 1.

DOI:10.1038/gene.2009.72
PMID:19798076
Abstract

Interferon (IFN)-lambda1, -2 and -3 (also designated as interleukin (IL)-29, IL-28alpha and IL-28beta) represent a new subfamily within the class II cytokine family. They show type I IFN-like antiviral and cytostatic activities in affected cells forming the basis for IFN-lambda1 therapy currently under development for hepatitis C infection. However, many aspects of IFN-lambdas are still unknown. This study aimed at identifying the target cells of IFN-lambdas within the immune system and the skin. Among skin cell populations, keratinocytes and melanocytes, but not fibroblasts, endothelial cells or subcutaneous adipocytes turned out to be targets. In contrast to these target cells, blood immune cell populations did not clearly respond to even high concentrations of these cytokines, despite an IFN-lambda receptor expression. Interestingly, immune cells expressed high levels of a short IFN-lambda receptor splice variant (sIFN-lambdaR1/sIL-28R1). Its characterization revealed a secreted, glycosylated protein that binds IFN-lambda1 with a moderate affinity (K(D) 73 nM) and was able to inhibit IFN-lambda1 effects. Our study suggests that IFN-lambda therapy should be suited for patients with verrucae, melanomas and non-melanoma skin cancers, apart from patients with viral hepatitis, and would not be accompanied by immune-mediated complications known from type I IFN application.

摘要

干扰素(IFN)-lambda1、-2 和 -3(也称为白细胞介素(IL)-29、IL-28alpha 和 IL-28beta)代表 II 类细胞因子家族中的一个新亚家族。它们在受影响的细胞中表现出类似于 I 型 IFN 的抗病毒和细胞抑制活性,这为目前正在开发的用于丙型肝炎感染的 IFN-lambda1 治疗奠定了基础。然而,IFN-lambdas 的许多方面仍然未知。本研究旨在确定免疫系统和皮肤中 IFN-lambdas 的靶细胞。在皮肤细胞群体中,角质形成细胞和黑素细胞,但不是成纤维细胞、内皮细胞或皮下脂肪细胞,被证明是靶细胞。与这些靶细胞相反,尽管存在 IFN-lambda 受体表达,但血液免疫细胞群体甚至对高浓度的这些细胞因子也没有明显反应。有趣的是,免疫细胞表达高水平的短 IFN-lambda 受体剪接变体(sIFN-lambdaR1/sIL-28R1)。其特征表明它是一种分泌的、糖基化的蛋白质,能够以中等亲和力(K(D)73 nM)结合 IFN-lambda1,并能够抑制 IFN-lambda1 的作用。我们的研究表明,除了患有病毒性肝炎的患者外,IFN-lambda 疗法还应适用于患有疣、黑色素瘤和非黑色素瘤皮肤癌的患者,并且不会伴有已知来自 I 型 IFN 应用的免疫介导的并发症。

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