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文昌鱼中的细胞因子受体多样性预测了脊椎动物的最小必需细胞因子网络。

Cytokine Receptor Diversity in the Lamprey Predicts the Minimal Essential Cytokine Networks of Vertebrates.

机构信息

Laboratory of Brain Tumor Immunotherapy and Biology, Department of BioMedicine, University Hospital of Basel and University of Basel, Basel, Switzerland;

Laboratory of Zoology and Evolutionary Biology, Department of Environmental Sciences, University of Basel, Basel, Switzerland; and.

出版信息

J Immunol. 2022 Sep 1;209(5):1013-1020. doi: 10.4049/jimmunol.2200274. Epub 2022 Aug 1.

Abstract

The vertebrate adaptive immune systems (Agnatha and Gnathostomata) use sets of T and B lymphocyte lineages that somatically generate highly diverse repertoires of Ag-specific receptors and Abs. In Gnathostomata, cytokine networks regulate the activation of lymphoid and myeloid cells, whereas little is known about these components in Agnathans. Most gnathostome cytokines are four-helix bundle cytokines with poorly conserved primary sequences. In contrast, sequence conservation across bilaterians has been observed for cognate cytokine receptor chains, allowing their structural classification into two classes, and for downstream JAK/STAT signaling mediators. With conserved numbers among Gnathostomata, human cytokine receptor chains (comprising 34 class I and 12 class II) are able to interact with 28 class I helical cytokines (including most ILs) and 16 class II cytokines (including all IFNs), respectively. Hypothesizing that the arsenal of cytokine receptors and transducers may reflect homologous cytokine networks, we analyzed the lamprey genome and transcriptome to identify genes and transcripts for 23 class I and five class II cytokine receptors alongside one JAK signal mediator and four STAT transcription factors. On the basis of deduction of their respective orthologs, we predict that these receptors may interact with 16 class I and 3 class II helical cytokines (including IL-4, IL-6, IL-7, IL-12, IL-10, IFN-γ, and thymic stromal lymphoprotein homologs). On the basis of their respective activities in mammals, this analysis suggests the existence of lamprey cytokine networks that may regulate myeloid and lymphoid cell differentiation, including potential Th1/Th2 polarization. The predicted networks thus appear remarkably homologous to those of Gnathostomata, albeit reduced to essential functions.

摘要

脊椎动物适应性免疫系统(无颌类和有颌类)利用 T 和 B 淋巴细胞谱系的集合,体细胞产生高度多样化的 Ag 特异性受体和 Abs。在有颌类中,细胞因子网络调节淋巴样和髓样细胞的激活,而关于无颌类中的这些成分知之甚少。大多数有颌类细胞因子是具有较差保守性初级序列的四螺旋束细胞因子。相比之下,在两侧对称动物中观察到同源细胞因子受体链的序列保守性,允许它们的结构分类为两类,以及下游 JAK/STAT 信号转导介质。有颌类的保守数量,人类细胞因子受体链(包括 34 个 I 类和 12 个 II 类)分别能够与 28 个 I 类螺旋细胞因子(包括大多数 ILs)和 16 个 II 类细胞因子(包括所有 IFNs)相互作用。假设细胞因子受体和转导器的武器库可能反映同源细胞因子网络,我们分析了七鳃鳗基因组和转录组,以鉴定 23 个 I 类和 5 个 II 类细胞因子受体以及一个 JAK 信号转导介质和四个 STAT 转录因子的基因和转录物。基于它们各自的同源物的推断,我们预测这些受体可能与 16 个 I 类和 3 个 II 类螺旋细胞因子(包括 IL-4、IL-6、IL-7、IL-12、IL-10、IFN-γ 和胸腺基质淋巴生成素同源物)相互作用。基于它们在哺乳动物中的各自活性,该分析表明存在可能调节髓样和淋巴样细胞分化的七鳃鳗细胞因子网络,包括潜在的 Th1/Th2 极化。预测的网络因此似乎与有颌类的网络非常相似,尽管简化为必需功能。

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