Identification of two novel regions of human IL-6 responsible for receptor binding and signal transduction.

糖蛋白130 受体 普通伽马链 信号转导 反平行(数学) 生物 细胞生物学 分子生物学 白细胞介素-21受体 生物化学 物理 量子力学 磁场 车站3
作者
Marc Ehlers,Joachim Grötzinger,F D deHon,Jürgen Müllberg,Just P. J. Brakenhoff,Jue Liu,Axel Wollmer,Stefan Rose‐John
出处
期刊:Journal of Immunology [American Association of Immunologists]
卷期号:153 (4): 1744-1753 被引量:104
标识
DOI:10.4049/jimmunol.153.4.1744
摘要

The pleiotropic cytokine IL-6 has been predicted to be a protein with four antiparallel alpha-helices. Human IL-6 acts on human and murine cells, whereas murine IL-6 is only active on murine cells. The construction of a set of chimeric human/murine IL-6 proteins has recently allowed us to define a new region (residues Lys41-Glu95) within the IL-6 molecule as being important for receptor binding and biologic activity. We subdivided and analyzed this region, which primarily corresponds to the loop between the first and second alpha-helix of IL-6 with respect to its role in the interaction with the ligand binding subunit of the IL-6 receptor complex and with the IL-6 signal-transducing protein gp130. By construction and analysis of human/murine chimeric IL-6 molecules with only 7 to 10 amino acid residues different from human IL-6 we show that two distinct parts of this region are responsible for receptor binding and signal transduction. On the basis of the recently published structure of granulocyte-CSF, we present a three-dimensional model for the tertiary structure of IL-6, which, together with the IL-6 receptor interaction data, allows for the rational design of human IL-6 receptor antagonists.

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