Taupin J L, Miossec V, Pitard V, Blanchard F, Daburon S, Raher S, Jacques Y, Godard A, Moreau J F
CNRS UMR 5540, Université de Bordeaux II, Bâtiment 1b, 146 rue Léo-Saignat, 33076 Bordeaux Cedex, France.
J Biol Chem. 1999 May 14;274(20):14482-9. doi: 10.1074/jbc.274.20.14482.
The gp190 transmembrane protein, the low affinity receptor for the leukemia inhibitory factor (LIF), belongs to the hematopoietin family of receptors characterized by the cytokine binding domain (CBD). gp190 is one of the very few members of this family to contain two such domains. The membrane-proximal CBD (herein called D2) is separated from the membrane-distal one (called D1) by an immunoglobulin-like (Ig) domain and is followed by three fibronectin type III repeats. We used truncated gp190 mutants and a blocking anti-gp190 monoclonal antibody to study the role of these repeats in low affinity receptor function. Our results showed that the D1Ig region was involved in LIF binding, while D2 appeared to be crucial for the proper folding of D1, suggesting functionally important interactions between the two CBDs in the wild-type protein. In addition, a point mutation in the carboxyl terminus of the Ig region strongly impaired ligand binding. These findings suggest that at least two distinct sites, both located within the D1Ig region, are involved in LIF binding to gp190, and more generally, that ligand binding sites on these receptors may well be located outside the canonical CBDs.
gp190跨膜蛋白是白血病抑制因子(LIF)的低亲和力受体,属于以细胞因子结合域(CBD)为特征的造血因子受体家族。gp190是该家族中极少数含有两个此类结构域的成员之一。膜近端的CBD(在此称为D2)通过一个免疫球蛋白样(Ig)结构域与膜远端的CBD(称为D1)隔开,随后是三个纤连蛋白III型重复序列。我们使用截短的gp190突变体和一种阻断性抗gp190单克隆抗体来研究这些重复序列在低亲和力受体功能中的作用。我们的结果表明,D1Ig区域参与LIF结合,而D2似乎对D1的正确折叠至关重要,这表明野生型蛋白中两个CBD之间存在功能上重要的相互作用。此外,Ig区域羧基末端的一个点突变严重损害了配体结合。这些发现表明,至少两个不同的位点,均位于D1Ig区域内,参与LIF与gp190的结合,更普遍地说,这些受体上的配体结合位点很可能位于经典CBD之外。
