Buchholz C J, Koller D, Devaux P, Mumenthaler C, Schneider-Schaulies J, Braun W, Gerlier D, Cattaneo R
Institut für Molekularbiologie, Abt.I, Universität Zürich, Hönggerberg, CH-8093 Zürich, Switzerland.
J Biol Chem. 1997 Aug 29;272(35):22072-9. doi: 10.1074/jbc.272.35.22072.
The measles virus (MV) hemagglutinin binds to the complement control protein (CCP) CD46 primarily through the two external modules, CCP-I and -II. To define the residues involved in binding, 40 amino acids predicted to be solvent-exposed on the CCP-I-II module surface were changed to either alanine or serine. Altered proteins were expressed on the cell surface, and their abilities to bind purified MV particles, a soluble form of hemagglutinin (sH) and nine CD46-specific antibodies competing to different levels with sH attachment, were measured. All proteins retained, at least in part, MV and sH binding, but some completely lost binding to certain antibodies. Amino acids essential for binding of antibodies weakly or moderately competing with sH attachment are situated in the membrane-distal tip of CCP-I, whereas residues involved in binding of strongly sH competing antibodies cluster in the center of CCP-I (Arg-25, Asp-27) or in CCP-II (Arg-69, Asp-70). Both clusters face the same side of CCP-I-II and map close to amino acid exchanges impairing sH binding (E11A, R29A, P39A, and D70A) or MV binding (D70A and E84A) and to a six-amino acid loop, previously shown to be necessary for sH binding.
麻疹病毒(MV)血凝素主要通过两个外部模块,即补体控制蛋白(CCP)CCP-I和- II与补体控制蛋白CD46结合。为了确定参与结合的残基,将预测在CCP-I-II模块表面暴露于溶剂中的40个氨基酸替换为丙氨酸或丝氨酸。改变后的蛋白质在细胞表面表达,并测量它们结合纯化的MV颗粒、可溶性血凝素形式(sH)以及与sH附着有不同程度竞争的九种CD46特异性抗体的能力。所有蛋白质至少部分保留了与MV和sH的结合,但有些完全失去了与某些抗体的结合。与sH附着有弱或中等程度竞争的抗体结合所必需的氨基酸位于CCP-I的膜远端末端,而与sH有强烈竞争的抗体结合所涉及的残基聚集在CCP-I的中心(Arg-25、Asp-27)或CCP-II中(Arg-69、Asp-70)。这两个簇都面向CCP-I-II的同一侧,并且映射到靠近损害sH结合(E11A、R29A、P39A和D70A)或MV结合(D70A和E84A)的氨基酸交换处,以及一个先前显示对sH结合必需的六氨基酸环附近。
