Gardberg Anna S, Dice Lezlee T, Ou Susan, Rich Rebecca L, Helmbrecht Elizabeth, Ko Jan, Wetzel Ronald, Myszka David G, Patterson Paul H, Dealwis Chris
Department of Biochemistry and Cellular and Molecular Biology, University of Tennessee, Knoxville, TN 37996, USA.
Proc Natl Acad Sci U S A. 2007 Oct 2;104(40):15659-64. doi: 10.1073/pnas.0705888104. Epub 2007 Sep 25.
Amyloid aggregates of the amyloid-beta (Abeta) peptide are implicated in the pathology of Alzheimer's disease. Anti-Abeta monoclonal antibodies (mAbs) have been shown to reduce amyloid plaques in vitro and in animal studies. Consequently, passive immunization is being considered for treating Alzheimer's, and anti-Abeta mAbs are now in phase II trials. We report the isolation of two mAbs (PFA1 and PFA2) that recognize Abeta monomers, protofibrils, and fibrils and the structures of their antigen binding fragments (Fabs) in complex with the Abeta(1-8) peptide DAEFRHDS. The immunodominant EFRHD sequence forms salt bridges, hydrogen bonds, and hydrophobic contacts, including interactions with a striking WWDDD motif of the antigen binding fragments. We also show that a similar sequence (AKFRHD) derived from the human protein GRIP1 is able to cross-react with both PFA1 and PFA2 and, when cocrystallized with PFA1, binds in an identical conformation to Abeta(1-8). Because such cross-reactivity has implications for potential side effects of immunotherapy, our structures provide a template for designing derivative mAbs that target Abeta with improved specificity and higher affinity.
β-淀粉样蛋白(Aβ)肽的淀粉样聚集体与阿尔茨海默病的病理过程有关。抗Aβ单克隆抗体(mAb)在体外和动物研究中已显示可减少淀粉样斑块。因此,正在考虑采用被动免疫疗法治疗阿尔茨海默病,抗Aβ mAb目前正处于II期试验阶段。我们报告了两种识别Aβ单体、原纤维和纤维的mAb(PFA1和PFA2)的分离情况,以及它们与Aβ(1-8)肽DAEFRHDS形成复合物的抗原结合片段(Fab)的结构。免疫显性的EFRHD序列形成盐桥、氢键和疏水相互作用,包括与抗原结合片段引人注目的WWDDD基序的相互作用。我们还表明,源自人类蛋白GRIP1的类似序列(AKFRHD)能够与PFA1和PFA2发生交叉反应,并且在与PFA1共结晶时,以与Aβ(1-8)相同的构象结合。由于这种交叉反应对免疫疗法的潜在副作用有影响,我们的结构为设计靶向Aβ的具有更高特异性和亲和力的衍生mAb提供了模板。
