Department of Medical Biochemistry, Membrane Receptors in Neuronal Disease (MIND) Center, University of Aarhus, OleWorms Allé, Aarhus C, Denmark.
J Biol Chem. 2010 Apr 16;285(16):12210-22. doi: 10.1074/jbc.M109.062364. Epub 2010 Feb 16.
Sortilin acts as a cell surface receptor for pro-neurotrophins (pro-NT) that upon complex formation with the p75 neurotrophin receptor (p75(NTR)) is able to signal neuronal cell death. Here we screened a sortilin peptide library comprising 16-mer overlapping sequences for binding of the pro-domains of nerve growth factor and brain-derived neurotrophic factor. We find that a linear surface-exposed sequence, (163)RIFRSSDFAKNF(174), constitutes an important pro-NT binding epitope in sortilin. Systematic mutational analysis revealed residues Arg(163), Phe(165), Arg(166), and Phe(170) to be critical for the interaction. Expression of a sortilin mutant in which these four amino acids were substituted by alanines disrupted pro-NT binding without affecting receptor heterodimerization with p75(NTR) or binding of ligands that selectively engages the centrally located tunnel in the beta-propeller of sortilin. We furthermore demonstrate that a peptide comprising the ligand-binding epitope can prevent pro-NT-induced apoptosis in RN22 schwannoma cells.
Sortilin 作为一种细胞表面受体,可与 p75 神经营养因子受体(p75(NTR))形成复合物,从而能够对神经元细胞死亡进行信号转导。在这里,我们筛选了一个由 16 个重叠序列组成的 sortilin 肽文库,以寻找与神经生长因子和脑源性神经营养因子前体结合的序列。我们发现,线性暴露于表面的序列(163)RIFRSSDFAKNF(174),构成了 sortilin 中重要的前体神经递质结合表位。系统的突变分析表明,残基 Arg(163)、Phe(165)、Arg(166)和 Phe(170)对于相互作用至关重要。表达的突变体 sortilin 中,这四个氨基酸被丙氨酸取代,破坏了前体神经递质的结合,而不影响与 p75(NTR)的受体异二聚体形成或与选择性结合 sortilin β-发夹区中央隧道的配体结合。此外,我们还证明,包含配体结合表位的肽可以防止 pro-NT 诱导的 RN22 雪旺细胞瘤细胞凋亡。
