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Super-resolution microscopy reveals majorly mono- and dimeric presenilin1/γ-secretase at the cell surface

机译:超分辨率显微镜显示在细胞表面上的主要单 - 和二聚体预衰老1 /γ分泌酶

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摘要

γ-Secretase is a multi-subunit enzyme whose aberrant activity is associated with Alzheimer’s disease and cancer. While its structure is atomically resolved, γ-secretase localization in the membrane in situ relies mostly on biochemical data. Here, we combined fluorescent tagging of γ-secretase subunits with super-resolution microscopy in fibroblasts. Structured illumination microscopy revealed single γ-secretase complexes with a monodisperse distribution and in a 1:1 stoichiometry of PSEN1 and nicastrin subunits. In living cells, sptPALM revealed PSEN1/γ-secretase mainly with directed motility and frequenting ‘hotspots’ or high track-density areas that are sensitive to γ-secretase inhibitors. We visualized γ-secretase association with substrates like amyloid precursor protein and N-cadherin, but not with its sheddases ADAM10 or BACE1 at the cell surface, arguing against pre-formed megadalton complexes. Nonetheless, in living cells PSEN1/γ-secretase transiently visits ADAM10 hotspots. Our results highlight the power of super-resolution microscopy for the study of γ-secretase distribution and dynamics in the membrane.
机译:γ-分泌酶是一种多亚基酶,其异常活性与阿尔茨海默病和癌症有关。虽然其结构是原子解析的,但原位膜中的γ-分泌酶定位主要依赖于生物化学数据。这里,我们将γ-分泌酶亚基的荧光标记与成纤维细胞中的超分辨率显微镜组合。结构化照明显微镜显示单分散分布的单γ-分泌酶复合物,在PSEN1和Nicastrin亚基的1:1化学计量中。在活细胞中,SPTPALM揭示了PSEN1 /γ-分泌酶,主要是针对γ-分泌酶抑制剂敏感的指向运动和频繁的“热点”或高轨道密度区域。我们与淀粉样蛋白前体蛋白和N-钙粘蛋白等底物相关的γ-分泌酶联合,但在细胞表面上没有用其脱落剂ADAM10或BACE1,反对预形成的Megadalton复合物。尽管如此,在活细胞中,PSEN1 /γ-分泌酶瞬时访问ADAM10热点。我们的结果突出了超分辨率显微镜的功率,以研究膜中γ-分泌酶分布和动力学的研究。

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