University of Bordeaux, F-33000, Bordeaux, France.
CNRS, Interdisciplinary Institute for Neuroscience, UMR 5297, F-33000, Bordeaux, France.
Nat Commun. 2019 Oct 1;10(1):4462. doi: 10.1038/s41467-019-12434-9.
During clathrin mediated endocytosis (CME), the concerted action of dynamin and its interacting partners drives membrane scission. Essential interactions occur between the proline/arginine-rich domain of dynamin (dynPRD) and the Src-homology domain 3 (SH3) of various proteins including amphiphysins. Here we show that multiple SH3 domains must bind simultaneously to dynPRD through three adjacent motifs for dynamin's efficient recruitment and function. First, we show that mutant dynamins modified in a single motif, including the central amphiphysin SH3 (amphSH3) binding motif, partially rescue CME in dynamin triple knock-out cells. However, mutating two motifs largely prevents that ability. Furthermore, we designed divalent dynPRD-derived peptides. These ligands bind multimers of amphSH3 with >100-fold higher affinity than monovalent ones in vitro. Accordingly, dialyzing living cells with these divalent peptides through a patch-clamp pipette blocks CME much more effectively than with monovalent ones. We conclude that dynamin drives vesicle scission via multivalent interactions in cells.
在网格蛋白介导的胞吞作用(CME)中,动力蛋白及其相互作用的伙伴的协同作用驱动膜的断裂。动力蛋白富含脯氨酸/精氨酸的结构域(dynPRD)与各种蛋白的Src 同源结构域 3(SH3)之间发生必需的相互作用,包括 amphiphysins。在这里,我们表明,多个 SH3 结构域必须通过三个相邻的基序同时结合到 dynPRD 上,才能使动力蛋白有效招募和发挥作用。首先,我们表明,单个基序(包括中央 amphiphysin SH3(amphSH3)结合基序)发生突变的动力蛋白,可部分挽救 dynamin 三重敲除细胞中的 CME。然而,突变两个基序在很大程度上阻止了这种能力。此外,我们设计了二价 dynPRD 衍生肽。这些配体在体外与 amphSH3 多聚体的结合亲和力比单价肽高 100 多倍。因此,通过膜片钳管内灌流将这些二价肽注入活细胞中,比使用单价肽更有效地阻断 CME。我们的结论是,动力蛋白通过细胞中的多价相互作用驱动囊泡的断裂。
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