Curved EFC/F-BAR-Domain Dimers Are Joined End to End into a Filament for Membrane Invagination in Endocytosis

Shimada, Akira; Niwa, Hideaki; Tsujita, Kazuya; Suetsugu, Shiro; Nitta, Koji; Hanawa-Suetsugu, Kyoko; Akasaka, Ryogo; Nishino, Yuri; Toyama, Motomichi; Chen, Lirong; Liu, Zhi Jie; Wang, Bi Cheng; Yamamoto, Masaki; Terada, Takaho; Miyazawa, Atsuo; Tanaka, Akiko; Sugano, Sumio; Shirouzu, Mikako; Nagayama, Kuniaki; Takenawa, Tadaomi; Yokoyama, Shigeyuki

doi:10.1016/j.cell.2007.03.040

Cited by 367 publications

(595 citation statements)

References 49 publications

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“…Here, interaction of receptors with adaptor proteins stabilise nascent clathrin-coated pits (CCPs) at random sites on the plasma membrane [3]. Growing CCPs acquire cargo and invaginate via clathrin polymerization [4] and the coordinated action of curvature-inducing/sensing BAR [5] and F-BAR domain proteins [6,7], ENTH domain proteins [8], and possibly actin [9][10][11]. The neck of the deeply invaginated CCP is severed in a mechanism involving the large GTPase dynamin [12,13], and possibly a phosphoinositide (PI) phosphatase [14], to release a clathrin-coated vesicle (CCV), which uncoats through the action of GAK/auxilin [15,16].…”

Section: Introductionmentioning

confidence: 99%

“…In a typical experiment using dual colour total internal reflection fluorescence microscopy (TIR-FM), the recruitment dynamics of fluorescent protein (FP)-tagged endocytic proteins were measured relative to the disappearance of spot-like CCPs, which was used as a fiducial marker to indicate internalization [6,18,19]. Using this strategy the recruitment dynamics of endocytic proteins were coarsely grouped into ''early'' and ''late'' relative to CCP disappearance [20] (Figure S1), but finer temporal resolution was not possible because the moment of scission, the endpoint of the invagination process, was unknown.…”

Section: Introductionmentioning

confidence: 99%

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A High Precision Survey of the Molecular Dynamics of Mammalian Clathrin-Mediated Endocytosis

Perrais²,

2011

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Dual colour total internal reflection fluorescence microscopy is a powerful tool for decoding the molecular dynamics of clathrin-mediated endocytosis (CME). Typically, the recruitment of a fluorescent protein-tagged endocytic protein was referenced to the disappearance of spot-like clathrin-coated structure (CCS), but the precision of spot-like CCS disappearance as a marker for canonical CME remained unknown. Here we have used an imaging assay based on total internal reflection fluorescence microscopy to detect scission events with a resolution of ,2 s. We found that scission events engulfed comparable amounts of transferrin receptor cargo at CCSs of different sizes and CCS did not always disappear following scission. We measured the recruitment dynamics of 34 types of endocytic protein to scission events: Abp1, ACK1, amphiphysin1, APPL1, Arp3, BIN1, CALM, CIP4, clathrin light chain (Clc), cofilin, coronin1B, cortactin, dynamin1/ 2, endophilin2, Eps15, Eps8, epsin2, FBP17, FCHo1/2, GAK, Hip1R, lifeAct, mu2 subunit of the AP2 complex, myosin1E, myosin6, NECAP, N-WASP, OCRL1, Rab5, SNX9, synaptojanin2b1, and syndapin2. For each protein we aligned ,1,000 recruitment profiles to their respective scission events and constructed characteristic ''recruitment signatures'' that were grouped, as for yeast, to reveal the modular organization of mammalian CME. A detailed analysis revealed the unanticipated recruitment dynamics of SNX9, FBP17, and CIP4 and showed that the same set of proteins was recruited, in the same order, to scission events at CCSs of different sizes and lifetimes. Collectively these data reveal the fine-grained temporal structure of CME and suggest a simplified canonical model of mammalian CME in which the same core mechanism of CME, involving actin, operates at CCSs of diverse sizes and lifetimes.

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Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

A High Precision Survey of the Molecular Dynamics of Mammalian Clathrin-Mediated Endocytosis

Perrais²,

2011

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“…Ceci est bien illustré par les fréquents treillis plats de clathrine observés à la surface de nombreuses cellules [23]. Le rôle actif de certaines protéines capables de « sculpter » la membrane plasmique a été établi [24][25][26][27]. En revanche, parmi les protéines connues ayant ces propriétés, la plupart ont un rôle tardif lors de la transition, au moment où les puits de clathrine deviennent des vésicules.…”

Section: Induction Des Vésicules De Clathrine : Le Rôle Controversé Dunclassified

“…En plus de leur capacité à se lier aux membranes, les domaines BAR ont aussi celle de sentir et d'induire une courbure chez celles-ci [26]. Les domaines F-BAR peuvent également se lier aux membranes et induire une courbure, mais, en raison de la formation d'un angle moins prononcé, ils n'induisent pas de courbure aussi extrême que celle qu'induisent les domaines BAR [27,32]. Le domaine F-BAR des protéines FCHo a une préférence pour le Pi(4,5)P 2 par rapport aux autres lipides [28], ce qui explique pourquoi ces protéines sont exclusivement recrutées à la membrane plasmique, qui est très riche en Pi(4,5)P 2 .…”

Section: Comment Les Protéines Fcho Induisent-elles La Formation Des unclassified

“…Lors d'expériences de tubulation in vitro, le domaine F-BAR de FCHo2 est capable de déformer des liposomes en tubes de diamètres allant de 130 à 18 nm selon la concentration de protéines [28]. Plusieurs autres protéines telles que l'amphi physine, SNX9, FBP17, l'endophiline et l'epsine sont impliquées dans la formation de vésicules de clathrine et ont la capacité d'induire une courbure de la membrane [25][26][27]31]. En revanche, toutes ces protéines ont un rôle plus tardif que les FCHo et n'induisent pas la nucléation des puits de clathrine.…”

Section: Comment Les Protéines Fcho Induisent-elles La Formation Des unclassified

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Initiation de l’endocytose par vésicules de clathrine

Boucrot¹,

McMahon²

2011

Med Sci (Paris)

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Endosomes

Galvez¹

2011

Cellular Domains

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Curved EFC/F-BAR-Domain Dimers Are Joined End to End into a Filament for Membrane Invagination in Endocytosis

Cited by 367 publications

References 49 publications

A High Precision Survey of the Molecular Dynamics of Mammalian Clathrin-Mediated Endocytosis

A High Precision Survey of the Molecular Dynamics of Mammalian Clathrin-Mediated Endocytosis

Initiation de l’endocytose par vésicules de clathrine

Endosomes

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