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Architecture of the IFT ciliary trafficking machinery and interplay between its components
Authors:Kazuhisa Nakayama  Yohei Katoh
Institution:1. Graduate School of Pharmaceutical Sciences, Kyoto University, Kyoto, Japankazunaka@pharm.kyoto-u.ac.jp;3. Graduate School of Pharmaceutical Sciences, Kyoto University, Kyoto, Japan
Abstract:Abstract

Cilia and flagella serve as cellular antennae and propellers in various eukaryotic cells, and contain specific receptors and ion channels as well as components of axonemal microtubules and molecular motors to achieve their sensory and motile functions. Not only the bidirectional trafficking of specific proteins within cilia but also their selective entry and exit across the ciliary gate is mediated by the intraflagellar transport (IFT) machinery with the aid of motor proteins. The IFT-B complex, which is powered by the kinesin-2 motor, mediates anterograde protein trafficking from the base to the tip of cilia, whereas the IFT-A complex together with the dynein-2 complex mediates retrograde protein trafficking. The BBSome complex connects ciliary membrane proteins to the IFT machinery. Defects in any component of this trafficking machinery lead to abnormal ciliogenesis and ciliary functions, and results in a broad spectrum of disorders, collectively called the ciliopathies. In this review article, we provide an overview of the architectures of the components of the IFT machinery and their functional interplay in ciliary protein trafficking.
Keywords:Cilia  ciliopathy  BBSome  dynein-2  IFT-A  IFT-B  kinesin-2
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