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Septins are protein filaments forming the cytoskeleton along with the microtubules, microfilaments, intermediate filaments, and other accessory proteins. In 1971 while studying the cell division cycle in mutant Saccharomyces cerevisiae Harwell et al. first identified the septin-related genes playing a crucial role in yeast cytokinesis. Fluorescence microscopy revealed that these proteins localize at the budding neck as rings. These ring-like proteins were then named Septins by John Pringle, and the characterization of these highly conserved cytoskeletal proteins began in the 1980s.

Structure and formation of Septins

Septin monomers can be broadly divided into a variable N-terminal domain, a GTP hydrolyzing domain, and a coiled-coil C-terminal domain. The GTP-binding domain consists of three GTP binding motifs, first G1 or P-loop or Walker A box; second the G3 Switch II and the third G4 for selective binding of GTP. The GTP binding domain ends in a septin unique region (SUR), which comprises 50 amino acid residues and is responsible for helping in septin filament formation.

Classification of Septins

The type and number of septins vary among different organisms. For example, S. cerevisiae has seven, while humans have thirteen. Based on protein sequence similarity, septins are classified into four groups: SEPT2, SEPT3, SEPT6, and SEPT7. In humans, group SEPT2 comprises SEPT1, SEPT2, SEPT4, and SEPT5; group SEPT3 has SEPT3, SEPT9, and SEPT 12; group SEPT6 has SEPT6, SEPT8, SEPT10, and SEPT11; and lastly, group SEPT7 only has SEPT7.

Tags
SeptinsProtein FilamentsCytoskeletonMicrotubulesMicrofilamentsIntermediate FilamentsAccessory ProteinsCell Division CycleMutant Saccharomyces CerevisiaeYeast CytokinesisFluorescence MicroscopyBudding NeckRingsJohn PringleHighly Conserved Cytoskeletal ProteinsN terminal DomainGTP Hydrolyzing DomainCoiled coil C terminal DomainGTP Binding MotifsSeptin Unique Region SURSeptin Filament FormationClassification Of SeptinsSEPT2SEPT3SEPT6SEPT7

来自章节 26:

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26.18 : Septins

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26.1 : 微管

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26.2 : 微管不稳定

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26.3 : 微管形成

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26.4 : 微管相关蛋白 (MAP)

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26.5 : 微管不稳定

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26.6 : 微管相关运动蛋白

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26.7 : 细胞器和囊泡的运动

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26.8 : 复杂微管结构的组装

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26.9 : 细胞运动中的微管

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26.10 : 睫状运动机制

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26.11 : 信号转导中的微管

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26.12 : 稳定微管的药物

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26.13 : 破坏微管稳定的药物

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26.14 : 中间细丝的结构

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