The protist parasite Trypanosoma brucei is an obligate extracellular pathogen that retains its highly polarized morphology during cell division and has evolved a novel cytokinetic process independent of non-muscle myosin II. The polo-like kinase homolog TbPLK is essential for transmission of cell polarity during division and for cytokinesis. We previously identified a putative TbPLK substrate named Tip of the Extending FAZ 1 (TOEFAZ1) as an essential kinetoplastid-specific component of the T. brucei cytokinetic machinery. We performed a proximity-dependent biotinylation identification (BioID) screen using TOEFAZ1 as a means to identify additional proteins that are involved in cytokinesis. Using quantitative proteomic methods, we identified nearly 500 TOEFAZ1-proximal proteins and characterized 59 in further detail. Among the candidates, we identified an essential putative phosphatase that regulates the expression level and localization of both TOEFAZ1 and TbPLK, a previously uncharacterized protein that is necessary for the assembly of a new cell posterior, and a microtubule plus-end directed orphan kinesin that is required for completing cleavage furrow ingression. The identification of these proteins provides new insight into T. brucei cytokinesis and establishes TOEFAZ1 as a key component of this essential and uniquely configured process in kinetoplastids.
Identification of TOEFAZ1-interacting proteins reveals key regulators of Trypanosoma brucei cytokinesis.
TOEFAZ1 相互作用蛋白的鉴定揭示了布氏锥虫胞质分裂的关键调节因子
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作者:Hilton Nicholas A, Sladewski Thomas E, Perry Jenna A, Pataki Zemplen, Sinclair-Davis Amy N, Muniz Richard S, Tran Holly L, Wurster Jenna I, Seo Jiwon, de Graffenried Christopher L
| 期刊: | Molecular Microbiology | 影响因子: | 2.600 |
| 时间: | 2018 | 起止号: | 2018 Aug;109(3):306-326 |
| doi: | 10.1111/mmi.13986 | 研究方向: | 免疫/内分泌 |
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