首页> 外文OA文献 >PpATG9 Encodes a Novel Membrane Protein That Traffics to Vacuolar Membranes, Which Sequester Peroxisomes during Pexophagy in Pichia pastoris
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PpATG9 Encodes a Novel Membrane Protein That Traffics to Vacuolar Membranes, Which Sequester Peroxisomes during Pexophagy in Pichia pastoris

机译:PpATG9编码一种新型的膜蛋白,该膜蛋白可以运输到液泡膜,该膜在毕赤酵母的排脓过程中会隔离过氧化物酶体。

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摘要

When Pichia pastoris adapts from methanol to glucose growth, peroxisomes are rapidly sequestered and degraded within the vacuole by micropexophagy. During micropexophagy, sequestering membranes arise from the vacuole to engulf the peroxisomes. Fusion of the sequestering membranes and incorporation of the peroxisomes into the vacuole is mediated by the micropexophagy-specific membrane apparatus (MIPA). In this study, we show the P. pastoris ortholog of Atg9, a novel membrane protein is essential for the formation of the sequestering membranes and assembly of MIPA. During methanol growth, GFP-PpAtg9 localizes to multiple structures situated near the plasma membrane referred as the peripheral compartment (Atg9-PC). On glucose-induced micropexophagy, PpAtg9 traffics from the Atg9-PC to unique perivacuolar structures (PVS) that contain PpAtg11, but lack PpAtg2 and PpAtg8. Afterward, PpAtg9 distributes to the vacuole surface and sequestering membranes. Movement of the PpAtg9 from the Atg9-PC to the PVS requires PpAtg11 and PpVps15. PpAtg2 and PpAtg7 are essential for PpAtg9 trafficking from the PVS to the vacuole and sequestering membranes, whereas trafficking of PpAtg9 proceeds independent of PpAtg1, PpAtg18, and PpVac8. In summary, our data suggest that PpAtg9 transits from the Atg9-PC to the PVS and then to the sequestering membranes that engulf the peroxisomes for degradation.
机译:当巴斯德毕赤酵母(Pichia pastoris)从甲醇适应葡萄糖生长时,过氧化物酶体很快被螯合,并通过微pexophagyy在液泡中降解。在微咽病期间,隔离膜从液泡中产生以吞噬过氧化物酶体。隔离膜的融合和过氧化物酶体掺入液泡是由微石蜡特异性膜装置(MIPA)介导的。在这项研究中,我们显示了Atg9的巴斯德毕赤酵母,一种新型的膜蛋白,对隔离膜的形成和MIPA的组装至关重要。在甲醇生长过程中,GFP-PpAtg9定位于质膜附近的多个结构,称为外围区室(Atg9-PC)。在葡萄糖引起的微咽病中,PpAtg9从Atg9-PC转运到包含PpAtg11但缺乏PpAtg2和PpAtg8的独特的周囊结构(PVS)。之后,PpAtg9分布到液泡表面和隔离膜。 PpAtg9从Atg9-PC到PVS的移动需要PpAtg11和PpVps15。 PpAtg2和PpAtg7对于PpAtg9从PVS到液泡和隔离膜的运输至关重要,而PpAtg9的运输独立于PpAtg1,PpAtg18和PpVac8。总而言之,我们的数据表明PpAtg9从Atg9-PC转移到PVS,然后转移到吞噬过氧化物酶体降解的螯合膜。

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