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首页> 外文期刊>Biomolecules >Molecular Recognition of PTS-1 Cargo Proteins by Pex5p: Implications for Protein Mistargeting in Primary Hyperoxaluria
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Molecular Recognition of PTS-1 Cargo Proteins by Pex5p: Implications for Protein Mistargeting in Primary Hyperoxaluria

机译:Pex5p对PTS-1货运蛋白质的分子识别:对原发性高草酸尿症的蛋白质误靶的影响。

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摘要

Peroxisomal biogenesis and function critically depends on the import of cytosolic proteins carrying a PTS1 sequence into this organelle upon interaction with the peroxin Pex5p. Recent structural studies have provided important insights into the molecular recognition of cargo proteins by Pex5p. Peroxisomal import is a key feature in the pathogenesis of primary hyperoxaluria type 1 (PH1), where alanine:glyoxylate aminotransferase (AGT) undergoes mitochondrial mistargeting in about a third of patients. Here, we study the molecular recognition of PTS1 cargo proteins by Pex5p using oligopeptides and AGT variants bearing different natural PTS1 sequences, and employing an array of biophysical, computational and cell biology techniques. Changes in affinity for Pex5p (spanning over 3–4 orders of magnitude) reflect different thermodynamic signatures, but overall bury similar amounts of molecular surface. Structure/energetic analyses provide information on the contribution of ancillary regions and the conformational changes induced in Pex5p and the PTS1 cargo upon complex formation. Pex5p stability in vitro is enhanced upon cargo binding according to their binding affinities. Moreover, we provide evidence that the rational modulation of the AGT: Pex5p binding affinity might be useful tools to investigate mistargeting and misfolding in PH1 by pulling the folding equilibria towards the native and peroxisomal import competent state.
机译:过氧化物酶体的生物发生和功能关键取决于与过氧化物酶Pex5p相互作用时,携带带有PTS1序列的胞质蛋白进入该细胞器。最近的结构研究为Pex5p对货物蛋白质的分子识别提供了重要的见识。过氧化物酶体的导入是原发性高草酸尿症1型(PH1)发病机理的关键特征,其中约三分之一的患者丙氨酸:乙醛酸氨基转移酶(AGT)发生线粒体靶向错误。在这里,我们研究了Pex5p使用带有不同天然PTS1序列的寡肽和AGT变体对PTS1货物蛋白的分子识别,并采用了一系列生物物理,计算和细胞生物学技术。对Pex5p的亲和力变化(跨越3-4个数量级)反映了不同的热力学特征,但总体上掩埋了相似量的分子表面。结构/能量分析提供了有关复杂区域形成时Pex5p和PTS1货物中辅助区域的贡献和构象变化的信息。货物结合后,根据其结合亲和力,Pex5p的体外稳定性得到增强。此外,我们提供的证据表明,AGT:Pex5p结合亲和力的合理调节可能是有用的工具,可通过向自然和过氧化物酶体导入感受态拉动折叠平衡来研究PH1中的错误靶向和错误折叠。

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