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首页> 外文期刊>Acta Biochimica Polonica >Kinetic and thermodynamic characterization of the interactions between the components of human plasma kinin-forming system and isolated and purified cell wall proteins of Candida albicans
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Kinetic and thermodynamic characterization of the interactions between the components of human plasma kinin-forming system and isolated and purified cell wall proteins of Candida albicans

机译:人体血浆激肽形成系统各成分与白色念珠菌分离纯化细胞壁相互作用的动力学和热力学表征

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Cell wall proteins of Candida albicans, besides their best known role in the adhesion of this fungal pathogen to host's tissues, also bind some soluble proteins, present in body fluids and involved in maintaining the biochemical homeostasis of the human organism. In particular, three plasma factors - high-molecular-mass kininogen (HK), factor XII (FXII) and prekallikrein (PPK) - have been shown to adhere to candidal cells. These proteins are involved in the surface-contact-catalyzed production of bradykinin-related peptides (kinins) that contribute to inflammatory states associated with microbial infections. We recently identified several proteins, associated with the candidal cell walls, and probably involved in the binding of HK. In our present study, a list of potential FXII-and PPK-binding proteins was proposed, using an affinity selection (on agarose-coupled FXII or PPK) from a whole mixture of beta-1,3-glucanase-extrated cell wall-associated proteins and the mass-spectrometry protein identification. Five of these fungal proteins, including agglutinin-like sequence protein 3 (Als3), triosephosphate isomerase 1 (Tpi1), enolase 1 (Eno1), phosphoglycerate mutase 1 (Gpm1) and glucose-6-phosphate isomerase 1 (Gpi1), were purified and characterized in terms of affinities to the human contact factors, using the surface plasmon resonance measurements. Except Gpm1 that bound only PPK, and Als3 that exhibited an affinity to HK and FXII, the other isolated proteins interacted with all three contact factors. The determined dissociation constants for the identified protein complexes were of 10(-7) M order, and the association rate constants were in a range of 10(4)-10(5) M(-1)s(-1). The identified fungal pathogen-host protein interactions are potential targets for novel anticandidal therapeutic approaches.
机译:白色念珠菌的细胞壁蛋白除了在这种真菌病原体与宿主组织的粘附中最广为人知的作用外,还与体液中存在的一些可溶性蛋白结合,并参与维持人体生物化学的稳态。特别是,三种血浆因子-高分子激肽原(HK),XII因子(FXII)和激肽释放酶(PPK)-已显示粘附于候选细胞。这些蛋白质参与缓激肽相关肽(激肽)的表面接触催化生产,激肽相关肽(激肽)促成与微生物感染相关的炎症状态。我们最近鉴定了几种与候选细胞壁相关的蛋白质,可能与HK的结合有关。在我们目前的研究中,提出了一系列潜在的FXII和PPK结合蛋白,使用的亲和力选择(在琼脂糖偶联的FXII或PPK上)是从与β-1,3-葡聚糖酶延伸的细胞壁相关的整个混合物中进行的。蛋白质和质谱蛋白质鉴定。纯化了其中的5种真菌蛋白,包括凝集素样序列蛋白3(Als3),磷酸三糖异构酶1(Tpi1),烯醇酶1(Eno1),磷酸甘油酸突变酶1(Gpm1)和葡萄糖6-磷酸异构酶1(Gpi1)。并使用表面等离振子共振测量法根据对人体接触因子的亲和力进行表征。除了仅结合PPK的Gpm1和对HK和FXII表现出亲和力的Als3,其他分离的蛋白质均与所有三个接触因子相互作用。所确定的蛋白质复合物的解离常数为10(-7)M阶,缔合速率常数为10(4)-10(5)M(-1)s(-1)。鉴定出的真菌病原体-宿主蛋白相互作用是新型抗候选治疗方法的潜在目标。

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