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首页> 外文期刊>European Journal of Pediatrics >Rab proteins and Rab-associated proteins: major actors in the mechanism of protein-trafficking disorders
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Rab proteins and Rab-associated proteins: major actors in the mechanism of protein-trafficking disorders

机译:Rab蛋白和Rab相关蛋白:蛋白贩运障碍机制中的主要角色

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摘要

Ras-associated binding (Rab) proteins and Rab-associated proteins are key regulators of vesicle transport, which is essential for the delivery of proteins to specific intracellular locations. More than 60 human Rab proteins have been identified, and their function has been shown to depend on their interaction with different Rab-associated proteins regulating Rab activation, post-translational modification and intracellular localization. The number of known inherited disorders of vesicle trafficking due to Rab cycle defects has increased substantially during the past decade. This review describes the important role played by Rab proteins in a number of rare monogenic diseases as well as common multifactorial human ones. Although the clinical phenotype in these monogenic inherited diseases is highly variable and dependent on the type of tissue in which the defective Rab or its associated protein is expressed, frequent features are hypopigmentation (Griscelli syndrome), eye defects (Choroideremia, Warburg Micro syndrome and Martsolf syndrome), disturbed immune function (Griscelli syndrome and Charcot–Marie–Tooth disease) and neurological dysfunction (X-linked non-specific mental retardation, Charcot–Marie–Tooth disease, Warburg Micro syndrome and Martsolf syndrome). There is also evidence that alterations in Rab function play an important role in the progression of multifactorial human diseases, such as infectious diseases and type 2 diabetes. Rab proteins must not only be bound to GTP, but they need also to be ‘prenylated’—i.e. bound to the cell membranes by isoprenes, which are intermediaries in the synthesis of cholesterol (e.g. geranyl geranyl or farnesyl compounds). This means that isoprenylation can be influenced by drugs such as statins, which inhibit isoprenylation, or biphosphonates, which inhibit that farnesyl pyrophosphate synthase necessary for Rab GTPase activity. Conclusion: Although protein-trafficking disorders are clinically heterogeneous and represented in almost every subspeciality of pediatrics, the identification of common pathogenic mechanisms may provide a better diagnosis and management of patients with still unknown Rab cycle defects and stimulate the development of therapeutic agents.
机译:Ras相关的结合(Rab)蛋白和Rab相关的蛋白是囊泡运输的关键调节器,这对于将蛋白递送到特定的细胞内位置至关重要。已鉴定出60多种人类Rab蛋白,其功能已显示出其与调节Rab活化,翻译后修饰和细胞内定位的不同Rab相关蛋白的相互作用。在过去的十年中,由于Rab循环缺陷导致的已知的囊泡运输的遗传性疾病的数量大大增加了。这篇综述描述了Rab蛋白在许多罕见的单基因疾病以及常见的多因素人类疾病中的重要作用。尽管这些单基因遗传疾病的临床表型高度可变,并取决于表达有缺陷的Rab或其相关蛋白的组织类型,但常见的特征是色素沉着不足(格里切利综合征),眼部缺陷(脉络膜血症,Warburg Micro综合征和Martsolf)综合征),免疫功能紊乱(Griscelli综合征和Charcot–Marie–Tooth疾病)和神经功能障碍(X连锁非特异性智力低下,Charcot–Marie–Tooth疾病,Warburg Micro综合征和Martsolf综合征)。也有证据表明,Rab功能的改变在多因素人类疾病(例如传染病和2型糖尿病)的进展中起着重要作用。 Rab蛋白不仅必须与GTP结合,而且还需要被“异戊二烯化”。异戊二烯结合到细胞膜上,异戊二烯是胆固醇合成中的中介(例如,香叶基香叶基或法呢基化合物)。这意味着异戊二烯化可以受到抑制他异戊烯化的他汀类药物或抑制Rab GTPase活性必需的法呢基焦磷酸合酶的双膦酸酯的影响。结论:尽管蛋白贩运障碍在临床上是异质性的,并且在儿科的几乎每个亚专业中均存在,但对常见致病机制的鉴定可以为仍未知的Rab周期缺陷患者提供更好的诊断和治疗,并刺激治疗剂的发展。

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