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Protein kinase A signalling in ' Schistosoma mansoni ' cercariae and udschistosomules

机译:'曼氏血吸虫'尾蚴中的蛋白激酶a信号传导和 ud血吸虫童虫

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摘要

Cyclic AMP (cAMP)-dependent protein kinase/protein kinase A regulates multiple processes in eukaryotes by phosphorylating diverse cellular substrates, including metabolic and signalling enzymes, ion channels and transcription factors. Here we provide insight into protein kinase A signalling in cercariae and 24h in vitro cultured somules of the blood parasite, Schistosoma mansoni, which causes human intestinal schistosomiasis. Functional mapping of activated protein kinase A using anti-phospho protein kinase A antibodies and confocal laser scanning microscopy revealed activated protein kinase A in the central and peripheral nervous system, oral-tip sensory papillae, oesophagus and excretory system of intact cercariae. Cultured 24h somules, which biologically represent the skin-resident stage of the parasite, exhibited similar activation patterns in oesophageal and nerve tissues but also displayed striking activation at the tegument and activation in a region resembling the germinal 'stem' cell cluster. The adenylyl cyclase activator, forskolin, stimulated somule protein kinase A activation and produced a hyperkinesia phenotype. The biogenic amines, serotonin and dopamine known to be present in skin also induced protein kinase A activation in somules, whereas neuropeptide Y or [Leu31,Pro34]-neuropeptide Y attenuated protein kinase A activation. However, neuropeptide Y did not block the forskolin-induced somule hyperkinesia. Bioinformatic investigation of potential protein associations revealed 193 medium confidence and 59 high confidence protein kinase A interacting partners in S. mansoni, many of which possess putative protein kinase A phosphorylation sites. These data provide valuable insight into the intricacies of protein kinase A signalling in S. mansoni and a framework for further physiological investigations into the roles of protein kinase A in schistosomes, particularly in the context of interactions between the parasite and the host.
机译:依赖于环AMP(cAMP)的蛋白激酶/蛋白激酶A通过磷酸化各种细胞底物(包括代谢和信号传导酶,离子通道和转录因子)来调节真核生物中的多个过程。在这里,我们提供了对尾c中的蛋白激酶A信号的深入了解,以及24小时体外培养的血寄生虫曼氏血吸虫(曼氏血吸虫病)菌群,它可导致人类肠道血吸虫病。使用抗磷酸化蛋白激酶A抗体和共​​聚焦激光扫描显微镜对活化蛋白激酶A进行功能作图,揭示了活化蛋白激酶A在中尾神经的口腔中枢神经系统,口腔感觉乳头,食道和排泄系统中。在生物学上代表寄生虫的皮肤停留阶段的培养的24h菌在食道和神经组织中表现出相似的活化模式,但在外皮处表现出惊人的活化,并在类似于生“茎”细胞簇的区域表现出活化。腺苷酸环化酶激活剂forskolin刺激了somule蛋白激酶A的激活并产生了运动亢进的表型。已知存在于皮肤中的生物胺,5-羟色胺和多巴胺也会诱导蛋白质激酶A的激活,而神经肽Y或[Leu31,Pro34]-神经肽Y会减弱蛋白激酶A的激活。但是,神经肽Y并不能阻止毛喉素诱导的运动亢进。生物信息学研究潜在的蛋白质缔合,发现曼氏葡萄球菌中有193个中等信度和59个高信度的蛋白激酶A相互作用伴侣,其中许多具有推定的蛋白激酶A磷酸化位点。这些数据为曼氏葡萄球菌中蛋白激酶A信号的复杂性提供了有价值的见解,并为进一步生理研究蛋白激酶A在血吸虫中的作用提供了框架,尤其是在寄生虫与宿主之间相互作用的情况下。

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