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Photodegradation illuminates the role of polyanions in prion infectivity

机译:光降解阐明了聚阴离子在病毒感染性中的作用

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摘要

Understanding the mechanism by which prion infectivity is encoded by the misfolded protein PrP Sc remains a high priority within the prion field. Work from several groups has indicated cellular cofactors may be necessary to form infectious prions in vitro. The identity of endogenous prion conversion cofactors is currently unknown, but may include polyanions and/or lipid molecules. In a recent study, we manufactured infectious hamster prions containing purified PrP Sc, co-purified lipid and a synthetic photocleavable polyanion. The polyanion was incorporated into infectious PrP Sc complexes and then specifically degraded by exposure to ultraviolet light. Light-induced in situ degradation of the incorporated polyanion had no effect on the specific infectivity of the samples as determined by end-point dilution sPMCA and scrapie incubation time assays. Furthermore, prion strain properties were not changed by polyanion degradation, suggesting that intact polyanions are not required to maintain the infectious properties of hamster prions. Here, we review these results and discuss the potential roles cofactors might play in encoding prion infectivity and/or strain properties.
机译:理解由错误折叠的蛋白质PrP Sc编码病毒感染性的机制仍然是the病毒领域的高度优先事项。来自几个小组的研究表明,细胞辅因子可能是体外形成感染性病毒所必需的。内源性pr病毒转化辅助因子的身份目前未知,但可能包括聚阴离子和/或脂质分子。在最近的研究中,我们制造了含有纯化的PrP Sc,共纯化的脂质和合成的可光裂解的聚阴离子的传染性仓鼠pr病毒。将该聚阴离子掺入感染性PrP Sc复合物中,然后通过暴露于紫外光而特异性降解。通过端点稀释sPMCA和瘙痒病温育时间测定法测定,掺入的聚阴离子的光诱导原位降解对样品的比传染性没有影响。此外,poly蛋白的应变特性不会因聚阴离子的降解而改变,这表明完整的聚阴离子不需要保持仓鼠病毒的感染性。在这里,我们回顾这些结果,并讨论辅因子在编码病毒感染性和/或菌株特性中可能发挥的潜在作用。

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