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首页> 外文期刊>Biomacromolecules >Guanidino- and Urea-Modified Dendrimers as Potent Solubilizers of Misfolded Prion Protein Aggregates under Non-cytotoxic Conditions. Dependence on Dendrimer Generation and Surface Charge
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Guanidino- and Urea-Modified Dendrimers as Potent Solubilizers of Misfolded Prion Protein Aggregates under Non-cytotoxic Conditions. Dependence on Dendrimer Generation and Surface Charge

机译:胍基和尿素修饰的树状聚合物作为有效的增溶剂,在非细胞毒性条件下折叠的Protein病毒蛋白质聚集体。依赖于树状大分子的生成和表面电荷

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摘要

Amino-terminated dendrimers are well-defined synthetic hyperbranched polymers and have previously been shown to destabilize aggregates of the misfolded, pathogenic, and partially protease-resistant form of the prion protein (PrP~(Sc)), transforming it into a partially dissociated, protease-sensitive form with strongly reduced infectivity. The mechanism behind this is not known, but a low pH, creating multiple positively charged primary amines on the dendrimer surface, increases the efficiency of the reaction. In the present study, surface amines of the dendrimers were modified to yield either guanidino surface groups (being positively charged at neutral pH) or urea groups (uncharged). The ability of several generations of modified dendrimers and unmodified amino-terminated dendrimers to deplete PrP~(Sc) from persistently PrP~(Sc)-infected cells in culture (SMB cells) was studied. It was found that destabilization correlated with both the generation number of the dendrimer, with higher generations being more efficient, and the charge density of the surface groups. Urea-decorated dendrimers having an uncharged surface were less efficient than positively charged unmodified- (amino) and guanidino-modified dendrimers. The most efficient dendrimers (generation 4 (G4) and G5-unmodified and guanidino dendrimers) cleared PrP~(Sc) completely by incubation for 4 days at less than 50 nM. In contrast to both unmodified and guanidine-modified dendrimers, the uncharged urea dendrimers showed much lower cytotoxicity toward noninfected SMB cells. Therapeutic uses of modified dendrimers are indicated by the low concentrations of dendrimers needed.
机译:氨基封端的树枝状聚合物是定义明确的合成超支化聚合物,先前已证明可以使the蛋白(PrP〜(Sc))的错误折叠,致病性和部分蛋白酶抗性形式的聚集体不稳定,将其转变为部分解离的,蛋白酶敏感性形式,传染性大大降低。其背后的机制尚不清楚,但低pH值会在树枝状聚合物表面上生成多个带正电荷的伯胺,从而提高了反应效率。在本研究中,对树枝状聚合物的表面胺进行改性,以产生胍基表面基团(在中性pH下带正电荷)或脲基团(不带电荷)。研究了几代修饰的树状聚合物和未修饰的氨基末端树状聚合物从培养物中持续感染PrP〜(Sc)的细胞(SMB细胞)中消耗PrP〜(Sc)的能力。发现去稳定化与树枝状大分子的生成数和高效率的生成以及表面基团的电荷密度有关。具有不带电表面的尿素修饰的树枝状聚合物的效率低于带正电荷的未修饰的(氨基)和胍基修饰的树枝状聚合物。最有效的树状聚合物(第4代(G4)和G5未修饰的和胍基树状聚合物)通过在低于50 nM的温度下孵育4天完全清除了PrP〜(Sc)。与未修饰的和胍修饰的树状聚合物相反,未带电荷的脲树状聚合物对未感染的SMB细胞显示出低得多的细胞毒性。所需的低树枝状聚合物浓度表明了改性树枝状聚合物的治疗用途。

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