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首页> 外文期刊>RSC Advances >Molecules with O-acetyl group protect protein glycation by acetylating lysine residues
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Molecules with O-acetyl group protect protein glycation by acetylating lysine residues

机译:用乙酰丙氨酸残留物保护蛋白质甘露出的分子

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摘要

Pharmaceutical intervention for reduction of advanced glycation end products (AGEs) is considered as a therapeutic strategy to attenuate the pathogenesis of diabetes. Many molecules have been reported to possess antiglycation activity, one such example is acetylsalicylic acid (aspirin). It protects proteins from glycation by acetylating the lysine residues. Therefore, in this study we have synthesized and screened molecules containing free N -acetyl, O -acetyl and acetophenone groups. All the selected molecules in this study showed glycation inhibition but interestingly, only molecules with O -acetyl but not N -acetyl and acetophenone groups were capable of acetylating lysine residue. Furthermore, we have demonstrated that pre-acetylation or aspirin treatment prior to the induction of diabetes helps in reducing HbA1c and AGE formation in the streptozotocin induced diabetic mice. Hence pre-acetylation may have an additional therapeutic efficacy of reducing AGE levels in vivo . Incorporation of O -acetyl group into anti-diabetic molecules could be a useful strategy, as it may have an additive effect in reducing AGEs. Identification of such novel acetylating agents represents a new area in the drug discovery process.
机译:用于减少晚期糖化末端产品(年龄)的药物干预被认为是患有糖尿病发病机制的治疗策略。已经报道了许多分子具有抗饱和活性,这样的实施例是乙酰胱氨酸(阿司匹林)。它通过乙酰化赖氨酸残基来保护蛋白质免受糖化。因此,在该研究中,我们已经合成和筛选的含有游离N-乙酰基,O-乙酰基和苯乙酮基团的分子。本研究中的所有选定的分子显示出糖化抑制但有趣的是,只有具有O-乙酰基但不是N-乙酰基和乙酮基团的分子能够致乙酰化赖氨酸残基。此外,我们已经证明,在诱导糖尿病之前在诱导糖尿病之前的预乙酰化或阿司匹林治疗有助于减少链脲佐菌素诱导的糖尿病小鼠的HBA1C和年龄形成。因此,预乙酰化可具有减少体内年龄水平的额外治疗效果。将O-乙酰基掺入抗糖尿病分子中可能是一种有用的策略,因为它可能在还原年龄中具有添加剂效应。鉴定这种新型乙酰化试剂代表了药物发现过程中的新区域。

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