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半合成和天然类黄酮对老龄大鼠小胶质细胞丰富培养物的保护作用。

Protective Effect of Semisynthetic and Natural Flavonoid on Aged Rat Microglia-enriched Cultures.

机构信息

Center of Experimental Medicine, Institute of Experimental Pharmacology and Toxicology, Slovak Academy of Sciences, Dubravska cesta 9, 841 04, Bratislava, Slovak Republic.

出版信息

Neurotox Res. 2019 Nov;36(4):844-858. doi: 10.1007/s12640-019-00071-5. Epub 2019 Jun 22.

Abstract

The ROS-mediated lysosomal dysfunction and coinciding deterioration of mitochondrial function are thought to be the prominent mechanisms responsible for aging. Microglia, the resident macrophages in the central nervous system, were postulated to belong to the major targets vulnerable to these detrimental processes, acting as principal drivers in brain aging. The present study investigated the potential protective effect of the semisynthetic flavonoid 3'-O-(3-chloropivaloyl) quercetin (CPQ) and quercetin (Q) on microglia-enriched mixed brain cultures (MBCs) established from aged Wistar rats. Both flavonoids tested suppressed the development of lipofuscin-related autofluorescence in aged cells. Further ensuing protective effects included reduction of protein oxidation markers in aged cells. Moreover, unlike Q, CPQ significantly suppressed sensitivity of aged cells to stimulation of superoxide burst. Other activation markers, cellular hypertrophy and isolectin B4 binding, were also downregulated by treatment with both CPQ and Q. In conclusion, results of our study suggest that both flavonoids tested may protect microglia with a quite comparable efficacy against aging-related accumulated alterations. The protective mechanism can include interference with the ROS-mediated vicious cycles involving lysosomal dysfunction. Nevertheless, the lipophilized quercetin, CPQ, a compound with proposed enhanced biological availability compared to parent molecule, can represent an agent potentially useful for new effective pharmaceutical intervention against brain aging, overcoming the limitations of clinical applicability of quercetin.

摘要

ROS 介导致密体功能障碍和线粒体功能同时恶化被认为是导致衰老的主要机制。小胶质细胞是中枢神经系统中的常驻巨噬细胞,被认为是易受这些有害过程影响的主要靶标,是大脑衰老的主要驱动因素。本研究探讨了半合成类黄酮 3'-O-(3-氯代异戊酰基)槲皮素 (CPQ) 和槲皮素 (Q) 对从小鼠大脑中分离的富含小胶质细胞的混合脑培养物 (MBC) 的潜在保护作用。两种黄酮类化合物都抑制了老化细胞中脂褐素相关自发荧光的发展。进一步的保护作用包括减少老化细胞中的蛋白质氧化标志物。此外,与 Q 不同,CPQ 显著抑制了老化细胞对超氧化物爆发刺激的敏感性。其他激活标志物,如细胞肥大和异凝集素 B4 结合,也被 CPQ 和 Q 的处理下调。总之,我们的研究结果表明,两种被测试的类黄酮可能以相当的功效保护小胶质细胞,对抗与衰老相关的累积改变。保护机制可能包括干扰涉及溶酶体功能障碍的 ROS 介导的恶性循环。然而,与母体分子相比,具有增强生物利用度的亲脂性槲皮素 CPQ 可能代表一种潜在有用的药物干预大脑衰老的新有效药物,克服了槲皮素临床应用的局限性。

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