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Deuteration enhances the anti-tumor effects and relative anti-inflammatory effects via affecting proliferation and apoptosis

机译:氘化通过影响增殖和细胞凋亡来增强抗肿瘤效应和相对抗炎作用

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摘要

Apigenin (AP) is a plant flavonoid with potential biomedical applications. To enhance the anti-tumour effect, AP was deuterated via hydrogen–deuterium exchange under hydrothermal conditions. The anti-tumor effects of deuterated AP (D-AP) were then tested on HCT116 cells and on a murine model of turpentine-induced inflammation. Cell cycle progression and cell proliferation were measured by flow cytometry, and in vivo immuno-inflammation was evaluated by quantitating glucose metabolism using 18F-fluorodeoxyglucose positron emission tomography. According to the mass spectral results, the efficiency of AP deuteration was 62.96%. For both the two groups of AP and D-AP at 24 h and 48 h, there were an obvious increase on perception of G2 phage. Apigenin showed the ability of blocking in G2 phage to inhibit cellular proliferation. Additionally, D-AP induced early apoptosis in more cells than did AP (12.1% vs. 10.4%). Moreover, D-AP induced a more severe process of anti-inflammation during the early period, resulting in a more effective anti-inflammatory response. Therefore, given the innate ability of D-AP to block cell proliferation and induce early apoptosis, we conclude that deuteration enhances the systemic anti-cancer effect of this flavonoid.
机译:Apigenin(AP)是一种植物黄酮类化合物,具有潜在的生物医学应用。为了增强抗肿瘤作用,AP通过水热条件下通过氢氘交换氘化。然后在HCT116细胞和松节油诱导的炎症的鼠模型上测试氘代AP(D-AP)的抗肿瘤作用。通过流式细胞术测量细胞周期进展和细胞增殖,并通过使用18氟氟氧氧葡萄糖正电子发射断层扫描定量葡萄糖代谢来评价体内免疫炎症。根据质谱结果,AP氘的效率为62.96%。对于24小时和48小时的两组AP和D-AP,G2噬菌体的感知显而易见。 Apigenin显示出在G2噬菌体中抑制细胞增殖的能力。此外,D-AP在比AP(12.1%对10.4%)的细胞中诱导早期细胞凋亡。此外,D-AP在早期诱导更严重的抗炎过程,导致更有效的抗炎反应。因此,鉴于D-AP的先天能力阻断细胞增殖并诱导早期细胞凋亡,我们得出结论,氘化可提高该类黄酮的全身抗癌作用。

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