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用于研究胃肠道过程的具有更高通量和更生理相关的两室式人离体肠道组织系统。

A higher throughput and physiologically relevant two-compartmental human ex vivo intestinal tissue system for studying gastrointestinal processes.

机构信息

The Netherlands Organization for Applied Scientific Research (TNO), Utrechtseweg 48, 3704 HE Zeist, the Netherlands.

Diakonessenhuis, Bosboomstraat 1, 3582 KE Utrecht, the Netherlands.

出版信息

Eur J Pharm Sci. 2019 Sep 1;137:104989. doi: 10.1016/j.ejps.2019.104989. Epub 2019 Jul 10.

Abstract

A majority of the preclinical intestinal screening models do not properly reflect the complex physiology of the human intestinal tract, resulting in low translational value to the clinical situation. The often used cell lines such as Caco-2 or HT-29 are not well suited to investigate the different processes that predict oral bioavailability in real life, or processes involved in general gut health aspects. Therefore, highly realistic models resembling the human in vivo situation are needed; application of ex vivo intestinal tissue is an interesting and feasible alternative. After previously using porcine intestinal tissue as a predictive model for human intestinal absorption, we now have successfully applied human intestinal tissue into a newly developed InTESTine™ two-compartmental disposable device suitable for standard 6- or 24-well plate format. With this set-up we demonstrated (regional differences in) drug absorption, by using a subset of compounds with known varying F (fraction absorbed) values. A rank-order relationship of R = 0.85 could be established between the F and P of these commercially available drugs. Additionally, comparison between the InTESTine system and the established Ussing chamber technology showed a correlation of R = 0.94 (10 drugs) with respect to P values, indicating good comparison of both models. Besides absorption, intestinal wall metabolism of testosterone (CYP3A4) was determined by showing a linear formation (R = 0.99; up to 165 min) of the main metabolites androstenedione and 6Beta-hydroxytestosterone, indicating no loss of metabolic capacity of the intestinal tissue within the system. Enteroendocrine responses were assessed of the satiety hormones GLP-1 and PYY after stimulation with rebaudioside A and casein, resulting in significantly increased secretion to the luminal side as well as to the basolateral side. Incubation with the probiotic strain LGG showed to enhance the viability of the tissue by showing to decrease the LDH secretion compared to blank intestinal tissue. In conclusion, we show that human ex vivo intestinal tissue mounted in the higher throughput InTESTine 6- 24-transwell plate system is easy to handle and a suitable system to study diverse functional GI processes.

摘要

大多数临床前肠道筛选模型不能很好地反映人体肠道的复杂生理学,因此对临床情况的转化价值较低。通常使用的细胞系,如 Caco-2 或 HT-29,并不适合研究预测实际生活中口服生物利用度的不同过程,或涉及一般肠道健康方面的过程。因此,需要高度逼真的模拟人体体内情况的模型;应用离体肠道组织是一种有趣且可行的替代方法。在之前使用猪肠道组织作为人体肠道吸收的预测模型之后,我们现在已经成功地将人体肠道组织应用于一种新开发的 InTESTine™ 两室一次性装置中,该装置适合标准的 6 孔或 24 孔板格式。通过使用一组具有已知不同 F(吸收率)值的化合物,我们用该装置证明了(区域性差异)药物吸收。可以建立这些市售药物的 F 和 P 之间的等级关系,R=0.85。此外,InTESTine 系统与已建立的 Ussing 室技术的比较显示,P 值的相关系数 R=0.94(10 种药物),表明两种模型的比较良好。除了吸收之外,还通过显示主要代谢物雄烯二酮和 6β-羟基睾酮的线性形成(R=0.99;长达 165 分钟)来确定睾酮(CYP3A4)在肠道壁中的代谢情况,表明系统内肠道组织的代谢能力没有损失。在用 Rebaudioside A 和酪蛋白刺激后,评估了饱腹激素 GLP-1 和 PYY 的肠内分泌反应,导致向腔侧和基底外侧侧显著增加分泌。与空白肠道组织相比,用益生菌株 LGG 孵育可通过显示减少 LDH 分泌来增强组织的活力。总之,我们表明,在高通量 InTESTine 6-24 转孔板系统中安装的离体人体肠道组织易于处理,是研究各种功能性 GI 过程的合适系统。

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