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肠类器官用于研究儿科肠道药物转运

Enteroids to Study Pediatric Intestinal Drug Transport.

机构信息

Division of Pharmacology and Toxicology, Department of Pharmacy, Radboud University Medical Center, Nijmegen 6525GA, The Netherlands.

Department of Metabolic Health Research, Netherlands Organization for Applied Scientific Research (TNO), Leiden 2333BE, The Netherlands.

出版信息

Mol Pharm. 2024 Oct 7;21(10):4983-4994. doi: 10.1021/acs.molpharmaceut.4c00339. Epub 2024 Sep 16.

Abstract

Intestinal maturational changes after birth affect the pharmacokinetics (PK) of drugs, having major implications for drug safety and efficacy. However, little is known about ontogeny-related PK patterns in the intestine. To explore the accuracy of human enteroid monolayers for studying drug transport in the pediatric intestine, we compared the drug transporter functionality and expression in enteroid monolayers and tissue from pediatrics and adults. Enteroid monolayers were cultured of 14 pediatric [median (range) age: 44 weeks (2 days-13 years)] and 5 adult donors, in which bidirectional drug transport experiments were performed. In parallel, we performed similar experiments with tissue explants in Ussing chamber using 11 pediatric [median (range) age: 54 weeks (15 weeks-10 years)] and 6 adult tissues. Enalaprilat, propranolol, talinolol, and rosuvastatin were used to test paracellular, transcellular, and transporter-mediated efflux by P-gp and breast cancer resistance protein (BCRP), respectively. In addition, we compared the expression patterns of ADME-related genes in pediatric and adult enteroid monolayers with tissues using RNA sequencing. Efflux transport by P-gp and BCRP was comparable between the enteroids and tissue. Efflux ratios (ERs) of talinolol and rosuvastatin by P-gp and BCRP, respectively, were higher in enteroid monolayers compared to Ussing chamber, likely caused by experimental differences in model setup and cellular layers present. Explorative statistics on the correlation with age showed trends of increasing ER with age for P-gp in enteroid monolayers; however, it was not significant. In the Ussing chamber setup, lower enalaprilat and propranolol transport was observed with age. Importantly, the RNA sequencing pathway analysis revealed that age-related variation in drug metabolism between neonates and adults was present in both enteroids and intestinal tissue. Age-related differences between 0 and 6 months old and adults were observed in tissue as well as in enteroid monolayers, although to a lesser extent. This study provides the first data for the further development of pediatric enteroids as an in vitro model to study age-related variation in drug transport. Overall, drug transport in enteroids was in line with data obtained from ex vivo tissue (using chamber) experiments. Additionally, pathway analysis showed similar PK-related differences between neonates and adults in both tissue and enteroid monolayers. Given the challenge to elucidate the effect of developmental changes in the pediatric age range in human tissue, intestinal enteroids derived from pediatric patients could provide a versatile experimental platform to study pediatric phenotypes.

摘要

出生后的肠道成熟变化会影响药物的药代动力学(PK),这对药物的安全性和疗效有重大影响。然而,人们对肠道中与个体发育相关的 PK 模式知之甚少。为了探索肠类器官单层在研究儿科肠道药物转运中的准确性,我们比较了肠类器官单层和儿科及成人组织中的药物转运体功能和表达。从 14 名儿科患者(中位数(范围)年龄:44 周(2 天-13 岁))和 5 名成人供体中培养肠类器官单层,进行双向药物转运实验。同时,我们使用 Ussing 室中的组织外植体进行了类似的实验,使用 11 名儿科患者(中位数(范围)年龄:54 周(15 周-10 岁))和 6 名成人组织。分别使用依那普利拉、普萘洛尔、他林洛尔和瑞舒伐他汀来测试 P-糖蛋白和乳腺癌耐药蛋白(BCRP)的旁细胞、跨细胞和转运体介导的外排。此外,我们使用 RNA 测序比较了儿科和成人肠类器官单层与组织中 ADME 相关基因的表达模式。肠类器官和组织中 P-糖蛋白和 BCRP 的外排转运相似。与 Ussing 室相比,P-糖蛋白和 BCRP 的他林洛尔和瑞舒伐他汀的外排比(ER)在肠类器官单层中更高,这可能是由于模型设置和存在的细胞层的实验差异所致。对与年龄相关的相关性的探索性统计显示,肠类器官中 P-糖蛋白的 ER 随年龄增长呈上升趋势;然而,这并不显著。在 Ussing 室设置中,随着年龄的增长,依那普利拉和普萘洛尔的转运减少。重要的是,通路分析表明,新生儿和成人之间药物代谢的年龄相关性差异在肠类器官和肠组织中都存在。在组织和肠类器官单层中观察到 0-6 个月龄和成人之间的年龄相关差异,尽管程度较小。本研究提供了将儿科肠类器官进一步开发为研究药物转运年龄相关性差异的体外模型的首批数据。总的来说,肠类器官中的药物转运与使用室(使用室)实验获得的组织数据一致。此外,通路分析表明,在组织和肠类器官单层中,新生儿和成人之间的 PK 相关差异相似。鉴于阐明儿科年龄范围内发育变化对人类组织的影响具有挑战性,来自儿科患者的肠道肠类器官可能提供一个通用的实验平台来研究儿科表型。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8b7f/11462498/64d87c39a8bd/mp4c00339_0001.jpg

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