Spatiotemporal Characterization of Sulfasalazine and 5-ASA Pharmacokinetics Using a Noninvasive Intestinal Sampling Device.

IF 5.5 2区医学 Q1 PHARMACOLOGY & PHARMACY

Clinical Pharmacology & Therapeutics Pub Date : 2025-08-23 DOI:10.1002/cpt.70035

Jingwei Cai, Jordan S Mar, Bennett Kapili, Kelly M Storek, Jasmina Uzunovic, Elizabeth Skippington, Daniela Keilberg, Dewakar Sangaraju, Alexis Auster, Cyrus Khojasteh, Horace Rhee, George Triadafilopoulos, Dari Shalon, Mary Keir

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引用次数: 0

Abstract

Sulfasalazine, a cornerstone therapy for inflammatory bowel disease, relies on bacterial azo-reduction to release its active component, 5-aminosalicylic acid (5-ASA), which is further metabolized into inactive N-acetyl-5-aminosalicylic acid (N-acetyl-5-ASA) by bacterial N-acetyltransferase. Due to complex pharmacokinetics, patient-specific microbial metabolism, and the lack of accurate, convenient direct sampling method for gastrointestinal drug concentrations, sulfasalazine clinical efficacy remains variable. The CapScan® luminal sampling device enables region-specific, minimally invasive collection of intestinal contents. To better understand sulfasalazine pharmacokinetics in relation to intestinal and systemic drug concentrations and bacterial metabolic capacity, 10 healthy volunteers ingested CapScan devices following sulfasalazine administration. Upon retrieval from the stool, CapScan samples were assigned intestinal locations based on metabolomic and metagenomic profiling. Systemic sulfasalazine peaked at 4 hours post-ingestion, while 5-ASA and N-acetyl-5-ASA peaked at 8 hours. In the gastrointestinal tract, maximal sulfasalazine concentration was observed in the proximal small intestine (SI), decreasing distally as 5-ASA and N-acetyl-5-ASA concentrations increased, peaking in the stool. 5-ASA plasma concentrations positively correlated with distal SI concentrations 4 hours after sulfasalazine ingestion. Putative bacterial azoreductase genes were detected in all gastrointestinal regions, while putative bacterial acetyltransferase genes were detected in all regions except the proximal SI. This study revealed spatially distinct luminal concentrations of sulfasalazine and its metabolites, with a strong correlation between distal SI 5-ASA levels and early plasma exposure, highlighting GI region-specific absorption and microbial metabolism. These findings support the potential utility of luminal sampling to enhance understanding of drug pharmacokinetics and inform future strategies for optimizing oral drug delivery.

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使用无创肠道采样装置的磺胺氮嘧啶和5-ASA药代动力学的时空表征。

磺胺吡啶是炎症性肠病的基础疗法，依靠细菌偶氮还原释放其活性成分5-氨基水杨酸（5-ASA），通过细菌n -乙酰基转移酶进一步代谢为无活性的n -乙酰基-5-氨基水杨酸（n -乙酰基-5-ASA）。由于复杂的药代动力学和患者特异性微生物代谢，以及缺乏准确、方便的胃肠道药物浓度直接采样方法，磺胺氮嗪的临床疗效仍不稳定。CapScan®腔内取样装置可实现特定区域的微创肠道内容物采集。为了更好地了解磺胺氮嗪的药代动力学与肠道和全身药物浓度以及细菌代谢能力的关系，10名健康志愿者在服用磺胺氮嗪后服用了CapScan装置。从粪便中提取后，CapScan样本根据代谢组学和宏基因组学分析被分配到肠道位置。全身磺胺吡啶在摄入后4小时达到峰值，而5-ASA和n -乙酰基-5-ASA在摄入后8小时达到峰值。在胃肠道中，磺胺吡啶的最高浓度出现在近端小肠（SI），随着5-ASA和n -乙酰基-5-ASA浓度的升高，远端呈下降趋势，在粪便中达到峰值。5-ASA血浆浓度与远端SI浓度在服用磺胺吡啶后4小时呈正相关。在所有胃肠道区域均检测到假定的细菌氮还原酶基因，而在除近端SI外的所有区域均检测到假定的细菌乙酰转移酶基因。该研究揭示了磺胺吡啶及其代谢物的腔内浓度具有空间差异，远端SI 5-ASA水平与早期血浆暴露有很强的相关性，突出了胃肠道区域特异性吸收和微生物代谢。这些发现支持了腔内取样的潜在效用，以加强对药物药代动力学的理解，并为优化口服药物递送的未来策略提供信息。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Clinical Pharmacology & Therapeutics 医学-药学

CiteScore

12.70

自引率

7.50%

发文量

290

审稿时长

2 months

期刊介绍： Clinical Pharmacology & Therapeutics (CPT) is the authoritative cross-disciplinary journal in experimental and clinical medicine devoted to publishing advances in the nature, action, efficacy, and evaluation of therapeutics. CPT welcomes original Articles in the emerging areas of translational, predictive and personalized medicine; new therapeutic modalities including gene and cell therapies; pharmacogenomics, proteomics and metabolomics; bioinformation and applied systems biology complementing areas of pharmacokinetics and pharmacodynamics, human investigation and clinical trials, pharmacovigilence, pharmacoepidemiology, pharmacometrics, and population pharmacology.