Effect of Short‐, Medium‐, and Long‐Chain Fatty Acid‐Based Vehicles on the Absolute Oral Bioavailability and Intestinal Lymphatic Transport of Halofantrine and Assessment of Mass Balance in Lymph‐Cannulated and Non‐cannulated Rats

生物利用度 淋巴系统 淋巴 化学 脂肪酸 药理学 药代动力学 卤凡特林 口服 药品 吸收(声学) 医学 生物化学 病理 物理 甲氟喹 氯喹 疟疾 声学
作者
Suzanne M. Caliph,William N. Charman,Christopher J. H. Porter
出处
期刊:Journal of Pharmaceutical Sciences [Elsevier]
卷期号:89 (8): 1073-1084 被引量:271
标识
DOI:10.1002/1520-6017(200008)89:8<1073::aid-jps12>3.0.co;2-v
摘要

Abstract

The contribution of lymphatic transport and absorption directly into the portal blood to the overall oral bioavailability of a model lipophilic drug, halofantrine (Hf), was determined in lymph‐cannulated, conscious, unrestrained rats after administration in lipidic vehicles with different fatty acid chain lengths. Both lymphatic transport (C18‐based vehicle, 15.8% of dose > C8–10, 5.5% > C4, 2.22% > C0, 0.34%) and total systemic exposure (C18, 22.7% of dose > C8–10, 19.2% > C4, 15.2% > C0, 6.4%) of Hf were enhanced by the presence of lipids in the formulation and specifically by an increase in the fatty acid chain length of the coadministered lipid. Increases in lymphatic drug transport appeared to correlate with increases in lymphatic lipid transport. Surprisingly, where lymphatic transport was the primary mechanism of drug transport to the systemic circulation (i.e., after administration in a C18‐based lipid vehicle), Hf bioavailability assessed in nonlymph‐cannulated animals was lower than the extent of total availability measured in lymph‐cannulated animals (estimated as percent appearing in the intestinal lymph plus percent transported directly into the blood), suggesting either presystemic drug clearance within the lymphatics or an altered systemic clearance pattern for lymphatically transported drug. © 2000 Wiley‐Liss, Inc. and the American Pharmaceutical Association J Pharm Sci 89: 1073–1084, 2000

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