The inhibitory effect of kakkonto, Japanese traditional (kampo) medicine, on brain penetration of oseltamivir carboxylate in mice with reduced blood-brain barrier function.

Kousuke Ohara,Akio Negishi,Seiichi Honma,Shingo Takenaka,Masayuki Akimoto,Shigeru Ohshima,Yumiko Ochiai,Daisuke Kobayashi,Shinji Oshima,Aki Kanamuro,Nanami Fukuda,Ayumi Maruyama

doi:10.1155/2015/917670

Abstract

Oseltamivir phosphate (OP) is used to treat influenza virus infections. However, its use may result in central nervous system (CNS) adverse effects. In Japan, OP is used with Kampo formulations to improve clinical effectiveness. We evaluated the potential for using Kampo formulations to reduce CNS adverse effects by quantifying the CNS distribution of oseltamivir and its active metabolite oseltamivir carboxylate (OC) when administered with maoto and kakkonto. We administered lipopolysaccharide (LPS) by intraperitoneal injection to C57BL/6 mice to reduce blood-brain barrier function. Saline, maoto, and kakkonto were administered orally at the same time as LPS. OP was orally administered 4 hours after the last LPS injection and the migration of oseltamivir and OC was examined. Additionally, we examined the brain distribution of OC following intravenous administration. Changes in OC concentrations in the brain suggest that, in comparison to LPS-treated control mice, both Kampo formulations increased plasma levels of OC, thereby enhancing its therapeutic effect. Additionally, our findings suggest kakkonto may not only improve the therapeutic effect of oseltamivir but also reduce the risk of CNS-based adverse effects. Considering these findings, it should be noted that administration of kakkonto during periods of inflammation has led to increased OAT3 expression.

Highlights

Oseltamivir phosphate (OP) elicits antiviral effects by selectively inhibiting the neuraminidase in influenza viruses A and B, making it an effective agent for prevention and treatment of influenza infections
In addition to observed reduction in blood-brain barrier (BBB) function, we observed that oral administration of OP to these mice markedly increased the cerebral penetration of oseltamivir and oseltamivir carboxylate (OC) [9]
Since no studies have directly evaluated this question far, we investigated the cerebral migration of oseltamivir and OC, which are involved in the onset of central nervous system (CNS) adverse effects, when maoto or kakkonto is administered concomitantly with OP

Summary

Introduction

Oseltamivir phosphate (OP) elicits antiviral effects by selectively inhibiting the neuraminidase in influenza viruses A and B, making it an effective agent for prevention and treatment of influenza infections. Infections with the influenza virus are inflammatory diseases Cytokines, such as tumor necrosis factor-alpha, interleukin-1 (IL-1), and IL-6, are secreted into serum and cerebrospinal fluid, with the increases in circulating levels of these cytokines resulting in attenuated blood-brain barrier (BBB) function [3, 4]. In order to investigate these phenomena, brain distribution of OP and OC has been analyzed in juvenile rats, Evidence-Based Complementary and Alternative Medicine in which BBB function is underdeveloped [6, 7]. Systemic inflammation induced by LPS administration is reported to be pathologically similar to influenza-associated encephalopathy [4]. In addition to observed reduction in BBB function, we observed that oral administration of OP to these mice markedly increased the cerebral penetration of oseltamivir and OC [9]

Methods

Results

Conclusion