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Liver Targeting of Interferon Through Pullulan Conjugation
Authors:Xi  Keli  Tabata  Yasuhiko  Uno  Kazuko  Yoshimoto  Miwa  Kishida  Tsunataro  Sokawa  Yoshihiro  Ikada  Yoshito
Affiliation:(1) Research Center for Biomedical Engineering, Kyoto University, 53 Kawahara-cho Shogoin, Sakyo-ku, Kyoto, 606, Japan;(2) Present address: Chemistry Department, Yunnan University, Kunming, 650031, China;(3) Institut Pastuer de Kyoto, 103-5 Monzen-cho, Tanaka, Sakyo-ku, Kyoto, 606, Japan;(4) Department of Biotechnology, Kyoto Institute of Technology, Gosyo-kaido-cho, Matsugasaki, Sakyo-ku, Kyoto, 606, Japan
Abstract:
Purpose. The purpose of this study was to actively target interferon (IFN) to the liver through its chemical conjugation with pullulan, a water-soluble polysaccharide with a high affinity for the liver.Methods. Chemical conjugation of IFN with pullulan was achieved by a cyanuric chloride method. Following intravenous injection of the conjugates to mice, their body distribution and the activity of an IFN-induced enzyme, 2prime,5prime-oligoadenylate (2-5A) synthetase in the liver and other organs, were evaluated.Results. The cyanuric chloride method enabled us to prepare an IFN-pullulan conjugate that retained approximately 7–uarr9 % of the biological activity of IFN. Pullulan conjugation enhanced the liver accumulation of IFN and the retention period with the results being reproducible. When injected intravenously to mice, the IFN-pullulan conjugate enhanced the activity of 2-5A synthetase in the liver. The activity could be induced at IFN doses much lower than those of free IFN injection. In addition, the liver 2-5A synthetase induced by conjugate injection was retained for 3 days, whereas it was lost within the first day for the free IFN-injected mice.Conclusions. IFN-pullulan conjugation was promising for IFN targeting to the liver with efficient exertion of its antiviral activity therein.
Keywords:interferon  pullulan conjugation  liver targeting  2-5A synthetase
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