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5-单磷酸阿糖腺苷(ara-AMP)的乳糖胺化白蛋白缀合物在小鼠肝脏中的选择性渗透和药理活性。

Selective penetration and pharmacological activity of lactosaminated albumin conjugates of adenine arabinoside 5-monophosphate (ara-AMP) in mouse liver.

作者信息

Fiume L, Mattioli A, Busi C, Accorsi C

出版信息

Gut. 1984 Dec;25(12):1392-8. doi: 10.1136/gut.25.12.1392.

Abstract

With the aim of improving the chemotherapeutic index of adenine arabinoside 5-monophosphate (ara-AMP) in the treatment of chronic hepatitis B, this drug was conjugated with lactosaminated serum albumin (L-SA), a neoglycoprotein which only enters into hepatocytes where it is digested in lysosomes. In mice, the L-[3H]SA-ara-AMP conjugates, intravenously injected, selectively penetrated the liver, only small quantities were taken up by cells of spleen, bone marrow, intestine, and brain. After administration of the conjugate to mice with Ectromelia virus hepatitis, ara-AMP was selectively concentrated in liver in a pharmacologically active form. If L-SA-ara-AMP conjugates behave in man as in mouse, their administration to patients with chronic hepatitis B should result in a selective concentration of ara-AMP in liver with a more efficient inhibition of virus replication accompanied by lower toxicity for other tissues.

摘要

为了提高单磷酸阿糖腺苷(ara-AMP)治疗慢性乙型肝炎的化疗指数,将该药物与乳糖胺化血清白蛋白(L-SA)偶联,L-SA是一种新糖蛋白,仅进入肝细胞并在溶酶体中被消化。在小鼠中,静脉注射的L-[3H]SA-ara-AMP偶联物选择性地渗透到肝脏,脾脏、骨髓、肠道和脑的细胞仅摄取少量。给感染埃可病毒肝炎的小鼠施用偶联物后,ara-AMP以药理活性形式选择性地浓集在肝脏中。如果L-SA-ara-AMP偶联物在人体中的行为与在小鼠中一样,那么给慢性乙型肝炎患者施用它们应该会导致ara-AMP在肝脏中选择性浓集,更有效地抑制病毒复制,同时对其他组织的毒性更低。

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