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In vitro and in vivo safety and efficacy Studies of amphotericin B on Babesia gibsoni

机译:体外和体内安全性和疗效研究Babesia Gibsoni上的两性霉素B.

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摘要

Babesia gibsoni is a causative pathogen of canine babesiosis, which is commonly treated with anti-babesial drugs; however, the development of novel, more effective anti-babesial drugs is necessary because the currently used drugs cannot remove the parasites from dogs. Therefore we investigated the anti-babesial effect of amphotericin B (AmB), a membrane-active polyene macrolide antibiotic. The interaction of such compounds with sterols in bilayer cell membranes can lead to cell damage and ultimately cell lysis. AmB exhibits in vitro activity against B. gibsoni in normal canine erythrocytes within 12 h. We also studied liposomal AmB (L-AmB), a liposomal formulation of AmB that required a longer incubation period to reduce the number of parasites. However, L-AmB completely inhibited the invasion of free parasites into erythrocytes. These results indicated that free parasites failed to invade erythrocytes in the presence of L-AmB. Both AmB and L-AmB induced mild hemolysis of erythrocytes. Moreover, the methemoglobin level and the turbidity index of erythrocytes were significantly increased when erythrocytes were incubated with AmB, suggesting that AmB induced oxidative damage in erythrocytes. Finally, the anti-babesial activity of AmB in vivo was observed. When experimentally B. gibsoni-infected dogs were administered 0.5 and 1 mg/kg AmB by the intravenous route, the number of parasites decreased; however, recurrence of parasitemia was observed, indicating that AmB did not eliminate parasites completely. Blood urea nitrogen and creatinine of dogs were abnormally elevated after the administration of 1 mg/kg AmB. These results indicate that AmB has in vivo activity against B. gibsoni; however, it does not eliminate parasites from infected dogs and affects kidney function at a high dose. (C) 2014 Elsevier B.V. All rights reserved.
机译:Babesia Gibsoni是犬嗜睡症的致病病原体,其通常用抗婴儿药物治疗;然而,新颖,更有效的抗宝贝药物的发展是必要的,因为目前使用的药物不能从狗中取出寄生虫。因此,我们研究了两性霉素B(AMB),膜活性多丙烯酯抗生素的抗婴儿作用。这些化合物与双层细胞膜中的甾醇的相互作用可以导致细胞损伤和最终细胞裂解。 AMB在12小时内对普通犬红细胞的B.Gibsoni进行体外活性。我们还研究了脂质体AMB(L-AMB),AMB的脂质体配方需要更长的培养期,以减少寄生虫的数量。然而,L-AMB完全抑制自由寄生虫进入红细胞的侵袭。这些结果表明,自由寄生虫未能在L-AMB存在下侵入红细胞。 AMB和L-AMB均诱导红细胞的温和溶血。此外,当与AMB孵育红细胞时,红细胞蛋白水平和红细胞的浊度指数显着增加,表明AMB诱导红细胞氧化损伤。最后,观察到体内AMB的抗婴儿活动。通过静脉内途径施用0.5和1mg / kg AMB的实验B.Gibsoni感染的犬,寄生虫的数量减少;然而,观察到寄生虫的复发,表明AMB没有完全消除寄生虫。血液尿素氮和肌酐在给药1mg / kg AMB后异常升高。这些结果表明,AMB对B. Gibsoni的体内活动;然而,它不会消除来自受感染的犬的寄生虫,并在高剂量下影响肾功能。 (c)2014 Elsevier B.v.保留所有权利。

著录项

  • 来源
    《Veterinary Parasitology》 |2014年第4期|共10页
  • 作者单位

    Hokkaido Univ Lab Vet Internal Med Dept Vet Clin Sci Grad Sch Vet Med Sapporo Hokkaido 0600818 Japan;

    Hokkaido Univ Lab Vet Internal Med Dept Vet Clin Sci Grad Sch Vet Med Sapporo Hokkaido 0600818 Japan;

    Hokkaido Univ Lab Vet Internal Med Dept Vet Clin Sci Grad Sch Vet Med Sapporo Hokkaido 0600818 Japan;

    Hokkaido Univ Lab Vet Internal Med Dept Vet Clin Sci Grad Sch Vet Med Sapporo Hokkaido 0600818 Japan;

    Hokkaido Univ Lab Vet Internal Med Dept Vet Clin Sci Grad Sch Vet Med Sapporo Hokkaido 0600818 Japan;

    Hokkaido Univ Lab Vet Internal Med Dept Vet Clin Sci Grad Sch Vet Med Sapporo Hokkaido 0600818 Japan;

    Hokkaido Univ Grad Sch Vet Med Vet Teaching Hosp Sapporo Hokkaido 0600818 Japan;

    Hokkaido Univ Grad Sch Vet Med Vet Teaching Hosp Sapporo Hokkaido 0600818 Japan;

    Hokkaido Univ Lab Vet Internal Med Dept Vet Clin Sci Grad Sch Vet Med Sapporo Hokkaido 0600818 Japan;

    Hokkaido Univ Lab Vet Internal Med Dept Vet Clin Sci Grad Sch Vet Med Sapporo Hokkaido 0600818 Japan;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 动物医学(兽医学);
  • 关键词

    Babesia gibsoni; Amphotericin B; Liposomal amphotericin B; Anti-babesial drug;

    机译:Babesia Gibsoni;两性霉素B;脂质体两性霉素B;抗婴儿药物;

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