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用葡萄糖酸锑钠的非离子表面活性剂囊泡制剂治疗BALB/c小鼠内脏利什曼病所获得的治愈免疫表型不能预防再次感染。

The cured immune phenotype achieved by treatment of visceral leishmaniasis in the BALB/c mouse with a nonionic surfactant vesicular formulation of sodium stibogluconate does not protect against reinfection.

作者信息

Carter K C, Baillie A J, Mullen A B

机构信息

Departments of Immunology, University of Strathclyde, Glasgow G4 ONR, United Kingdom.

出版信息

Clin Diagn Lab Immunol. 1999 Jan;6(1):61-5. doi: 10.1128/CDLI.6.1.61-65.1999.

DOI:10.1128/CDLI.6.1.61-65.1999
PMID:9874665
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC95661/
Abstract

Single-dose treatment with sodium stibogluconate solution (SSG) and treatment with a nonionic surfactant vesicular formulation of sodium stibogluconate (SSG-NIV) were compared for the ability to protect BALB/c mice against infection with Leishmania donovani. Prophylactic treatment with SSG-NIV protected against infection, although its effects were time and organ dependent; protection was not obtained with SSG. Protection against reinfection with L. donovani was observed only in mice cured by treatment with SSG-NIV. However, this protective effect was probably due to the presence of residual drug rather than an immune effect, since prophylactic SSG-NIV treatment gave similar results. Transfer of enriched spleen T-cell populations from L. donovani-infected mice or from infected SSG-NIV-treated mice gave no protection against L. donovani infection in the recipients. T cells from infected mice, but not from infected SSG-NIV-treated mice, were infectious to recipients. SSG-NIV treatment was equally effective against visceral leishmaniasis in immunocompetent and SCID mice, whereas SSG treatment was less effective in the latter. The results of this study suggest that the high antileishmanial activity of SSG-NIV is due to favorable modification of SSG delivery and does not require a fully functional immune response. Cure of visceral leishmaniasis by SSG-NIV treatment in the BALB/c mouse did not protect against reinfection.

摘要

比较了葡糖酸锑钠溶液(SSG)单剂量治疗和葡糖酸锑钠非离子表面活性剂囊泡制剂(SSG-NIV)治疗保护BALB/c小鼠免受杜氏利什曼原虫感染的能力。SSG-NIV预防性治疗可预防感染,但其效果具有时间和器官依赖性;SSG则未获得保护效果。仅在经SSG-NIV治疗治愈的小鼠中观察到对杜氏利什曼原虫再感染的保护作用。然而,这种保护作用可能是由于残留药物的存在而非免疫效应,因为预防性SSG-NIV治疗给出了相似的结果。从感染杜氏利什曼原虫的小鼠或感染后经SSG-NIV治疗的小鼠中转移富集的脾脏T细胞群体,对受体小鼠的杜氏利什曼原虫感染没有保护作用。来自感染小鼠而非感染后经SSG-NIV治疗小鼠的T细胞对受体具有感染性。SSG-NIV治疗对免疫健全小鼠和SCID小鼠的内脏利什曼病同样有效,而SSG治疗在后者中效果较差。本研究结果表明,SSG-NIV的高抗利什曼原虫活性归因于对SSG递送的有利修饰,且不需要完全功能性的免疫反应。BALB/c小鼠经SSG-NIV治疗治愈内脏利什曼病后并不能预防再感染。

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引用本文的文献

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本文引用的文献

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2
Immune responses of Leishmania donovani infected BALB/c mice following treatment with free and vesicular sodium stibogluconate formulations.用游离和囊泡型葡萄糖酸锑钠制剂治疗后,杜氏利什曼原虫感染的BALB/c小鼠的免疫反应
Int J Immunopharmacol. 1997 Apr;19(4):195-203. doi: 10.1016/s0192-0561(97)00009-x.
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Visceral leishmaniasis in the BALB/c mouse: a comparison of the in vivo activity of five non-ionic surfactant vesicle preparations of sodium stibogluconate.BALB/c小鼠内脏利什曼病:五种葡糖酸锑钠非离子表面活性剂囊泡制剂体内活性的比较
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