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对来自流行地区的利什曼原虫皮肤试验阴性个体中针对硕大利什曼原虫免疫的替代标志物进行重新研究。

Surrogate markers of immunity to Leishmania major in leishmanin skin test negative individuals from an endemic area re-visited.

作者信息

Nylén Susanne, Khamesipour Ali, Mohammadi Akram, Jafari-Shakib Reza, Eidsmo Liv, Noazin Sassan, Modabber Farrokh, Akuffo Hannah

机构信息

Microbiology and Tumor biology Center (MTC), Karolinska Institutet, Stockholm, Sweden.

出版信息

Vaccine. 2006 Nov 17;24(47-48):6944-54. doi: 10.1016/j.vaccine.2006.05.016. Epub 2006 May 30.

Abstract

BACKGROUND

In the screening of vaccine candidates it is important to select candidates that evoke immune responses associated with protection. Valid surrogate markers against human leishmaniasis are still lacking.

METHODS

A controlled injection of live Leishmania known as leishmanization, (LZ), was used to evaluate vaccine (alum-precipitated autoclaved Leishmania major with BCG) efficacy and more accurately define surrogate markers of immunity to leishmaniasis in humans. Cellular immune responses to this artificial infection were monitored in the volunteers prior to and 9 months post infection. Comparisons were made between those who developed a lesion after infection and those who did not.

RESULTS

In the volunteers monitored there was no significant difference in LST, IFNgamma production, or source of IFNgamma between those who developed a lesion and those who did not after LZ, with the exception that ulcer development was associated with an enhanced number of IFNgamma secreting CD4(+) CD45RA(-) (memory) T cells.

DISCUSSION

Ulcer development following LZ was lower than anticipated by a pilot study (47% versus 78%) using the same stabilate several years earlier. While this may be an effect of low viability/virulence of the LZ inocula, alternative explanations are also possible. The IFNgamma responses in the study subjects were significantly lower compared to volunteers with previous history of cutaneous leishmaniasis. The findings raise the possibility that the selection of LST-negative volunteers in an endemic area may bias the study towards potentially non/low L. major-reactive volunteers.

摘要

背景

在筛选候选疫苗时,选择能引发与保护相关免疫反应的候选疫苗很重要。目前仍缺乏针对人类利什曼病的有效替代标志物。

方法

采用一种名为利什曼化(LZ)的活利什曼原虫对照注射,来评估疫苗(卡介苗与明矾沉淀高压灭菌的硕大利什曼原虫)的疗效,并更准确地确定人类对利什曼病免疫的替代标志物。在志愿者感染前及感染后9个月监测其对这种人工感染的细胞免疫反应。对感染后出现病变的志愿者和未出现病变的志愿者进行比较。

结果

在监测的志愿者中,利什曼化后出现病变的志愿者和未出现病变的志愿者之间,在淋巴细胞刺激试验(LST)、γ干扰素产生或γ干扰素来源方面没有显著差异,唯一的例外是溃疡的出现与分泌γ干扰素的CD4(+) CD45RA(-)(记忆)T细胞数量增加有关。

讨论

利什曼化后溃疡的发生率低于几年前使用相同冻干制剂的一项初步研究预期的发生率(47%对78%)。虽然这可能是利什曼化接种物活力/毒力低的影响,但也可能有其他解释。与有皮肤利什曼病既往史的志愿者相比,本研究对象中的γ干扰素反应明显较低。这些发现增加了一种可能性,即在流行地区选择淋巴细胞刺激试验阴性的志愿者可能会使研究偏向于潜在的对硕大利什曼原虫无反应/低反应的志愿者。

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