Barral-Netto M, Reed S G, Sadigursky M, Sonnenfeld G
Clin Exp Immunol. 1987 Jan;67(1):11-9.
Successful immunization of highly susceptible BALB/c mice against progressive infection by Leishmania mexicana amazonensis, using whole solubilized promastigotes was achieved. The best immunization schedule consisted of three weekly injections of 5 X 10(7) parasite equivalents. Intravenous was superior to intraperitoneal or subcutaneous immunization. Protection persisted for up to 2 months after immunization, and beneficial effects could be observed in long-term follow-up (24 weeks after infection). Immunized mice exhibited marked reduction in primary lesion size, as well as reduction of the number of parasites in the spleen, and developed less metastases. High titres of specific anti-L. m. amazonensis IgG antibodies resulted from immunization, but titres did not correlate with protection. Groups with widely differing pre-infection antibody titres were equally protected, and similar antibody titres resulted in different levels of protection. Immunization alone did not induce significant serum interferon-gamma levels and specific delayed-type hypersensitivity (DTH) reactions, but resulted in the persistence of positive (DTH) reactions after infection, at a time when infected control animals had suppressed responses. Resistance to leishmaniasis appears to depend on cell mediated immune mechanisms, and the possibility of immunization with a solubilized antigen without adjuvant is intriguing and opens new perspectives in this area.
利用全溶解前鞭毛体成功地使高度易感的BALB/c小鼠获得针对墨西哥利什曼原虫亚马逊亚种进行性感染的免疫。最佳免疫方案包括每周注射三次,每次5×10⁷个寄生虫当量。静脉注射优于腹腔或皮下免疫。免疫后保护作用可持续长达2个月,并且在长期随访(感染后24周)中可观察到有益效果。免疫小鼠的原发性病变大小显著减小,脾脏中的寄生虫数量减少,转移灶也更少。免疫导致产生高滴度的特异性抗墨西哥利什曼原虫亚马逊亚种IgG抗体,但滴度与保护作用无关。感染前抗体滴度差异很大的组受到同等程度的保护,而相似的抗体滴度导致不同程度的保护作用。单独免疫不会诱导显著的血清干扰素-γ水平和特异性迟发型超敏反应(DTH),但在感染后会导致阳性(DTH)反应持续存在,而此时感染的对照动物的反应已受到抑制。对利什曼病的抵抗力似乎取决于细胞介导的免疫机制,并且使用无佐剂的溶解抗原进行免疫的可能性很有趣,并为该领域开辟了新的前景。