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用全血期抗原和共聚物佐剂诱导对约氏疟原虫疟疾的持久免疫力。

Induction of long-lasting immunity to Plasmodium yoelii malaria with whole blood-stage antigens and copolymer adjuvants.

作者信息

Hunter R L, Kidd M R, Olsen M R, Patterson P S, Lal A A

机构信息

Department of Pathology and Laboratory Medicine, Emory University, Atlanta, GA 30322.

出版信息

J Immunol. 1995 Feb 15;154(4):1762-9.

PMID:7836760
Abstract

We previously reported that protection of mice from nonlethal Plasmodium yoelii malaria by immunization with whole killed blood-stage parasites was dependent on the adjuvant and that adjuvants influenced both the specificity and isotype of Ab. Additional studies with the most effective formulations were undertaken to better define the protective responses and 100% protection from lethal P. yoelii malaria was produced by three immunizations with Ag in copolymer P1004 and detoxified RaLPS as adjuvants and 83% protection was induced by a single immunization. The protection lasted for 9 mo and was associated with an anamnestic rise in Ab titer of the IgG2a isotype during the challenge infection. Passive immunization with Ab from animals that had been immunized and challenged transferred sterile immunity. Splenectomy reduced, but did not abolish, protection. These data suggest that the effective Ab is directed against labile epitopes on the surface of blood-stage parasites. The vaccines primed animals for production of such Ab, but its synthesis was efficiently induced only by challenge with live organisms.

摘要

我们之前报道过,用全灭活的血液期寄生虫免疫小鼠使其免受非致死性约氏疟原虫疟疾感染,这取决于佐剂,并且佐剂会影响抗体的特异性和同种型。我们使用最有效的配方进行了更多研究,以更好地确定保护性反应,用抗原与共聚物P1004和解毒的RaLPS作为佐剂进行三次免疫可使小鼠对致死性约氏疟原虫疟疾产生100%的保护,单次免疫可诱导83%的保护。这种保护持续了9个月,并且在攻击感染期间与IgG2a同种型抗体效价的回忆性升高有关。用已免疫并受到攻击的动物的抗体进行被动免疫可传递无菌免疫力。脾切除术可降低但不能消除保护作用。这些数据表明,有效的抗体是针对血液期寄生虫表面不稳定表位的。疫苗使动物准备产生此类抗体,但其合成仅通过活生物体攻击才能有效诱导。

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