Cazorla Silvia I, Matos Marina N, Cerny Natacha, Ramirez Carolina, Alberti Andrés Sanchez, Bivona Augusto E, Morales Celina, Guzmán Carlos A, Malchiodi Emilio L
Cátedra de Inmunología and Instituto de Estudios de la Inmunidad Humoral Dr. R. A. Margni, Consejo Nacional de Investigaciones Científicas y Técnicas-Universidad de Buenos Aires (CONICET-UBA), Facultad de Farmacia y Bioquímica, Universidad de Buenos Aires Instituto de Microbiología y Parasitología Médica (IMPaM), UBA-CONICET and Departamento de Microbiología, Parasitología e Inmunología, Facultad de Medicina, UBA.
Departamento de Patología, Facultad de Medicina UBA, Instituto de Fisiopatología Cardiovascular, Buenos Aires, Argentina.
J Infect Dis. 2015 Mar 1;211(5):698-707. doi: 10.1093/infdis/jiu480. Epub 2014 Aug 25.
We have reported that attenuated Salmonella (S) carrying plasmids encoding the cysteine protease cruzipain (Cz) protects against Trypanosoma cruzi infection. Here, we determined whether immunoprotection could be improved by the oral coadministration of 3 Salmonella carrying the plasmids that encode the antigens Cz, Tc52, and Tc24. SCz+STc52+STc24-immunized mice presented an increased antibody response against each antigen compared with those in the single antigen-immunized groups, as well as higher trypomastigotes antibody-mediated lyses and cell invasion inhibition compared with controls. SCz+STc52+STc24-immunized and -challenged mice rendered lower parasitemia. Weight loss after infection was detected in all mice except those in the SCz+STc52+STc24 group. Moreover, cardiomyopathy-associated enzyme activity was significantly lower in SCz+STc24+STc52-immunized mice compared with controls. Few or no abnormalities were found in muscle tissues of SCz+STc24+STc52-immunized mice, whereas controls presented with inflammatory foci, necrosis, and amastigote nests. We conclude that a multicomponent approach that targets several invasion and metabolic mechanisms improves protection compared with single-component vaccines.
我们曾报道,携带编码半胱氨酸蛋白酶克氏锥虫蛋白酶(Cz)质粒的减毒沙门氏菌(S)可预防克氏锥虫感染。在此,我们确定通过口服共同给予携带编码抗原Cz、Tc52和Tc24质粒的3种沙门氏菌,免疫保护作用是否能够得到改善。与单抗原免疫组相比,SCz+STc52+STc24免疫的小鼠对每种抗原的抗体反应增强,并且与对照组相比,其锥鞭毛体抗体介导的裂解作用和细胞侵袭抑制作用更高。SCz+STc52+STc24免疫并受到攻击的小鼠的寄生虫血症较低。除SCz+STc52+STc24组的小鼠外,所有小鼠在感染后均出现体重减轻。此外,与对照组相比,SCz+STc24+STc52免疫的小鼠中与心肌病相关的酶活性显著降低。在SCz+STc24+STc52免疫的小鼠的肌肉组织中几乎未发现或未发现异常,而对照组则出现炎症灶、坏死和无鞭毛体巢。我们得出结论,与单组分疫苗相比,针对多种侵袭和代谢机制的多组分方法可提高保护作用。
