Gomes Daniele Crespo, Fonseca-Ribeiro Maria Paula, Alves-Silva Marcus Vinicius, Palatnik-de-Sousa Clarisa B
Laboratório de Biologia e Bioquímica de Leishmania, Instituto de Microbiologia Paulo de Góes, Departamento de Microbiologia Geral, Universidade Federal do Rio de Janeiro, Rio de Janeiro, Brazil.
Front Immunol. 2025 Jul 1;16:1598755. doi: 10.3389/fimmu.2025.1598755. eCollection 2025.
Visceral leishmaniasis (VL) is a severe human vector-borne CD4-immunosuppressive disease that can be lethal if untreated soon after symptoms arise. No vaccine is available against human VL, and its chemotherapy is highly toxic and requires hospitalization. VL patients show substantially decreased CD4 total and -specific CD4+ T cell counts. nucleoside hydrolase (NH36) is a DNA metabolism enzyme and a conserved marker of the genus. It has been considered, among other antigens, a vaccine candidate. In mice vaccinated with NH36, protection against VL is mediated by a CD4 T cell response to the NH36 C-terminal domain (F3), and against cutaneous leishmaniasis (CL), by a CD4+ response against F3 and a CD8+ response against the NH36 N-terminal (F1). Vaccination with a recombinant chimera containing the F1 and F3 domains expressed in tandem (F1F3) protected mice against the heterologous CL infection by and .
In this investigation, BALB/c mice were immunized with either F1, F3, a mixture of both, or with the F1F3 chimera, plus saponin and challenged with amastigotes of , the agent of VL in America.
Before and after infection, the F1F3 chimera and the F3 vaccines promoted the highest IgA, IgM, IgG, IgG1, IgG2a, IgG2b, and IgG3 antibody responses. The F1F3 chimera promoted the strongest intradermal response against the leishmanial antigen, the highest body weight gain, and the most potent reduction of the spleen and liver relative weights. In addition, the F1F3 chimera vaccine increased the secretion of IFN-γ, and, together with the F3 vaccine, the secretion of TNF-α by splenocytes. The F1F3 chimera and the F1 vaccine also promoted the strongest secretion of IL-10, which was very low in mice immunized with F3. Thus, the IFN-γ/IL-10 and TNF-α/IL-10 ratios, characteristic of a Th1 response, were increased in mice vaccinated with F3. The F1F3 chimera and the F3 vaccine reduced the parasite load in the liver.
The F1F3 chimera, as described for the heterologous CL infections, also optimizes protection against the homologous visceral leishmaniasis infection by , by a Th1 contribution from the F3 peptide and a regulatory response from the F1 peptide. Expression of the F1 and F3 domains induced higher efficacy than the simple mixture of the F1 and F3 domains.
内脏利什曼病(VL)是一种严重的人类媒介传播的CD4免疫抑制疾病,如果在症状出现后不及时治疗可能会致命。目前尚无针对人类VL的疫苗,其化疗毒性很高且需要住院治疗。VL患者的CD4总数和特异性CD4 + T细胞计数大幅下降。核苷水解酶(NH36)是一种DNA代谢酶,也是该属的保守标志物。在其他抗原中,它被认为是一种疫苗候选物。在用NH36疫苗接种的小鼠中,对VL的保护作用由对NH36 C末端结构域(F3)的CD4 T细胞反应介导,而对皮肤利什曼病(CL)的保护作用则由对F3的CD4 +反应和对NH36 N末端(F1)的CD8 +反应介导。用含有串联表达的F1和F3结构域的重组嵌合体(F1F3)进行疫苗接种可使小鼠免受异源CL感染。
在本研究中,用F1、F3、两者的混合物或F1F3嵌合体加皂苷对BALB / c小鼠进行免疫,并用地鼠利什曼原虫(美国VL病原体)的无鞭毛体进行攻击。
在感染前后,F1F3嵌合体和F3疫苗促进了最高的IgA、IgM、IgG、IgG1、IgG2a、IgG2b和IgG3抗体反应。F1F3嵌合体促进了针对利什曼原虫抗原的最强皮内反应、最高的体重增加以及脾脏和肝脏相对重量的最有效降低。此外,F1F3嵌合体疫苗增加了IFN-γ的分泌,并且与F3疫苗一起增加了脾细胞分泌TNF-α。F1F3嵌合体和F1疫苗还促进了最强的IL-10分泌,在用F3免疫的小鼠中IL-10分泌非常低。因此,在用F3疫苗接种的小鼠中,Th1反应特征性的IFN-γ/IL-10和TNF-α/IL-10比率增加。F1F3嵌合体和F3疫苗降低了肝脏中的寄生虫负荷。
如针对异源CL感染所述,F1F3嵌合体通过F3肽的Th1贡献和F1肽的调节反应,也优化了针对同源地鼠利什曼病感染的保护作用。F1和F3结构域的表达诱导的疗效高于F1和F3结构域的简单混合物。
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