Carrillo Eugenia, Fernandez Laura, Ibarra-Meneses Ana Victoria, Santos Micheli L B, Nico Dirlei, de Luca Paula M, Correa Cristiane Bani, de Almeida Roque Pacheco, Moreno Javier, Palatnik-de-Sousa Clarisa B
WHO Collaborating Centre for Leishmaniasis, Centro Nacional de Microbiologia, Instituto de Salud Carlos III, Madrid, Spain.
Departamento de Medicina, Hospital Universitário, Universidade Federal de Sergipe, Aracaju, Brazil.
Front Immunol. 2017 Jul 12;8:750. doi: 10.3389/fimmu.2017.00750. eCollection 2017.
The nucleoside hydrolase NH36 is the main antigen of the Leishmune vaccine and one of the promising candidates for vaccination against visceral leishmaniasis. The antigenicity of the N-terminal (F1), the central (F2), or the C-terminal recombinant domain (F3) of NH36 was evaluated using peripheral blood mononuclear cells (PBMC) from individuals infected with from an endemic area of visceral leishmaniasis of Spain. Both NH36 and F1 domains significantly increased the PBMC proliferation stimulation index of cured patients and infected asymptomatic individuals compared to healthy controls. Moreover, F1 induced a 19% higher proliferative response than NH36 in asymptomatic exposed subjects. In addition, in patients cured from visceral leishmaniasis, proliferation in response to NH36 and F1 was accompanied by a significant increase of IFN-γ and TNF-α secretion, which was 42-43% higher, in response to F1 than to NH36. The interleukin 17 (IL-17) secretion was stronger in asymptomatic subjects, in response to F1, as well as in cured cutaneous leishmaniasis after NH36 stimulation. While no IL-10 secretion was determined by F1, a granzyme B increase was detected in supernatants from cured patients after stimulation with either NH36 or F1. These data demonstrate that F1 is the domain of NH36 that induces a recall cellular response in individuals with acquired resistance to the infection by . In addition, F1 and NH36 discriminated the IgG3 humoral response in patients with active visceral leishmaniasis due to (Ethiopia) and (Spain) from that of endemic and non-endemic area controls. NH36 showed higher reactivity with sera from -infected individuals, indicating species specificity. We conclude that the F1 domain, previously characterized as an inducer of the Th1 and Th17 responses in cured/exposed patients infected with , may also be involved in the generation of a protective response against and represents a potential vaccine candidate for the control of human leishmaniasis alone, or in combination with other HLA epitopes/antigens.
核苷水解酶NH36是利什曼疫苗的主要抗原,也是用于预防内脏利什曼病的有前景的候选疫苗之一。使用来自西班牙内脏利什曼病流行地区感染个体的外周血单核细胞(PBMC),评估了NH36的N端(F1)、中央(F2)或C端重组结构域(F3)的抗原性。与健康对照相比,NH36和F1结构域均显著提高了治愈患者和感染无症状个体的PBMC增殖刺激指数。此外,在无症状暴露个体中,F1诱导的增殖反应比NH36高19%。此外,在内脏利什曼病治愈的患者中,对NH36和F1的增殖反应伴随着IFN-γ和TNF-α分泌的显著增加,对F1的反应比NH36高42-43%。在无症状个体中,白细胞介素17(IL-17)对F1的分泌更强,在NH36刺激后治愈的皮肤利什曼病患者中也是如此。虽然F1未检测到IL-10分泌,但在用NH36或F1刺激后,在治愈患者的上清液中检测到颗粒酶B增加。这些数据表明,F1是NH36的一个结构域,可在对感染具有获得性抗性的个体中诱导回忆性细胞反应。此外,F1和NH36区分了因杜氏利什曼原虫(埃塞俄比亚)和婴儿利什曼原虫(西班牙)导致的活动性内脏利什曼病患者与流行和非流行地区对照的IgG3体液反应。NH36与杜氏利什曼原虫感染个体的血清反应性更高,表明具有种属特异性。我们得出结论,F1结构域先前被表征为在感染杜氏利什曼原虫的治愈/暴露患者中Th1和Th17反应的诱导剂,它也可能参与针对杜氏利什曼原虫的保护性反应的产生,并且单独或与其他HLA表位/抗原联合,是控制人类利什曼病的潜在候选疫苗。
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