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Dectin-1-Fc(IgG)融合蛋白抗侵袭性真菌感染的体内外疗效。

In vitro and in vivo efficacies of Dectin-1-Fc(IgG)(s) fusion proteins against invasive fungal infections.

机构信息

Laboratório de Bioquímica e Imunologia das Micoses, Instituto Biomédico, Fluminense Federal University, 24020-150, Brazil.

Programa de Pós-Graduação em Imunologia e Inflamação, Federal University of Rio de Janeiro, 21941-902, Brazil.

出版信息

Med Mycol. 2022 Aug 4;60(8). doi: 10.1093/mmy/myac050.

Abstract

UNLABELLED

Fungal infections have increased in the last years, particularly associated to an increment in the number of immunocompromised individuals and the emergence of known or new resistant species, despite the difficulties in the often time-consuming diagnosis. The controversial efficacy of the currently available strategies for their clinical management, apart from their high toxicity and severe side effects, has renewed the interest in the research and development of new broad antifungal alternatives. These encompass vaccines and passive immunization strategies with monoclonal antibodies (mAbs), recognizing ubiquitous fungal targets, such as fungal cell wall β-1,3-glucan polysaccharides, which could be used in early therapeutic intervention without the need for the diagnosis at species level. As additional alternatives, based on the Dectin-1 great affinity to β-1,3-glucan, our group developed broad antibody-like Dectin1-Fc(IgG)(s) from distinct subclasses (IgG2a and IgG2b) and compared their antifungal in vitro and passive immunizations in vivo performances. Dectin1-Fc(IgG2a) and Dectin1-Fc(IgG2b) demonstrated high affinity to laminarin and the fungal cell wall by ELISA, flow cytometry, and microscopy. Both Dectin-1-Fc(IgG)(s) inhibited Histoplasma capsulatum and Cryptococcus neoformans growth in a dose-dependent fashion. For Candida albicans, such inhibitory effect was observed with concentrations as low as 0.098 and 0.049 μg/ml, respectively, which correlated with the impairment of the kinetics and lengths of germ tubes in comparison to controls. Previous opsonization with Dectin-1-Fc(IgG)(s) enhanced considerably the macrophage antifungal effector functions, increasing the fungi macrophages interactions and significantly reducing the intraphagosome fungal survival, as lower CFUs were observed. The administration of both Dectin1-Fc(IgG)(s) reduced the fungal burden and mortality in murine histoplasmosis and candidiasis models, in accordance with previous evaluations in aspergillosis model. These results altogether strongly suggested that therapeutic interventions with Dectin-1-Fc(IgG)(s) fusion proteins could directly impact the innate immunity and disease outcome in favor of the host, by direct neutralization, opsonization, phagocytosis, and fungal elimination, providing interesting information on the potential of these new strategies for the control of invasive fungal infections.

LAY SUMMARY

Mycoses have increased worldwide, and new efficient therapeutics are needed. Passive immunizations targeting universally the fungal cell would allow early interventions without the species-level diagnosis. Lectins with affinity to carbohydrates could be used to engineer 'antibody-like' strategies.

摘要

未加说明

近年来,真菌感染有所增加,特别是与免疫功能低下个体数量的增加以及已知或新的耐药物种的出现有关,尽管诊断往往耗时且困难。目前用于临床管理的策略的疗效存在争议,除了它们的高毒性和严重的副作用外,还重新激发了对新的广泛抗真菌替代药物的研究和开发的兴趣。这些包括针对真菌细胞壁β-1,3-葡聚糖多糖等普遍存在的真菌靶标的疫苗和单克隆抗体(mAb)的被动免疫策略,可在无需进行物种水平诊断的情况下,用于早期治疗干预。作为额外的替代方案,基于 Dectin-1 对β-1,3-葡聚糖的高亲和力,我们的团队开发了来自不同亚类(IgG2a 和 IgG2b)的广谱抗体样 Dectin1-Fc(IgG)(s),并比较了它们的体外抗真菌和体内被动免疫性能。Dectin1-Fc(IgG2a)和 Dectin1-Fc(IgG2b)通过 ELISA、流式细胞术和显微镜显示出对昆布多糖和真菌细胞壁的高亲和力。两种 Dectin-1-Fc(IgG)(s)均以剂量依赖性方式抑制荚膜组织胞浆菌和新生隐球菌的生长。对于白色念珠菌,以低至 0.098 和 0.049μg/ml 的浓度观察到这种抑制作用,与与对照相比,芽管的动力学和长度受损相关。用 Dectin-1-Fc(IgG)(s)预先调理大大增强了巨噬细胞的抗真菌效应功能,增加了真菌与巨噬细胞的相互作用,并显著降低了吞噬体内真菌的存活,因为观察到较低的 CFU。在组织胞浆菌病和念珠菌病模型中,给予 Dectin1-Fc(IgG)(s)均可降低真菌负荷和死亡率,与曲霉病模型中的先前评估一致。这些结果强烈表明,通过直接中和、调理、吞噬和真菌消除,用 Dectin-1-Fc(IgG)(s)融合蛋白进行的治疗干预可能直接影响宿主的固有免疫和疾病结局,为控制侵袭性真菌感染提供了有价值的信息。

总结

世界各地的真菌病都有所增加,需要新的有效疗法。针对真菌普遍存在的细胞的被动免疫可以在无需进行物种水平诊断的情况下进行早期干预。具有碳水化合物亲和力的凝集素可用于设计“抗体样”策略。

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