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抗体向皮肤的转运仅部分依赖于新生 Fc 受体。

Transport of antibody into the skin is only partially dependent upon the neonatal Fc-receptor.

机构信息

Johns Hopkins Malaria Institute and Johns Hopkins Bloomberg School of Public Health, Baltimore, Maryland, United States of America.

出版信息

PLoS One. 2023 Apr 24;18(4):e0273960. doi: 10.1371/journal.pone.0273960. eCollection 2023.

Abstract

The dermis is the portal of entry for most vector-transmitted pathogens, making the host's immune response at this site critical in mitigating the magnitude of infection. For malaria, antibody-mediated neutralization of Plasmodium parasites in the dermis was recently demonstrated. However, surprisingly little is known about the mechanisms that govern antibody transport into the skin. Since the neonatal Fc receptor (FcRn) has been shown to transcytose IgG into various tissues, we sought to understand its contribution to IgG transport into the skin and antibody-mediated inhibition of Plasmodium parasites following mosquito bite inoculation. Using confocal imaging, we show that the transport of an anti-Langerin mAb into the skin occurs but is only partially reduced in mice lacking FcRn. To understand the relevance of FcRn in the context of malaria infection, we use the rodent parasite Plasmodium berghei and show that passively-administered anti-malarial antibody in FcRn deficient mice, does not reduce parasite burden to the same extent as previously observed in wildtype mice. Overall, our data suggest that FcRn plays a role in the transport of IgG into the skin but is not the major driver of IgG transport into this tissue. These findings have implications for the rational design of antibody-based therapeutics for malaria as well as other vector-transmitted pathogens.

摘要

真皮是大多数媒介传播病原体的入口,因此宿主在该部位的免疫反应对于减轻感染程度至关重要。最近已经证明,在真皮中抗体介导的疟原虫寄生虫中和作用。然而,对于控制抗体向皮肤转运的机制,人们知之甚少。由于新生 Fc 受体(FcRn)已被证明可将 IgG 转导到各种组织中,因此我们试图了解其对 IgG 向皮肤转运以及蚊虫叮咬接种后抗体介导的疟原虫寄生虫抑制的贡献。通过共聚焦成像,我们表明抗 Langerin mAb 进入皮肤的转运确实发生了,但在缺乏 FcRn 的小鼠中仅部分减少。为了了解 FcRn 在疟疾感染背景下的相关性,我们使用啮齿动物寄生虫疟原虫 berghei 并表明,在 FcRn 缺陷型小鼠中被动给予抗疟抗体并不能像以前在野生型小鼠中观察到的那样,将寄生虫负担降低到相同程度。总体而言,我们的数据表明 FcRn 在 IgG 向皮肤的转运中起作用,但不是 IgG 向该组织转运的主要驱动因素。这些发现对于基于抗体的疟疾治疗以及其他媒介传播病原体的合理设计具有重要意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d47c/10124839/c66e1d5daafa/pone.0273960.g001.jpg

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