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交替活化巨噬细胞在蠕虫感染中的不同作用

The divergent roles of alternatively activated macrophages in helminthic infections.

作者信息

Reyes J L, Terrazas L I

机构信息

Laboratory of Immunoparasitology, Unidad de Biomedicina, Facultad de Estudios Superiores-Iztacala, Universidad Nacional Autónoma de México, Mexico.

出版信息

Parasite Immunol. 2007 Dec;29(12):609-19. doi: 10.1111/j.1365-3024.2007.00973.x.

Abstract

Macrophages play crucial roles in the immune response, as they can initiate, modulate and also be final effector cells during immune responses to infections. Macrophages are derived from myeloid precursor cells in bone marrow and are widely distributed in every tissue of the body. Over the past 10 years, the concepts about macrophage activation have clearly changed; macrophages are not called activated or inactivated as they used to be. These changes in the concept of macrophage response is the result of many in vitro and in vivo studies, but the major support for the current concept of alternatively activated macrophages (AAMphi) comes from parasitic helminth infections. Parasitic helminths have developed complex mechanisms to evade and modulate host immunity. Infections with these parasites induce strong polarized Th2-type immune responses frequently associated with impaired T-cell proliferative responses to parasitic or unrelated antigens. Given the recent advances in understanding the immunoregulatory capabilities of helminthic infections, it has been suggested that macrophages can be a target for immunomodulation. Furthermore, they become altered when a host experiences chronic exposure to helminth parasites or their by-products, which favour the induction of AAMphi. How AAMphi participate in modulating host immunity during helminth infections and what their roles are in clearing or favouring parasite survival remains elusive. Here we review the most recent advances in the literature on AAMphi at the host-parasite interface, including three classes of helminths: nematodes (Brugia, Nippostrongylus, Litomosoides, Heligmosomoides), trematodes (Schistosoma, Fasciola) and cestodes (Taenia, Echinococcus, Hymenolepis).

摘要

巨噬细胞在免疫反应中发挥着关键作用,因为它们在对感染的免疫反应过程中可以启动、调节免疫反应,并且还是最终的效应细胞。巨噬细胞起源于骨髓中的髓样前体细胞,广泛分布于身体的各个组织。在过去十年中,关于巨噬细胞激活的概念发生了明显变化;巨噬细胞不再像过去那样被简单地称为激活或未激活状态。巨噬细胞反应概念的这些变化是许多体外和体内研究的结果,但目前关于替代性激活巨噬细胞(AAMphi)概念的主要支持来自寄生虫感染。寄生蠕虫已经发展出复杂的机制来逃避和调节宿主免疫。感染这些寄生虫会引发强烈的极化Th2型免疫反应,这种反应通常与对寄生虫或无关抗原的T细胞增殖反应受损有关。鉴于最近在理解蠕虫感染的免疫调节能力方面取得的进展,有人提出巨噬细胞可以成为免疫调节的靶点。此外,当宿主长期接触蠕虫寄生虫或其副产物时,巨噬细胞会发生改变,这有利于诱导AAMphi。AAMphi在蠕虫感染期间如何参与调节宿主免疫以及它们在清除寄生虫或促进寄生虫存活中的作用仍然不清楚。在这里,我们综述了关于宿主 - 寄生虫界面处AAMphi的文献中的最新进展,包括三类蠕虫:线虫(布鲁氏线虫、日本血吸虫、丝状线虫、Heligmosomoides)、吸虫(血吸虫、肝片吸虫)和绦虫(绦虫、棘球绦虫、微小膜壳绦虫)。

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