科学家报道：sle中巨噬细胞失去了灵活性触发人体免疫防疫系统

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来源:觅健 2015-07-06 09:58:34

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文章来源：Science Daily

翻译：病患如我社区

转载请注明来源“病患如我”社区

日期：2015/06/22

来源：伯明翰阿拉巴马大学

摘要：巨噬细胞清除消化死细胞和防止自身免疫反应时需要灵活性。科学家报道，在红斑狼疮中巨噬细胞失去了这种灵活性

每天人体中有超过500亿的细胞死亡，这种程序性的细胞死亡过程称为凋亡。这些细胞进行内部的降解，断裂成细胞小体随后被免疫细胞清除，这整个过程是在没有触发人体免疫防御系统的情况下进行的。

细胞在脾脏淋巴结附近死亡是最危险的情况之一。淋巴结通过增加剧烈的免疫活动来应对传染性细菌和病毒。如果凋亡细胞（AC，正在进行程序性死亡的细胞）进入淋巴结将会引发自身免疫应答。这将导致如系统性红斑狼疮这样的自身免疫性疾病，这种疾病中免疫系统会攻击自身健康组织。

在脾脏边缘部位的淋巴结附近的巨噬细胞可以阻挡住AC细胞，就像是足球中的防线或“最终驱逐屏障”，伯明翰阿拉巴马大学临床免疫学和风湿病部门医学教授，医学博士John Mountz说。

在一篇于6月22日发表于在线版《临床医学》杂志的文章中，Mountz和他的同事们博士Hui-Chen Hsu和博士Hao Li，用狼疮小鼠的新模型展示了为什么这种防线会存在漏洞，并且展示了这种崩溃下的机制。就像“地段、地段、地段”是区分好坏房产的标准，Mountz的小组和同事说B细胞免疫系统的位置也是区别健康动物和会发展成自身免疫性疾病动物的关键。错误的位置会导致巨噬细胞的细胞骨架产生问题，这些将会导致细胞僵化的吞食和消化死亡细胞。

Mountz等发现存在于淋巴外部边缘区域的B细胞对于保持巨噬细胞防线的稳定性至关重要。他们发现在狼疮病症中含量升高的I型干扰素会导致B细胞迁离边缘区域而进入淋巴结，这将阻断B细胞与边缘区域巨噬细胞之间的重要交流。在这个模型中，自身免疫治病B细胞的定义是建立在它的解剖位置上的。

Mountz小组的实验展示了这种交流的机制：边缘位置的B细胞通过其细胞膜表面的淋巴毒素与边缘位置的巨噬细胞进行交流。淋巴毒素与巨噬细胞表面的淋巴毒素受体结合。这种结合激发了巨噬细胞中的机械传感复合体，随后激活了一种称为成巨核细胞造血细胞1（MKL1）的基因调控器的产生，MKL1可调控细胞肌动蛋白细胞骨架并且可使巨噬细胞对AC细胞进行应答并且吞食它们。没了这种与B细胞间的交流，巨噬细胞中MKL1的表达量的减少会改变肌动蛋白细胞骨架的活动。

这种信号轴——从B细胞到巨噬细胞再到机械传感信号——使巨噬细胞防线保持健康坚固。相比，MKL1基因被敲除的小鼠随着年龄的增加开始与狼疮模型小鼠情况相似。MKL1基因敲除小鼠展现了AC细胞清除量减少，脾脏淋巴结边缘区域的巨噬细胞缺陷以及自身免疫抗体的产生增加等现象。这表明了巨噬细胞机械传感信号通路在狼疮病中的重要性。

检测系统性红斑狼疮病患的脾脏切片发现了与两种狼疮小鼠模型相似的规律：淋巴结附近的B细胞数量减少，淋巴结内部B细胞数量增加以及边缘区域的MKL1基因表达量减少。

“除非感觉到了周围环境，细胞是不会做任何事情的，”Mountz说，不论感觉到的是热度、化学信号、含氧量、机械接触还是其他刺激。“我们知道狼疮病中，抵抗AC细胞的抗体大量产生。研究人员认为这可能与巨噬细胞不能吃掉和消化掉AC细胞有关。有很多假设已经被提出，但是没有人知道最根本的原因。”

“这篇文章表明免疫系统也是有机械感应调节的，”Mountz说。

他说这篇报道首次阐明了脆弱细胞（巨噬细胞的移动和它吞食AC细胞的作用，由慢性I型干扰素诱发）与红斑狼疮之间的联系。

与这篇文章相关的是一篇发表在JCI上的评论文章，由英国伦敦大学学院的Claudia Mauri 和Madhvi Menon撰写，题目是“在系统性红斑狼疮中I型干扰素的多面性。”他们写道，“这项研究的结果为了解阻止AC细胞清除作用的因素提供了线索，并且促进了系统性红斑狼疮的发展。”

原文：

Hui-Chen Hsu and John Mountz

Credit: UAB

More than 50 billion cells die in the human body every day, a spectacle of programmed cell death called apoptosis. These cells undergo internal degradation and then fracture into apoptotic bodies that are scavenged by immune cells, all without triggering the body's immune system defense.

One of the most dangerous places for cells to die is near the follicles of the spleen. The follicles are primed to mount intense immune attacks against infectious bacteria or viruses. If an apoptotic cell (AC, a cell undergoing programmed cell death) goes into the follicle, it can trigger an autoimmune response. This can lead to autoimmune diseases like systemic lupus erythematosus, where the immune system attacks its own body.

Macrophages in the spleen marginal zone around the follicles keep the ACs out, acting like the defensive line in football or a "final exclusion barrier," says John Mountz, M.D., Ph.D., professor of medicine in the University of Alabama at Birmingham Division of Clinical Immunology and Rheumatology.

In a paper published online in the Journal of Clinical Investigation on June 22, Mountz and colleagues, including Hui-Chen Hsu, Ph.D., and Hao Li, Ph.D., present a new model of why this defensive line becomes porous in mouse models of lupus, and they show the mechanism that underlies this breakdown. Just as "location, location, location" is the difference between good and bad real estate, the Mountz group and colleagues say that the location of immune system B cells is a key difference between healthy animals and those that develop autoimmune disease. The wrong location leads to macrophage cells that have problems in their cytoskeletons -- they become too stiff to engulf and digest dead cells.

Mountz and colleagues found that the presence of B cells in the marginal zone outside the follicle is essential to maintain the defensive line of macrophages. They found that type I interferon -- which is elevated in lupus -- causes the B cells to migrate away from the marginal zone and into the follicle, which interrupts vital cross-talk between the B cells and the marginal zone macrophages. In this model, the definition of an autoimmune pathogenic B cell is now based on its anatomic location.

Experiments by the Mountz group show the mechanism of this cross-talk: B cells in the marginal zone of the follicle interact with the marginal zone macrophages by means of a membrane lymphotoxin present on the surface of the B cells. This lymphotoxin binds to a lymphotoxin receptor on the surface of the macrophages. That connection stimulates a mechanosensing complex in the macrophage, triggering the production of a gene regulator called megakaryoblastic leukemia 1 (MKL1) that regulates the cell's actin cytoskeleton and enables a macrophage to respond to and engulf ACs. Without that B cell interaction, MKL1 expression in the macrophage decreases, changing the activity of the actin cytoskeleton.

This signaling axis -- from B cell to macrophage to mechanosensing signaling -- keeps the defensive line of macrophages strong and healthy. In contrast, mice that have had the MKL1 gene knocked out begin to resemble lupus-model mice as they age. They show decreased AC clearance, a deficiency of macrophages in the marginal zone of spleen follicles and increased production of autoimmune antibodies. This suggests a key role for macrophage mechanosensing signaling in lupus.

Examination of slides of spleens from human systemic lupus erythematosus patients showed a pattern similar to that seen in two mouse models of lupus: reduced numbers of B cells surrounding the follicle, increased numbers of B cells inside the follicle and a loss of MKL1 expression in the marginal zone.

"A cell doesn't do anything unless it senses its environment," said Mountz, whether the sensation is heat, chemical signals, oxygen availability, mechanical touching or other stimuli. "We knew that, in lupus, there was an overwhelming production of antibodies against materials derived from ACs. Researchers thought that this may be related to failure of macrophages to eat and digest ACs. Many possibilities have been suggested, but no one knew the basic cause."

"This paper shows that the immune system is also regulated by mechanosensing," Mountz said.

He says this paper is the first connection between poor agility of a cell (the movement of the macrophage and its engulfment of ACs, as a result of chronic type I interferon stimulation) and the etiology of lupus.

The paper is accompanied by a commentary in JCI by Claudia Mauri and Madhvi Menon, University College London, titled, "The many faces of type I interferon in systemic lupus erythematosus." They write that, "The results of this study provide important insight into factors that inhibit AC clearance and promote the development of systemic lupus erythematosus."

Story Source:

The above post is reprinted from materials provided by University of Alabama at Birmingham. Note: Materials may be edited for content and length.