Lowrance J H, O'Sullivan F X, Caver T E, Waegell W, Gresham H D
Research Service, Harry S. Truman Veterans Affairs Medical Center, Columbia, Missouri 65201.
J Exp Med. 1994 Nov 1;180(5):1693-703. doi: 10.1084/jem.180.5.1693.
Infection with gram-negative and gram-positive bacteria remains a leading cause of death in patients with systemic lupus erythematosis (SLE), even in the absence of immunosuppressive therapy. To elucidate the mechanisms that underly the increased risk of infection observed in patients with systemic autoimmunity, we have investigated host defense against bacterial infection in a murine model of autoimmunity, the MRL/Mp-lpr/lpr (MRL/lpr) mouse. Our previous study implicated transforming growth factor beta (TGF-beta) in a novel acquired defect in neutrophil function in MRL/lpr but not congenic MRL/Mp-+/+ (MRL/n) mice (Gresham, H.D., C.J. Ray, and F.K. O'Sullivan. 1991. J. Immunol. 146:3911). We hypothesized from these observations that MRL/lpr mice would have defects in host defense against bacterial infection and that they would have constitutively higher local and systemic levels of active TGF-beta which would be responsible, at least in part, for the defect in host defense. We show in this paper that spontaneous elaboration of active TGF-beta adversely affects host defense against both gram-negative and gram-positive bacterial infection in MRL/lpr mice. Our data indicate that MRL/lpr mice, as compared with congenic MRL/n mice, exhibit decreased survival in response to bacterial infection, that polymorphonuclear leukocytes (PMN) from MRl/lpr mice fail to migrate to the site of infection during the initial stages of infection, that MRL/lpr mice have a significantly increased bacterial burden at the site of infection and at other tissue sites, and that this increased bacterial growth occurs at a time (> 20 h after infection) when PMN influx is greatly enhanced in MRL/lpr mice. Most intriguingly, the alteration in PMN extravasation during the initial stages of infection and failure to restrict bacterial growth in vivo could be duplicated in MRL/n mice with a parenteral injection of active TGF-beta 1 at the time of bacterial challenge. Moreover, these alterations in host defense, including survival in response to lethal infection, could be ameliorated in MRL/lpr mice by the parenteral administration of a monoclonal antibody that neutralizes the activity of TGF-beta. These data indicate that elaboration of TGF-beta as a result of autoimmune phenomenon suppresses host defense against bacterial infection and that such a mechanism could be responsible for the increased risk of bacterial infection observed in patients with autoimmune diseases.
革兰氏阴性菌和革兰氏阳性菌感染仍然是系统性红斑狼疮(SLE)患者死亡的主要原因,即便在未进行免疫抑制治疗的情况下也是如此。为了阐明在系统性自身免疫患者中观察到的感染风险增加背后的机制,我们在自身免疫的小鼠模型MRL/Mp-lpr/lpr(MRL/lpr)小鼠中研究了宿主对细菌感染的防御。我们之前的研究表明,转化生长因子β(TGF-β)在MRL/lpr小鼠而非同基因的MRL/Mp-+/+(MRL/n)小鼠中性粒细胞功能的一种新获得性缺陷中起作用(格雷沙姆,H.D.,C.J.雷,和F.K.奥沙利文。1991年。《免疫学杂志》146:3911)。基于这些观察结果,我们推测MRL/lpr小鼠在宿主对细菌感染的防御方面存在缺陷,并且它们体内活性TGF-β的局部和全身水平会持续较高,这至少部分地导致了宿主防御缺陷。我们在本文中表明,活性TGF-β的自发分泌对MRL/lpr小鼠抵抗革兰氏阴性菌和革兰氏阳性菌感染的宿主防御产生不利影响。我们的数据表明,与同基因的MRL/n小鼠相比,MRL/lpr小鼠在受到细菌感染时存活率降低,MRL/lpr小鼠的多形核白细胞(PMN)在感染初始阶段未能迁移到感染部位,MRL/lpr小鼠在感染部位和其他组织部位的细菌负荷显著增加,并且这种细菌生长增加发生在MRL/lpr小鼠PMN流入大大增强的时间(感染后>20小时)。最有趣的是,在细菌攻击时对MRL/n小鼠进行皮下注射活性TGF-β1,可重现感染初始阶段PMN外渗的改变以及在体内无法限制细菌生长的情况。此外,通过皮下注射中和TGF-β活性的单克隆抗体,MRL/lpr小鼠的这些宿主防御改变,包括对致死性感染的存活率,都可以得到改善。这些数据表明,自身免疫现象导致的TGF-β分泌抑制了宿主对细菌感染的防御,并且这种机制可能是自身免疫疾病患者中观察到的细菌感染风险增加的原因。
