Butterfield R J, Blankenhorn E P, Roper R J, Zachary J F, Doerge R W, Sudweeks J, Rose J, Teuscher C
Department of Veterinary Pathobiology, University of Illinois at Urbana-Champaign, Urbana, IL 61802, USA.
J Immunol. 1999 Mar 1;162(5):3096-102.
Experimental allergic encephalomyelitis (EAE) is the principal animal model of multiple sclerosis (MS), the major inflammatory disease of the central nervous system. Murine EAE is generally either an acute monophasic or relapsing disease. Because the clinical spectrum of MS is more diverse, the limited range of disease subtypes observed in EAE has raised concern regarding its relevance as a model for MS. During the generation of a large F2 mapping population between the EAE-susceptible SJL/J and EAE-resistant B10.S/DvTe inbred lines, we identified four distinct subtypes of murine EAE resembling clinical subtypes seen in MS. We observed acute progressive, chronic/nonremitting, remitting/relapsing, and monophasic remitting/nonrelapsing EAE. An additional subtype, benign EAE, was identified after histologic examination revealed that some mice had inflammatory infiltrates of the central nervous system, but did not show clinical signs of EAE. Genome exclusion mapping was performed to identify the loci controlling susceptibility to each disease subtype. We report three novel EAE-modifying loci on chromosomes 16, 7, and 13 (eae11-13, respectively). Additionally, unique loci with gender-specific effects govern susceptibility to remitting/relapsing (eae12) and monophasic remitting/nonrelapsing (eae7 and 13) EAE.
实验性自身免疫性脑脊髓炎(EAE)是多发性硬化症(MS)的主要动物模型,MS是中枢神经系统的主要炎症性疾病。小鼠EAE通常是急性单相或复发性疾病。由于MS的临床谱更为多样,EAE中观察到的疾病亚型范围有限,这引发了人们对其作为MS模型相关性的担忧。在EAE易感的SJL/J和EAE抗性的B10.S/DvTe近交系之间产生大量F2定位群体的过程中,我们鉴定出了四种不同的小鼠EAE亚型,类似于MS中所见的临床亚型。我们观察到急性进行性、慢性/非缓解性、缓解/复发性和单相缓解/非复发性EAE。在组织学检查显示一些小鼠有中枢神经系统的炎性浸润但未表现出EAE临床症状后,鉴定出了另一种亚型,即良性EAE。进行了基因组排除定位以确定控制每种疾病亚型易感性的基因座。我们报告了位于16号、7号和13号染色体上的三个新的EAE修饰基因座(分别为eae11 - 13)。此外,具有性别特异性效应的独特基因座控制着对缓解/复发性(eae12)和单相缓解/非复发性(eae7和13)EAE的易感性。
