McDermott M F, Aksentijevich I, Galon J, McDermott E M, Ogunkolade B W, Centola M, Mansfield E, Gadina M, Karenko L, Pettersson T, McCarthy J, Frucht D M, Aringer M, Torosyan Y, Teppo A M, Wilson M, Karaarslan H M, Wan Y, Todd I, Wood G, Schlimgen R, Kumarajeewa T R, Cooper S M, Vella J P, Amos C I, Mulley J, Quane K A, Molloy M G, Ranki A, Powell R J, Hitman G A, O'Shea J J, Kastner D L
Medical Unit, St. Bartholomew's and the Royal London Hospital School of Medicine and Dentistry, Whitechapel, London, England.
Cell. 1999 Apr 2;97(1):133-44. doi: 10.1016/s0092-8674(00)80721-7.
Autosomal dominant periodic fever syndromes are characterized by unexplained episodes of fever and severe localized inflammation. In seven affected families, we found six different missense mutations of the 55 kDa tumor necrosis factor receptor (TNFR1), five of which disrupt conserved extracellular disulfide bonds. Soluble plasma TNFR1 levels in patients were approximately half normal. Leukocytes bearing a C52F mutation showed increased membrane TNFR1 and reduced receptor cleavage following stimulation. We propose that the autoinflammatory phenotype results from impaired downregulation of membrane TNFR1 and diminished shedding of potentially antagonistic soluble receptor. TNFR1-associated periodic syndromes (TRAPS) establish an important class of mutations in TNF receptors. Detailed analysis of one such mutation suggests impaired cytokine receptor clearance as a novel mechanism of disease.
常染色体显性遗传性周期性发热综合征的特征是不明原因的发热发作和严重的局部炎症。在七个患病家族中,我们发现了55 kDa肿瘤坏死因子受体(TNFR1)的六种不同错义突变,其中五种破坏了保守的细胞外二硫键。患者血浆中可溶性TNFR1水平约为正常水平的一半。携带C52F突变的白细胞在刺激后显示膜TNFR1增加且受体裂解减少。我们认为,自身炎症表型是由于膜TNFR1下调受损以及潜在拮抗可溶性受体的脱落减少所致。TNFR1相关周期性综合征(TRAPS)在TNF受体中建立了一类重要的突变。对其中一种此类突变的详细分析表明,细胞因子受体清除受损是一种新的疾病机制。
