Martin Annalise M, Almeida Coral-Ann, Cameron Paul, Purcell Anthony W, Nolan David, James Ian, McCluskey James, Phillips Elizabeth, Landay Alan, Mallal Simon
Centre for Clinical Immunology and Biomedical Statistics, Royal Perth Hospital and Murdoch University, Perth, Western Australia 6000, Australia.
AIDS. 2007 Jun 19;21(10):1233-44. doi: 10.1097/QAD.0b013e3280119579.
A potentially life-threatening hypersensitive reaction accompanies the use of HIV nucleoside analogue abacavir (ABC) in 4-8% of Caucasian individuals. HLA-B*5701 and Hsp70 493T alleles have been shown to predict susceptibility to this hypersensitivity.
This study was undertaken to provide a mechanistic understanding of the highly significant genetic association of HLA Class I and Hsp70 alleles with ABC hypersensitivity.
In this study an ABC-induced localization of intracellular HSP70 to endosomal vesicles of antigen-presenting cells was demonstrated. This ABC-stimulated redistribution of endogenous HSP70 was substantially higher in the genetically homogenous HLA-B*5701, Hsp70 493T ABC-hypersensitive individuals and ABC-naive individuals in comparison with the heterogeneous tolerant patients (P = 0.023). Increased expression of HSP70 was also detected in the hypersensitive group as measured by flow cytometry (P = 0.032). Blocking of HSP70 and HSP70 cell surface receptors CD14 and TLR2 abrogated ABC-stimulated HSP70 redistribution in sensitized individuals to basal levels (P < 0.004). In addition, the use of TcRalphabeta and HLA-B57/58 antibodies also ablated the expression of HSP70. Cells expressing the activation markers CD40 were increased after ABC stimulation in the hypersensitive patients (P = 0.006). ABC-stimulated interferon-gamma levels were higher in hypersensitive patients in comparison with ABC-tolerant individuals with a mean of 123.54 versus 0 pg/ml (P = 0.001).
The present data indicates that ABC stimulates an innate immune response and activates antigen-presenting cells via the endogenous HSP70-mediated Toll-like receptor pathway in genetically susceptible individuals potentially initiating the immuno-pathological hypersensitive response.
在4% - 8%的白种人中,使用人类免疫缺陷病毒核苷类似物阿巴卡韦(ABC)会伴随出现潜在危及生命的超敏反应。已证明HLA - B*5701和热休克蛋白70(Hsp70)493T等位基因可预测对这种超敏反应的易感性。
进行本研究以从机制上理解HLA I类和Hsp70等位基因与ABC超敏反应之间高度显著的遗传关联。
在本研究中,证明了ABC诱导细胞内HSP70定位到抗原呈递细胞的内体囊泡。与异质耐受患者相比,在基因同质的HLA - B*5701、Hsp70 493T ABC超敏个体和未接触过ABC的个体中,这种ABC刺激的内源性HSP70重新分布显著更高(P = 0.023)。通过流式细胞术检测,超敏组中也检测到HSP70表达增加(P = 0.032)。阻断HSP70和HSP70细胞表面受体CD14和TLR2可将致敏个体中ABC刺激的HSP70重新分布消除至基础水平(P < 0.004)。此外,使用T细胞受体αβ和HLA - B57/58抗体也消除了HSP70的表达。超敏患者在ABC刺激后表达激活标志物CD40的细胞增加(P = 0.006)。与ABC耐受个体相比,超敏患者中ABC刺激的干扰素 - γ水平更高,平均值分别为123.54与0 pg/ml(P = 0.001)。
目前的数据表明,在基因易感个体中,ABC通过内源性HSP70介导的Toll样受体途径刺激先天性免疫反应并激活抗原呈递细胞,可能引发免疫病理超敏反应。
