Tian Wei, Zeng Xiao-Min, Li Li-Xin, Jin He-Kun, Luo Qi-Zhi, Wang Fan, Guo Shi-Shi, Cao Ya
Department of Immunology, Xiang-Ya School of Medicine, Central South University, Changsha, Hunan, 410078, People's Republic of China.
Immunogenetics. 2006 Apr;58(2-3):113-21. doi: 10.1007/s00251-006-0093-6. Epub 2006 Mar 18.
Previous studies have identified several HLA-B specificities that are associated with nasopharyngeal carcinoma (NPC) in populations of Chinese descent, in particular HLA-B35, -B38, -B46, and -B58. Perhaps except for HLA-B46, other associations cannot be simply accounted for by the linkage disequilibrium between HLA-A and B loci. The human major histocompatibility complex (MHC) class I chain-related gene A (MICA) maps 46 kb centromeric to HLA-B and is highly polymorphic; it encodes a stress-inducible protein which functions as a ligand for the NKG2D/DAP10 complex to activate natural killer (NK) cells, gammadelta T cells, and CD8(+) T cells. We postulated MICA gene as a susceptibility factor for nasopharyngeal carcinoma, an Epstein-Barr virus-associated malignancy. In this study, 218 unrelated patients newly diagnosed with NPC and 196 randomly selected healthy controls from southern China mainland were analyzed for the short tandem repeat polymorphism of exon 5 of MICA gene (MICA-STR) and MICA gene deletion, using fluorescent polymerase chain reaction-gene scanning (PCR/size-sequencing) and polymerase chain reaction-sequence-specific priming (PCR/SSP) technology. MICAA9 was present at significantly increased frequency in the patient group (P (C)=0.0001002, OR=2.528, 95% CI=1.636-3.907), whereas the frequency of MICAA5.1 was significantly decreased (P (C)=0.006, OR=0.594, 95% CI=0.437-0.806). Gender-based stratification revealed a significant increase of MICAA9 frequency (P (C)=0.000072, OR=3.255, 95% CI=1.855-5.709) and a significant decrease of MICAA5.1 frequency (P (C)=0.000737, OR=0.486, 95% CI=0.337-0.702) in male patients with NPC (N=166), compared with male normal controls (N=120). A significant interaction between MICAA9 and gender was observed ([see text]=41.58, P=0.0001). Statistics also revealed heterogeneity of effects among MICAA5.1/MICAA9-bearing phenotypes and a dose-dependent effect of MICAA5.1 and MICAA9 on NPC risk in male subgroup. This constitutes the first demonstration of a gender-specific association between MICA-STR polymorphism and NPC, which could largely be attributable to the underlying gender-related mechanisms that modulate MICA gene expression. The results provide strong supporting evidence suggesting that MICAA9 may be a genetic risk factor for NPC in male individuals in this population. The potential interaction between MICA and other non-HLA host factors and environmental exposures remains to be further studied.
以往研究已确定了几种与中国血统人群鼻咽癌(NPC)相关的HLA - B特异性,特别是HLA - B35、- B38、- B46和 - B58。或许除了HLA - B46外,其他关联不能简单地用HLA - A和B位点之间的连锁不平衡来解释。人类主要组织相容性复合体(MHC)I类链相关基因A(MICA)定位于HLA - B着丝粒方向46 kb处,且具有高度多态性;它编码一种应激诱导蛋白,作为NKG2D / DAP10复合体的配体,可激活自然杀伤(NK)细胞、γδ T细胞和CD8(+) T细胞。我们推测MICA基因是鼻咽癌(一种与爱泼斯坦 - 巴尔病毒相关的恶性肿瘤)的易感因素。在本研究中,采用荧光聚合酶链反应 - 基因扫描(PCR / 大小测序)和聚合酶链反应 - 序列特异性引物(PCR / SSP)技术,对218例新诊断的NPC无关患者和196例从中国大陆南方随机选取的健康对照进行了MICA基因第5外显子短串联重复多态性(MICA - STR)和MICA基因缺失分析。MICAA9在患者组中的出现频率显著增加(P(C)=0.0001002,OR = 2.528,95% CI = 1.636 - 3.907),而MICAA5.1的频率显著降低(P(C)=0.006,OR = 0.594,95% CI = 0.437 - 0.806)。基于性别的分层显示,与男性正常对照(n = 120)相比,男性NPC患者(n = 166)中MICAA9频率显著增加(P(C)=0.000072,OR = 3.255,95% CI = 1.855 - 5.709),MICAA5.1频率显著降低(P(C)=0.000737,OR = 0.486,95% CI = 0.337 - 0.702)。观察到MICAA9与性别之间存在显著相互作用([见正文]=41.58,P = 0.0001)。统计分析还揭示了携带MICAA5.1 / MICAA9表型之间效应的异质性以及MICAA5.1和MICAA9对男性亚组中NPC风险的剂量依赖性效应。这首次证明了MICA - STR多态性与NPC之间存在性别特异性关联,这在很大程度上可能归因于调节MICA基因表达的潜在性别相关机制。结果提供了有力的支持证据,表明MICAA9可能是该人群男性个体中NPC的遗传危险因素。MICA与其他非HLA宿主因素及环境暴露之间的潜在相互作用仍有待进一步研究。
