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鉴定与外周血淋巴细胞的自然细胞毒性活性和癌症免疫监视相关的NKG2D单倍型。

Identification of the NKG2D haplotypes associated with natural cytotoxic activity of peripheral blood lymphocytes and cancer immunosurveillance.

作者信息

Hayashi Tomonori, Imai Kazue, Morishita Yukari, Hayashi Ikue, Kusunoki Yoichiro, Nakachi Kei

机构信息

Department of Radiobiology/Molecular Epidemiology, Radiation Effects Research Foundation, Hiroshima, Japan.

出版信息

Cancer Res. 2006 Jan 1;66(1):563-70. doi: 10.1158/0008-5472.CAN-05-2776.

DOI:10.1158/0008-5472.CAN-05-2776
PMID:16397273
Abstract

We have previously shown that natural cytotoxic activity of peripheral blood lymphocytes was inversely related to cancer development based on a prospective cohort study. The genetic fraction of cytotoxic activity needs to be clarified, identifying individuals immunogenetically susceptible to cancer. A case-control study within the cohort members was designed: 102 cancer cases with peripheral lymphocyte DNA available and three control groups, each of which consisted of 204 subjects with each tertile level of cytotoxic activity. We first compared two control groups with high and low cytotoxic activity in terms of the single nucleotide polymorphisms in the natural killer complex gene region on chromosome 12p, identifying the haplotype alleles that were associated with the activity. Next, cancer risks were assessed for these haplotypes. We found two haplotype blocks, each of which generated two major haplotype alleles: low-activity-related LNK1 (frequency 0.478 and 0.615 in groups with high and low activity, respectively; P < 0.00008) and high-activity-related HNK1 (0.480 and 0.348; P < 0.0001), LNK2 (0.711 and 0.821; P < 0.0002), and HNK2 (0.272 and 0.174; P < 0.0008). These NKG2D haplotype alleles showed a significant difference between cases (0.632 for LNK1 and 0.333 for HNK1) and controls (0.554 for LNK1 and 0.406 for HNK1). The haplotype HNK1/HNK1 revealed a decreased risk of cancer (odds ratio, 0.471; 95% confidence interval, 0.233-0.952) compared with LNK1/LNK1. Individuals who are genetically predisposed to have low or high natural cytotoxic activity can in part be determined by NKG2D haplotyping, which in turn reveals an increased or decreased risk of cancer development.

摘要

我们之前基于一项前瞻性队列研究表明,外周血淋巴细胞的自然细胞毒性活性与癌症发展呈负相关。细胞毒性活性的遗传成分需要阐明,以识别在免疫遗传学上易患癌症的个体。在队列成员中设计了一项病例对照研究:102例可获取外周淋巴细胞DNA的癌症病例以及三个对照组,每个对照组由204名具有不同三分位数细胞毒性活性水平的受试者组成。我们首先比较了细胞毒性活性高和低的两个对照组在12号染色体p臂自然杀伤复合体基因区域的单核苷酸多态性,确定与该活性相关的单倍型等位基因。接下来,评估这些单倍型的癌症风险。我们发现两个单倍型模块,每个模块产生两个主要的单倍型等位基因:与低活性相关的LNK1(在高活性组和低活性组中的频率分别为0.478和0.615;P < 0.00008)以及与高活性相关的HNK1(0.480和0.348;P < 0.0001)、LNK2(0.711和0.821;P < 0.0002)和HNK2(0.272和0.174;P < 0.0008)。这些NKG2D单倍型等位基因在病例组(LNK1为0.632,HNK1为0.333)和对照组(LNK1为0.554,HNK1为

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