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自然杀伤细胞在未能表达人类白细胞抗原-A2等位基因的突变淋巴细胞阴性选择中的可能作用。

Possible role of natural killer cells in negative selection of mutant lymphocytes that fail to express the human leukocyte antigen-A2 allele.

作者信息

Kusunoki Y, Kyoizumi S, Kubo Y, Hayashi T, MacPhee D G

机构信息

Department of Radiobiology, Radiation Effects Research Foundation, 5-2 Hijiyama Park, Minami Ward, Hiroshima 732-0815, Japan.

出版信息

Mutat Res. 2001 May 9;476(1-2):123-32. doi: 10.1016/s0027-5107(01)00106-3.

Abstract

Increased frequencies of cells carrying mutations at several loci have been found in the blood cells of atomic-bomb (A-bomb) survivors upon testing four or five decades after the bombing. Interestingly, though, we have been unable to demonstrate any radiation-associated increases in the frequencies of mutant blood cells in which human leukocyte antigen (HLA)-A expression has been disrupted; this is true both of preliminary tests on the T cells of a small subset of A-bomb survivors and of the much more extensive study reported here in which we screened a much larger group of survivors for HLA-A2 loss mutations in B cells and granulocytes as well as in T cells. In attempting to explain our inability to detect any increases in HLA-A2-negative cell numbers in HLA-A2 heterozygous individuals exposed to A-bomb irradiation, we decided to test the hypothesis that HLA-A mutant lymphocytes might well have been induced by radiation exposure in much the same way as every other type of mutant we encountered, but may subsequently have been eliminated by the strong negative selection associated with their almost inevitable exposure to autologous natural killer (NK) cells in the bloodstream of each of the individuals concerned. We now report that mutant B lymphocyte cell lines that have lost the ability to express the HLA-A2 antigen do indeed appear to be much more readily eliminated than their parental heterozygous counterparts during co-culture in vitro with autologous NK cells. We make this claim first because we have observed that adding autologous NK cells to in vitro cultures of HLA-A2 heterozygous B or T cell lines appeared to cause a dose-dependent decrease in the numbers of HLA-A2-negative mutants that could be detected over a period of 3 days, and second because when we used peripheral blood HLA-A2 heterozygous lymphocyte cultures from which most of the autologous NK cells had been removed we found that we were able to detect newly-arising HLA-A2 mutant T cells in substantial numbers. Taken together, these results strongly support the hypothesis that autologous NK cells are responsible for eliminating mutant lymphocytes that have lost the ability to express self-HLA class I molecules in vivo, and may well therefore explain why we have been unable to detect increased frequencies of HLA-A2 mutants in samples from any of the 164 A-bomb survivors whose HLA-A2 heterozygote status made their lymphocytes suitable for our tests.

摘要

在原子弹爆炸后的四五十年进行检测时,发现原子弹(A 弹)幸存者血细胞中携带多个位点突变的细胞频率有所增加。然而,有趣的是,我们无法证明人类白细胞抗原(HLA)-A 表达被破坏的突变血细胞频率因辐射而增加;无论是对一小部分 A 弹幸存者的 T 细胞进行的初步检测,还是在此报告的更为广泛的研究(在该研究中,我们在 B 细胞、粒细胞以及 T 细胞中筛选了更多的幸存者以寻找 HLA-A2 缺失突变),都是如此。在试图解释我们无法在暴露于原子弹辐射的 HLA-A2 杂合个体中检测到 HLA-A2 阴性细胞数量增加的原因时,我们决定检验这样一个假设:HLA-A 突变淋巴细胞很可能像我们遇到的其他类型的突变一样,是由辐射暴露诱导产生的,但随后可能因与它们几乎不可避免地暴露于相关个体血液中的自体自然杀伤(NK)细胞有关的强烈负选择而被清除。我们现在报告,在与自体 NK 细胞进行体外共培养时,确实失去表达 HLA-A2 抗原能力的突变 B 淋巴细胞系似乎比其亲本杂合对应物更容易被清除。我们提出这一主张,首先是因为我们观察到,向 HLA-A2 杂合 B 或 T 细胞系的体外培养物中添加自体 NK 细胞,似乎会导致在 3 天时间内可检测到的 HLA-A2 阴性突变体数量呈剂量依赖性减少;其次是因为当我们使用去除了大部分自体 NK 细胞的外周血 HLA-A2 杂合淋巴细胞培养物时,我们发现能够大量检测到新出现的 HLA-A2 突变 T 细胞。综合这些结果,有力地支持了这样一个假设:自体 NK 细胞负责在体内清除失去表达自身 HLA I 类分子能力的突变淋巴细胞,因此很可能解释了为什么我们在 164 名 HLA-A2 杂合状态使其淋巴细胞适合我们检测的 A 弹幸存者的样本中,未能检测到 HLA-A2 突变频率增加。

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