Holliday R
Br J Cancer. 1979 Oct;40(4):513-22. doi: 10.1038/bjc.1979.216.
Although many carcinogens are mutagens, there is no direct evidence that the cancer-cell phenotype is the result of gene mutation. Transplantation experiments have strongly indicated that malignant cells can arise or revert to the normal phenotype in the absence of mutation. It is suggested that damage to DNA followed by repair triggers the epigenetic changes in gene expression which are responsible for malignancy. We previously proposed that methylation of specific DNA sequences adjacent to structural genes determines whether or not transcription will occur. Specific methylases are required for the switching on of genes and for the stable maintenance of the methylated state, which provides a basis for the control of gene expression in differentiated cells. It is now seen that damage to DNA followed by repair, just before or just after DNA replication, can lead to the loss of methyl groups. This can induce a switch in gene activity which is heritable, but potentially reversible. The known large difference in the probability of malignant transformation in cells of rodents and large mammals is hard to explain if mutation is responsible. On the other hand, this new theory provides an explanation for this difference, since the probability of epigenetic changes in gene activity will depend on the activity of methylating enzymes and the rate of excision repair. The theory is supported by the evidence that excision repair is more efficient in cultured fibroblasts from large long-lived animals than from small short-lived ones.
虽然许多致癌物是诱变剂,但没有直接证据表明癌细胞表型是基因突变的结果。移植实验有力地表明,恶性细胞可以在没有突变的情况下产生或恢复到正常表型。有人提出,DNA损伤后修复会触发基因表达的表观遗传变化,而这正是导致恶性肿瘤的原因。我们之前提出,与结构基因相邻的特定DNA序列的甲基化决定了转录是否会发生。开启基因和稳定维持甲基化状态都需要特定的甲基化酶,这为分化细胞中基因表达的控制提供了基础。现在可以看到,在DNA复制之前或之后,DNA损伤后修复会导致甲基基团的丢失。这可以诱导基因活性的转变,这种转变是可遗传的,但可能是可逆的。如果突变是导致恶性转化的原因,那么很难解释啮齿动物和大型哺乳动物细胞中恶性转化概率的已知巨大差异。另一方面,这个新理论为这种差异提供了解释,因为基因活性表观遗传变化的概率将取决于甲基化酶的活性和切除修复的速率。该理论得到了以下证据的支持:大型长寿动物培养的成纤维细胞中的切除修复比小型短寿动物的更有效。