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On genetic information uncertainty and the mutator phenotype in cancer

机译:癌症的遗传信息不确定性和变异表型

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摘要

Recent evidence supports the existence of a mutator phenotype in cancer cells, although the mechanistic basis remains unknown. In this paper, it is shown that this enhanced genetic instability is generated by an amplified measurement uncertainty on genetic information during DNA replication. At baseline, an inherent measurement uncertainty implies an imprecision of the recognition, replication and transfer genetic information, and forms the basis for an intrinsic genetic instability in all biological cells. Genetic information is contained in the sequence of DNA bases, each existing due to proton tunnelling, as a coherent superposition of quantum states composed of both the canonical and rare tautomeric forms until decoherence by interaction with DNA polymerase. The result of such a quantum measurement process may be interpreted classically as akin to a Bernoulli trial, whose outcome X is random and can be either of two possibilities, depending on whether the proton is tunnelled (X=1) or not (X=0). This inherent quantum uncertainty is represented by a binary entropy function and quantified in terms of Shannon information entropy H(X)=-P(X=1)log _2P(X=1)-P(X=0)log _2P(X=0). Enhanced genetic instability may either be directly derived from amplified uncertainty induced by increases in quantum and thermodynamic fluctuation, or indirectly arise from the loss of natural uncertainty reduction mechanisms.
机译:最近的证据支持癌细胞中存在突变体表型,尽管其机理基础尚不清楚。在本文中,表明这种增强的遗传不稳定性是由DNA复制过程中遗传信息的测量不确定性放大所产生的。在基线时,内在的测量不确定性意味着识别,复制和转移遗传信息的不精确性,并构成了所有生物细胞内在遗传不稳定性的基础。遗传信息包含在DNA碱基的序列中,每个碱基由于质子隧穿而存在,它们是由规范和稀有互变异构形式组成的量子态的相干叠加,直到通过与DNA聚合酶相互作用而脱去相干为止。这种量子测量过程的结果可以经典地解释为类似于伯努利试验,其结果X是随机的,并且可以是两种可能性中的一种,具体取决于质子是否被隧穿(X = 1)(X = 1) )。此固有的量子不确定性由二进制熵函数表示,并根据香农信息熵H(X)=-P(X = 1)log _2P(X = 1)-P(X = 0)log _2P(X = 0)。增强的遗传不稳定性可能直接来自因量子和热力学波动增加而引起的放大不确定性,也可能间接归因于自然不确定性降低机制的丧失。

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