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A mathematical model and a computerized simulation of PCR using complex templates.

机译:使用复杂模板的PCR的数学模型和计算机仿真。

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摘要

A mathematical model and a computer simulation were used to study PCR specificity. The model describes the occurrences of non-targeted PCR products formed through random primer-template interactions. The PCR simulation scans DNA sequence databases with primers pairs. According to the model prediction, PCR with complex templates should rarely yield non-targeted products under typical reaction conditions. This is surprising as such products are often amplified in real PCR under conditions optimized for stringency. The causes for this 'PCR paradox' were investigated by comparing the model predictions with simulation results. We found that deviations from randomness in sequences from real genomes could not explain the frequent occurrence of non-targeted products in real PCR. The most likely explanation to the 'PCR paradox' is a relatively high tolerance of PCR to mismatches. The model also predicts that mismatch tolerance has the strongest effect on the number of non-targeted products, followed by primer length, template size and product size limit. The model and the simulation can be utilized for PCR studies, primer design and probing DNA uniqueness and randomness.
机译:使用数学模型和计算机模拟来研究PCR特异性。该模型描述了通过随机引物-模板相互作用形成的非靶向PCR产物的出现。 PCR模拟使用引物对扫描DNA序列数据库。根据模型预测,具有复杂模板的PCR在典型的反应条件下很少会产生非目标产物。令人惊讶的是,此类产物通常在针对严格性优化的条件下于真实PCR中扩增。通过将模型预测与仿真结果进行比较,研究了这种“ PCR悖论”的原因。我们发现与真实基因组序列的随机性差异不能解释真实PCR中非目标产物的频繁发生。 “ PCR悖论”最可能的解释是PCR对错配的较高耐受性。该模型还预测,错配耐受性对非目标产品的数量影响最大,其次是引物长度,模板大小和产品大小限制。该模型和仿真可用于PCR研究,引物设计以及探测DNA的唯一性和随机性。

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