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Determination of hammerhead ribozyme kinetic constants at high molar ratio ribozyme-substrate

机译:高摩尔比核酶-底物下锤头状核酶动力学常数的测定

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摘要

Hammerhead ribozymes provide valuable tools in the field of gene therapy due to their cleavage specificity and the broad range of RNA targets. A major prerequisite for the selection of suitable ribozymes for in vivo application is represented by in vitro determination of ribozyme cleavage kinetic constants. From the experimental cleavage data, kinetic constants are usually calculated under the assumption of rapid conversion of the substrate into the ribozyme-substrate complex. However. this condition is often not satisfied for ribozymes carrying additional RNA stretches, due to cloning strategies or necessary for ribozyme expression in the cell. To overcome this problem. we propose a mathematical model which is able to calculate ribozyme kinetic constants in the case of non-rapid conversion of substrate into ribozyme-substrate complex. In addition, our system gives the opportunity to evaluate the nature of the S conversion into ES through the determination of a model parameter. The validity of the proposed model is restricted to the hypothesis of a ribozyme excess over the substrate at the beginning of the cleavage reaction and to the absence of any mass exchange with the external environment. [References: 22]
机译:锤头型核酶因其裂解特异性和广泛的RNA靶点而在基因治疗领域提供了有价值的工具。选择适合体内应用的核酶的主要前提条件是在体外测定核酶裂解动力学常数。根据实验裂解数据,通常在底物迅速转化为核酶-底物复合物的假设下计算动力学常数。然而。由于克隆策略或细胞中核酶表达的必要条件,这种条件对于携带额外RNA片段的核酶通常无法满足。为了克服这个问题。我们提出了一个数学模型,该模型能够在底物不快速转化为核酶-底物复合物的情况下计算核酶的动力学常数。此外,我们的系统还提供了通过确定模型参数来评估S转换为ES的性质的机会。提出的模型的有效性仅限于在裂解反应开始时核酶比底物过量的假设,以及与外界环境之间没有任何质量交换的假设。 [参考:22]

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