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System that generates pharmacokinetic analyses of oligonucleotide total effects from full-scan mass spectra

机译:从全扫描质谱产生寡核苷酸总效应的药代动力学分析的系统

摘要

System that automates analysis of mass spectrometry data for oligonucleotides to generate pharmacokinetic parameters and models. A user inputs an oligonucleotide sequence and a maximum number of nucleotides that may be lost during metabolism while retaining therapeutic effectiveness. The system calculates the possible active metabolites and develops a mass spectrum filter for the mass-to-charge ratio of ions for these metabolites. Full-scan spectra are analyzed to calculate the total concentration of these active molecules present in a time series of samples. Pharmacokinetic models and parameters are calculated from the time series of total concentration. Because full-scan spectra are captured, assumptions may be modified and analyses may be quickly rerun without collecting additional data. Overall pharmacokinetic analysis is therefore much more streamlined and efficient, reducing cost, delay, and the need for a mass spectrometrist who is highly skilled in spectral analysis.
机译:系统自动分析寡核苷酸质谱数据以产生药代动力学参数和模型。用户输入寡核苷酸序列和最大数量的核苷酸,其在代谢期间可能丢失,同时保持治疗效果。该系统计算可能的活性代谢物,并为这些代谢物的离子的质量谱滤波器开发质谱滤波器。分析全扫描光谱以计算在一系列样品中存在的这些活性分子的总浓度。从总浓度的时间序列计算药代动力学模型和参数。因为捕获全扫描光谱,所以可以修改假设,并且可以在不收集附加数据的情况下快速重新运行分析。因此,整体药代动力学分析更精简和有效,降低成本,延迟以及对光谱分析技术人员高技能的质谱仪的需要。

著录项

  • 公开/公告号US10937525B2

    专利类型

  • 公开/公告日2021-03-02

    原文格式PDF

  • 申请/专利权人 BIOTUNE COMPUTATIONS LLC;

    申请/专利号US202016911038

  • 发明设计人 RENEE WILLIAMS;

    申请日2020-06-24

  • 分类号G16B40/10;G16B30;C12Q1/6872;

  • 国家 US

  • 入库时间 2022-08-24 17:26:03

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