在动物研究中对人源单克隆抗体蛋白候选药物进行生物分析的双通用肽方法。
Dual universal peptide approach to bioanalysis of human monoclonal antibody protein drug candidates in animal studies.
作者信息
Furlong Michael T, Zhao Song, Mylott William, Jenkins Rand, Gao Mian, Hegde Vendana, Tamura James, Tymiak Adrienne, Jemal Mohammed
机构信息
Bristol-Myers Squibb, Analytical & Bioanalytical Development, Princeton, NJ 08543, USA.
出版信息
Bioanalysis. 2013 Jun;5(11):1363-76. doi: 10.4155/bio.13.55.
BACKGROUND
There is a need for general and reliable LC-MS assays capable of supporting the bioanalysis of a variety of human monoclonal antibody-based therapeutic drug candidates in animal PK/TK studies.
RESULTS
We present herein improvements in our previously reported universal peptide approach to the bioanalysis of human monoclonal antibody protein drug candidates in animal studies. These improvements include incorporation of a second, light chain-based universal peptide into the assay, thus introducing the concept of a dual universal peptide assay; and incorporation of a universal stable isotope-labeled monoclonal antibody into the assay.
CONCLUSION
Improvements reported herein to the universal peptide assay will enable more reliable quantification of human monoclonal antibody protein drug candidates in animal studies.
背景
在动物药代动力学/药效动力学(PK/TK)研究中,需要通用且可靠的液相色谱-质谱(LC-MS)分析方法来支持对多种基于人源单克隆抗体的治疗性药物候选物进行生物分析。
结果
本文展示了我们先前报道的用于动物研究中对人源单克隆抗体蛋白药物候选物进行生物分析的通用肽方法的改进。这些改进包括在分析方法中纳入第二条基于轻链的通用肽,从而引入了双通用肽分析的概念;以及在分析方法中纳入通用稳定同位素标记的单克隆抗体。
结论
本文报道的对通用肽分析方法的改进将能够在动物研究中更可靠地定量人源单克隆抗体蛋白药物候选物。
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