Reactivity of N terminal histidine of peptides towards excipients/impurity of excipients: A case study of liraglutide excipient compatibility study

IF 3.7 3区 医学 Q2 CHEMISTRY, MEDICINAL Journal of pharmaceutical sciences Pub Date : 2024-11-01 DOI:10.1016/j.xphs.2024.08.007
Azahar R. Sheikh , Jyotsna G. Vitore , Vijay S. Bhalekar , Sonali Jain , Divya Kukreja , Tushar Giri , Nitish Sharma , Derajram Benival , Ravi P. Shah
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Abstract

The selection of quality excipients is a crucial step in peptide formulation development. Apart from excipient incompatibility, process-related impurities or degradants of an excipient can interact with peptide-active pharmaceutical ingredients, forming the interaction products. The formaldehyde has been reported as an impurity of excipient in polyethylene glycol, glycerol, magnesium stearate, microcrystalline cellulose, mannitol, etc. The peptide contains various amino acids such as histidine, lysine, and arginine having free amine groups. These amine groups act as strong nucleophile and can increase the reactivity of peptides. PLGA is the most widely used biodegradable polymer in sustained-release formulations. The hydrolysis of PLGA generates glycolic acid and lactic acid impurities, which can form the interaction product with the amines of peptides. During the formulation development of Liraglutide, we have found few interaction products. The systematic characterization and mechanistic understanding of these interaction products lead us to imidazopyrimidine, glycolyl, and lactolyl moieties. These interaction products have been characterized thoroughly with the use of LC-HRMS, MS/MS, and hydrogen-deuterium exchange mass studies. The study revealed that the reactivity of N-terminal histidine must be considered for formulation development. Moreover, the quality of excipients with respect to presence of impurities must be considered as critical material attributes.
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肽的 N 端组氨酸与辅料/辅料杂质的反应性:利拉鲁肽辅料兼容性案例研究。
选择优质辅料是多肽制剂研发的关键步骤。除了辅料不相容外,辅料中与工艺相关的杂质或降解物也会与多肽活性药物成分发生作用,形成相互作用产物。据报道,甲醛是聚乙二醇、甘油、硬脂酸镁、微晶纤维素、甘露醇等辅料中的杂质。肽含有多种氨基酸,如组氨酸、赖氨酸和精氨酸,这些氨基酸具有游离胺基团。这些胺基可作为强亲核体,提高肽的反应活性。PLGA 是缓释制剂中使用最广泛的生物可降解聚合物。PLGA 在水解过程中会产生乙醇酸和乳酸杂质,这些杂质会与多肽的胺形成相互作用产物。在利拉鲁肽的制剂开发过程中,我们几乎没有发现相互作用产物。通过对这些相互作用产物的系统表征和机理了解,我们发现了咪唑嘧啶、乙二醇和乳醇分子。我们利用 LC-HRMS、MS/MS 和氢氘交换质量研究对这些相互作用产物进行了彻底表征。研究结果表明,配方开发必须考虑 N 端组氨酸的反应性。此外,辅料的质量和杂质含量也是关键的材料属性。
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来源期刊
CiteScore
7.30
自引率
13.20%
发文量
367
审稿时长
33 days
期刊介绍: The Journal of Pharmaceutical Sciences will publish original research papers, original research notes, invited topical reviews (including Minireviews), and editorial commentary and news. The area of focus shall be concepts in basic pharmaceutical science and such topics as chemical processing of pharmaceuticals, including crystallization, lyophilization, chemical stability of drugs, pharmacokinetics, biopharmaceutics, pharmacodynamics, pro-drug developments, metabolic disposition of bioactive agents, dosage form design, protein-peptide chemistry and biotechnology specifically as these relate to pharmaceutical technology, and targeted drug delivery.
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