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辅料诱导的抗菌药物在注射剂中可逆性结合治疗性肽。

Antimicrobial Excipient-Induced Reversible Association of Therapeutic Peptides in Parenteral Formulations.

机构信息

Pharmaceutical Sciences, Merck & Co., Inc, Kenilworth, NJ 07033, USA.

Pharmaceutical Sciences, Merck & Co., Inc, Kenilworth, NJ 07033, USA.

出版信息

J Pharm Sci. 2021 Feb;110(2):850-859. doi: 10.1016/j.xphs.2020.09.027. Epub 2020 Sep 24.

DOI:10.1016/j.xphs.2020.09.027
PMID:32980392
Abstract

New classes of therapeutic peptides are being developed to prosecute biological targets which have been inaccessible to other modalities. Higher potency and longer half-life peptides have given rise to multiuse injectable formulations that enable convenient, low volume, and self-administered dosing; however, inclusion of antimicrobial preservatives to meet bactericidal requirements can impact other attributes of peptide formulations. Peptide-preservative interactions influencing solution-phase self-association of a non-insulin, linear, palmitoylated 31 amino acid peptide and two structurally similar peptides were assessed via turbidity, intrinsic fluorescence shifts and quenching, isothermal titration calorimetry, and H NMR. Meta-cresol and phenol specifically interact with the peptide, result in increased hydrophobicity near the tryptophan residue, and induce conformational changes, while benzyl alcohol does not impact tryptophan fluorescence, demonstrate any interaction enthalpy, or induce conformational changes. These same trends did not hold true for the other palmitoylated peptides evaluated, reinforcing the impacts of unique peptide sequences. Importantly, the presence of benzyl alcohol does increase the physical stability and solubility of the linear, 31 amino acid peptide under salt stress. We report new insights into the physical interactions of peptides with antimicrobial excipients, demonstrating a reversible association phenomenon and highlighting practical implications for formulation design and excipient selection.

摘要

新型治疗性肽类药物正在被开发,以针对其他方法无法触及的生物靶点。更高的效力和更长的半衰期肽类药物已经产生了多用途的可注射制剂,使方便、低容量和自我给药成为可能;然而,为了满足杀菌要求而加入抗菌防腐剂会影响肽制剂的其他属性。通过浊度、本征荧光位移和猝灭、等温滴定量热法和 H NMR 评估了影响非胰岛素、线性、棕榈酰化 31 个氨基酸肽和两种结构相似肽的溶液相自组装的肽-防腐剂相互作用。间甲酚和苯酚特异性地与肽相互作用,导致色氨酸残基附近的疏水性增加,并诱导构象变化,而苯甲醇不影响色氨酸荧光,不显示任何相互作用焓,也不诱导构象变化。对于评估的其他棕榈酰化肽,这些相同的趋势并不成立,这强化了独特肽序列的影响。重要的是,苯甲醇的存在确实增加了线性、31 个氨基酸肽在盐应力下的物理稳定性和溶解度。我们报告了肽与抗菌赋形剂的物理相互作用的新见解,证明了一种可逆的缔合现象,并突出了配方设计和赋形剂选择的实际意义。

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Antimicrobial Excipient-Induced Reversible Association of Therapeutic Peptides in Parenteral Formulations.辅料诱导的抗菌药物在注射剂中可逆性结合治疗性肽。
J Pharm Sci. 2021 Feb;110(2):850-859. doi: 10.1016/j.xphs.2020.09.027. Epub 2020 Sep 24.
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