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一种胰高血糖素样肽-1类似物形成的非共价聚集体的生物物理特征:生物制药聚集体的一个典型例子。

Biophysical signatures of noncovalent aggregates formed by a glucagonlike peptide-1 analog: a prototypical example of biopharmaceutical aggregation.

作者信息

Doyle Brandon L, Pollo Mark J, Pekar Allen H, Roy Michael L, Thomas Beth Ann, Brader Mark L

机构信息

Biopharmaceutical Research and Development, Lilly Research Laboratories, Eli Lilly and Company, Indianapolis, IN 46285, USA.

出版信息

J Pharm Sci. 2005 Dec;94(12):2749-63. doi: 10.1002/jps.20420.

DOI:10.1002/jps.20420
PMID:16258989
Abstract

LY307161 is a 31 amino acid analog of glucagonlike peptide-1(7-37)OH susceptible to physical instability associated with pharmaceutical processing. Orthogonal biophysical studies were conducted to explore the origins of this physical instability and to distinguish pharmaceutically desirable states of this aggregating peptide from undesirable ones. Equilibrium sedimentation analysis established that LY307161 exists as a monomer at pH 3, and reversibly self-associates in the pH range 7.5-10.5. Causative factors for physical instability related to lyophilization conditions were investigated. Solution pH, acetonitrile content, and concentration of the peptide prior to lyophilization each impacted physicochemical properties of the resultant powders. A comparative study of two powder samples exhibiting physicochemically disparate properties established that LY307161 forms soluble noncovalent aggregates. FT-IR analyses in the solid and solution states identified a prominent band at 1657-1659 cm(-1) attributed to alpha-helix structure. Noncovalent soluble aggregate exhibited characteristic bands at 1615 and 1698 cm(-1) indicative of intermolecular beta-sheet structure. An agitation-induced, precipitated solid form of LY307161 exhibited a different FT-IR signature indicative of a conformationally distinct species. Circular dichroism and fluorescence spectroscopy, together with dynamic light scattering measurements and dye-aggregate complexation, provided additional insights into the distinctions between aggregated and native LY307161.

摘要

LY307161是胰高血糖素样肽-1(7-37)OH的31个氨基酸类似物,易受与药物加工相关的物理不稳定性影响。进行了正交生物物理研究,以探究这种物理不稳定性的根源,并区分这种聚集肽在药学上理想的状态和不理想的状态。平衡沉降分析表明,LY307161在pH 3时以单体形式存在,并在pH 7.5-10.5范围内可逆地自缔合。研究了与冻干条件相关的物理不稳定性的成因。溶液pH值、乙腈含量以及冻干前肽的浓度均会影响所得粉末的物理化学性质。对两个物理化学性质不同的粉末样品进行的对比研究表明,LY307161形成了可溶性非共价聚集体。固态和溶液态的傅里叶变换红外光谱分析在1657-1659 cm(-1)处发现了一条归属于α-螺旋结构的突出谱带。非共价可溶性聚集体在1615和1698 cm(-1)处表现出特征谱带,表明存在分子间β-折叠结构。搅拌诱导的LY307161沉淀固体形式表现出不同的傅里叶变换红外光谱特征,表明其构象不同。圆二色光谱和荧光光谱,以及动态光散射测量和染料-聚集体络合,为聚集态和天然态LY307161之间的差异提供了更多见解。

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