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一种生产利拉鲁肽前体肽的新策略和一种新型长效肠促胰岛素类似物的开发。

A novel strategy for production of liraglutide precursor peptide and development of a new long-acting incretin mimic.

机构信息

Department of Biology, Protein Chemistry Laboratory (PCL), College of Sciences, Shiraz University, Shiraz, Iran.

Department of Biosciences and Bioengineering, IIT Bombay, Powai, Mumbai, India.

出版信息

PLoS One. 2022 May 2;17(5):e0266833. doi: 10.1371/journal.pone.0266833. eCollection 2022.

Abstract

Nowadays, a small number of incretin mimics are used to treat type 2 diabetes mellitus (T2DM) due to their longer half-life. The present study aimed to introduce a novel method for producing the liraglutide precursor peptide (LPP) and developing a potentially new incretin mimic. Here, human αB-crystallin (αB-Cry) was ligated to the LPP at the gene level, and the gene construct was expressed in Escherichia coli with a relatively good efficiency. The hybrid protein (αB-lir) was then purified by a precipitation method followed by anion exchange chromatography. After that, the peptide was released from the carrier protein by a chemical cleavage method yielding about 70%. The LPP was then purified by gel filtration chromatography, and HPLC estimated its purity to be about 98%. Also, the molecular mass of the purified peptide was finally confirmed by mass spectroscopy analysis. Assessment of the secondary structures suggested a dominant α-helical structure for the LPP and a β-sheet rich structure for the hybrid protein. The subcutaneous injection of the LPP and the αB-lir hybrid protein significantly reduced the blood sugar levels in healthy and diabetic mice and stimulated insulin secretion. Also, the hybrid protein exerts its bioactivities more effectively than the LPP over a relatively longer period of time. The results of this study suggested a novel method for the easy and cost-effective production of the LPP and introduced a new long-acting incretin mimic that can be potentially used for the treatment of T2DM patients.

摘要

如今,由于半衰期较长,有少量的肠促胰岛素类似物被用于治疗 2 型糖尿病(T2DM)。本研究旨在介绍一种生产利拉鲁肽前体肽(LPP)的新方法,并开发一种潜在的新型肠促胰岛素类似物。本研究将人αB-晶体蛋白(αB-Cry)与 LPP 在基因水平上连接,并在大肠杆菌中以相对较高的效率表达该基因构建体。然后通过沉淀法和阴离子交换层析对杂合蛋白(αB-lir)进行纯化。之后,通过化学切割法将肽从载体蛋白上释放出来,产率约为 70%。然后通过凝胶过滤层析对 LPP 进行纯化,HPLC 估计其纯度约为 98%。最后,通过质谱分析确认了纯化肽的分子量。对二级结构的评估表明,LPP 具有主要的α-螺旋结构,而杂合蛋白则具有富含β-折叠的结构。LPP 和αB-lir 杂合蛋白的皮下注射可显著降低健康和糖尿病小鼠的血糖水平,并刺激胰岛素分泌。此外,与 LPP 相比,该杂合蛋白在相对较长的时间内更有效地发挥其生物活性。本研究结果提出了一种生产 LPP 的简便、经济有效的新方法,并介绍了一种新的长效肠促胰岛素类似物,可潜在用于治疗 T2DM 患者。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d6f6/9060347/b898035f5e3d/pone.0266833.g001.jpg

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