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兰瑞肽差向异构体的树脂上合成及其构效关系研究。

On-resin synthesis of Lanreotide epimers and studies of their structure-activity relationships.

作者信息

Chowdhury Arnab, Tripathi Nitesh Mani, Jadav Rohit, Gour Vinod, Purohit Parva, Bandyopadhyay Anupam

机构信息

Biomimetic Peptide Engineering Laboratory, Department of Chemistry, Indian Institute of Technology Ropar Rupnagar Punjab-140001 India

Kashiv BioSciences Pvt Ltd. Block-B, Sardar Patel Ring Rd, opp. Applewoods Township Ahmedabad Gujarat-382210 India.

出版信息

RSC Med Chem. 2024 Jul 1;15(8):2766-2772. doi: 10.1039/d4md00338a. eCollection 2024 Aug 14.

Abstract

Peptide drugs often accompany epimeric impurities (isomers). Therefore, efficient chemical synthesis of epimers is critical to identify them correctly and investigate their biological activities. Here, we report the rapid synthesis and structure-activity relationship (SAR) studies of eight possible epimers of a somatostatin synthetic analog (SSA), lanreotide (LAN). SPPS and the subsequent on-resin rapid disulfide closure method offered >90% conversion yield for all epimers (P1-P8). Further, we developed an analytical method to separate these epimers, which enabled the profiling of five epimeric impurities in the API, purchased for Somatuline generic formulations. In SAR studies, most LAN epimers revealed compromised antiproliferative activity, while the P7 epimer retained antiproliferative activity similar to LAN API, as supported by SAR studies in detail. Additionally, P7 showed serum stability nearly identical to LAN, suggesting that drug epimers could be a potential API. Current studies will further encourage the development of novel SSA scaffolds.

摘要

肽类药物常常伴有差向异构杂质(异构体)。因此,高效化学合成差向异构体对于正确鉴定它们并研究其生物活性至关重要。在此,我们报告了生长抑素合成类似物(SSA)兰瑞肽(LAN)的八种可能差向异构体的快速合成及构效关系(SAR)研究。固相肽合成(SPPS)及随后的树脂上快速二硫键环化方法使所有差向异构体(P1 - P8)的转化产率>90%。此外,我们开发了一种分离这些差向异构体的分析方法,该方法能够对购买用于善龙仿制药制剂的原料药中五种差向异构杂质进行分析。在构效关系研究中,大多数LAN差向异构体显示出抗增殖活性受损,而P7差向异构体保留了与LAN原料药相似的抗增殖活性,详细的构效关系研究证实了这一点。此外,P7显示出与LAN几乎相同的血清稳定性,表明药物差向异构体可能是一种潜在的原料药。当前的研究将进一步推动新型SSA支架的开发。

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