Ligand‐Enabled Pd‐Catalyzed sp3 C‒H Macrocyclization: Synthesis and Evaluation of Macrocyclic Sulfonamide for the Treatment of Parkinson’s Disease

Author:

Bi Tongyu1,Cui Yunxia2,Liu Shuai3,Yu Haiyue1,Qiu Weirong1,Hou Ke-Qiang1,Zou Jiaqi4,Yu Zhipeng4,Zhang Feili1,Xu Zhongliang1,Zhang Jian5,Xu Xiaojun6,Yang Weibo7

Affiliation:

1. Shanghai Institute of Materia Medica Chinese Academy of Sciences Medicinal chemistry CHINA

2. Shanghai Jiaotong University School of Medicine CHINA

3. Zhejiang University Medicinal chemistry CHINA

4. Nanjing University of Chinese Medicine Medicinal chemistry CHINA

5. Shanghai Jiaotong University Pharmacology CHINA

6. Zhejiang University Pharmacology CHINA

7. Shanghai Institute of Materia Medica (SIMM), Chinese Academy of Sciences State Key Laboratory of Drug Research 555 Zuchongzhi Road, Shanghai 201203, China 201203 Shanghai CHINA

Abstract

The development of simplified synthetic strategy to create structurally and functionally diverse pseudo‐natural macrocyclic molecules is highly appealing but poses a marked challenge. Inspired by natural scaffolds, herein, we describe a practical and concise ligand‐enabled Pd(II)‐catalysed sp3 C‒H alkylation, olefination and arylation macrocyclization, which could offer a novel set of pseudo‐natural macrocyclic sulfonamides. Interestingly, the potential of ligand acceleration in C‒H activation is also demonstrated by an unprecedented enantioselective sp3 C‒H alkylation macrocyclization. Moreover, a combination of in silico screening and biological evaluation led to the identification of a novel spiro‐grafted macrocyclic sulfonamide 2a, which showed a promising efficacy for the treatment of Parkinson’s disease (PD) in a mouse model through the activation of silent information regulator sirtuin 3 (SIRT3).

Publisher

Wiley

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