Acceptor‐Reactivity‐Controlled Stereoconvergent Synthesis and Immunological Activity of a Unique Pentasaccharide from the Cell Wall Polysaccharide of Cutibacterium acnes C7

Author:

Hao Tianhui12,Feng Ke3,Jin Hongzhen4,Li Jiawei1,Zhou Chenkai1,Liu Xingbang1,Zhao Wei3,Yu Fan4,Li Tiehai12ORCID

Affiliation:

1. State Key Laboratory of Chemical Biology Carbohydrate-Based Drug Research Center Institute of Materia Medica Chinese Academy of Sciences Shanghai 201203 China

2. University of Chinese Academy of Sciences Beijing 100049 China

3. State Key Laboratory of Medicinal Chemical Biology College of Pharmacy Nankai University Tianjin 300350 China

4. School of Health and Life Sciences Qingdao Central Hospital University of Health and Rehabilitation Sciences Qingdao 266113 China

Abstract

AbstractBacterial cell‐surface polysaccharides are involved in various biological processes and have attracted widespread attention as potential targets for developing carbohydrate‐based drugs. However, the accessibility to structurally well‐defined polysaccharide or related active oligosaccharide domains remains challenging. Herein, we describe an efficiently stereocontrolled approach for the first total synthesis of a unique pentasaccharide repeating unit containing four difficult‐to‐construct 1,2‐cis‐glycosidic linkages from the cell wall polysaccharide of Cutibacterium acnes C7. The features of our approach include: 1) acceptor‐reactivity‐controlled glycosylation to stereoselectively construct two challenging rare 1,2‐cis‐ManA2,3(NAc)2 (β‐2,3‐diacetamido‐2,3‐dideoxymannuronic acid) linkages, 2) combination use of 6‐Otert‐butyldiphenylsilyl (6‐O‐TBDPS)‐mediated steric shielding effect and ether solvent effect to stereoselectively install a 1,2‐cis‐glucosidic linkage, 3) bulky 4,6‐di‐Otert‐butylsilylene (DTBS)‐directed glycosylation to stereospecifically construct a 1,2‐cis‐galactosidic linkage, 4) stereoconvergent [2+2+1] and one‐pot chemoselective glycosylation to rapidly assemble the target pentasaccharide. Immunological activity tests suggest that the pentasaccharide can induce the production of proinflammatory cytokine TNF‐α in a dose‐dependent manner.

Funder

National Natural Science Foundation of China

Fundamental Research Funds for the Central Universities

Publisher

Wiley

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