Specific Clearance of Lipopolysaccharide from Blood Based on Peptide Bottlebrush Polymer for Sepsis Therapy

Author:

Shi Zhenqiang1ORCID,Zhang Xiancheng1,Yang Xijing2,Zhang Xiaoyu1,Ma Fei3,Gan Hui3,Chen Junjun1,Wang Dongdong1,Sun Wenjing1,Wang Jingxia4,Wang Cunli1,Lyu Liting5,Yang Kaiguang1,Deng Lijing6,Qing Guangyan1ORCID

Affiliation:

1. CAS Key Laboratory of Separation Science for Analytical Chemistry Dalian Institute of Chemical Physics Chinese Academy of Sciences Dalian 116023 P.R. China

2. Animal Experiment Center West China Hospital Sichuan University Chengdu 610041 P.R. China

3. Department of Pharmaceutical Sciences Beijing Institute of Radiation Medicine Beijing 100850 P.R. China

4. Radiation Chemistry Department Sichuan Institute of Atomic Energy Chengdu 610101 P.R. China

5. Dalian Key Laboratory of Energy Biotechnology Dalian Institute of Chemical Physics Chinese Academy of Sciences Dalian 116023 P.R. China

6. Pediatric Intensive Care Unit Department of Critical Care Medicine West China Hospital Sichuan University Chengdu 610041 P.R. China

Abstract

AbstractLipopolysaccharide (LPS) is the primary bacterial toxin that is vital to the pathogenesis and progression of sepsis associated with extremely high morbidity and mortality worldwide. However, specific clearance of LPS from circulating blood is highly challenging because of the structural complexity and its variation between/within bacterial species. Herein, a robust strategy based on phage display screening and hemocompatible peptide bottlebrush polymer design for specific clearance of targeted LPS from circulating blood is proposed. Using LPS extracted from Escherichia coli as an example, a novel peptide (HWKAVNWLKPWT) with high affinity (KD < 1.0 nм), specificity, and neutralization activity (95.9 ± 0.1%) against the targeted LPS is discovered via iterative affinity selection coupled with endotoxin detoxification screening. A hemocompatible bottlebrush polymer bearing the short peptide [poly(PEGMEA‐co‐PEP‐1)] exhibits high LPS selectivity to reduce circulating LPS level from 2.63 ± 0.01 to 0.78 ± 0.05 EU mL−1 in sepsis rabbits via extracorporeal hemoperfusion (LPS clearance ratio > 70%), reversing the LPS‐induced leukocytopenia and multiple organ damages significantly. This work provides a universal paradigm for developing a highly selective hemoadsorbent library fully covering the LPS family, which is promising to create a new era of precision medicine in sepsis therapy.

Funder

National Natural Science Foundation of China

National Key Research and Development Program of China

Publisher

Wiley

Subject

Mechanical Engineering,Mechanics of Materials,General Materials Science

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