Precise magnetic resonance imaging-guided sonodynamic therapy for drug-resistant bacterial deep infection

The precise treatment of drug-resistant deep bacterial infections remains a huge challenge in clinic. Herein, a polymer-peptide-porphyrin conjugate (PPPC), which can be real-time monitored in infectious site, is developed for accurate and deep sonodynamic therapy (SDT) based on “in vivo self-assembl...

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Published inBiomaterials Vol. 264; p. 120386
Main Authors Wang, Dong, Cheng, Dong-Bing, Ji, Lei, Niu, Li-Juan, Zhang, Xue-Hao, Cong, Yong, Cao, Rong-Hui, Zhou, Lei, Bai, Feng, Qiao, Zeng-Ying, Wang, Hao
Format Journal Article
LanguageEnglish
Published Netherlands Elsevier Ltd 01.01.2021
Subjects
Bacteria
bacterial infections
biocompatible materials
drug resistance
Drug-resistant bacteria
drugs
Magnetic Resonance Imaging
magnetism
minimum inhibitory concentration
Nanoparticles
Peptide
peptides
Pharmaceutical Preparations
polymers
Porphyrin
porphyrins
Self-assembly
Sonodynamic
therapeutics
Ultrasonic Therapy
ultrasonic treatment
Self-assembly
Drug-resistant bacteria
Porphyrin
Peptide
Sonodynamic
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Summary:The precise treatment of drug-resistant deep bacterial infections remains a huge challenge in clinic. Herein, a polymer-peptide-porphyrin conjugate (PPPC), which can be real-time monitored in infectious site, is developed for accurate and deep sonodynamic therapy (SDT) based on “in vivo self-assembly” strategy. The PPPC contains four moieties, i.e., a hyperbranched polymer backbone, a self-assembled peptide linked with an enzyme-cleavable peptide-poly (ethylene glycol) terminal, a bacterial targeting peptide, and a porphyrin sonosensitizer (MnTCPP) segment. Once PPPC nanoparticles reach the infectious area, the protecting PEG layers are removed due to the over-expressed gelatinase, leading to the secondary assembly into large nanoaggregates and resultant enhanced accumulation of sonosensitizer. The nanoaggregates exhibit enhanced interaction with bacterial membrane and decrease the minimum inhibitory concentration (MIC) significantly. Meanwhile, compared with free MnTCPP, the concentration of which can not be accurately quantified, the accumulation amount of MnTCPP in PPPCs at infectious site can be in situ monitored by magnetic resonance imaging (MRI) using T1 combined with T2. When the concentration of PPPC-1 reaches MIC, the drug-resistant bacterial infection area is exposed to ultrasound irradiation, causing the precise and efficient elimination of bacteria. Therefore, the MRI-guided SDT system shows extraordinary tissue penetration depth, drug concentration monitoring, morphology-transformation induced accumulation and improved treatment capacity toward drug-resistant bacteria.
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ISSN:0142-9612
1878-5905
1878-5905
DOI:10.1016/j.biomaterials.2020.120386