A novel antibacterial material (L-PET) was prepared by immobilizing ε-polylysine on polyethylene terephthalate (PET) nonwoven fabrics. Surface modifications of the fabric were performed by using a chemical modifi...A novel antibacterial material (L-PET) was prepared by immobilizing ε-polylysine on polyethylene terephthalate (PET) nonwoven fabrics. Surface modifications of the fabric were performed by using a chemical modification procedure where carboxyl groups were prepared on the PET surface, a coupling agent was grafted, and the ε-polylysine was immobilized. Scanning electron microscopy (SEM) was used to analyze the surface morphology of the fabrics, while the toluidine blue method and X-ray photoelectron spectroscopy (XPS) were used to evaluate the grafting densities. The antibacterial activities of the L-PET were investigated by using the shaking-flask method. The electron micrographs showed that the surface of the blank PET and the modified fabrics did not change. The results of XPS analysis confirmed that ε-polylysine was successfully grafted onto the surface of PET. The results of the antibacterial experiments showed that L-PET fabrics had excellent antibacterial activity against Escherichia coli and Staphylococcus aureus, and that L-PET fabrics were stable in storage for at least two years.展开更多
Cytidine 5'-monophosphate(5'-CMP)is an essential nucleotide for additives.In this study,enhanced production of 5'-CMP was realized by the transformation of cytidine using co-immobilized di-enzymes,uridine-...Cytidine 5'-monophosphate(5'-CMP)is an essential nucleotide for additives.In this study,enhanced production of 5'-CMP was realized by the transformation of cytidine using co-immobilized di-enzymes,uridine-cytidine kinase(UCK)and acetate kinase(AcK).The immobilization yield of the enzyme had a clear correlation with the surface charges as zeta potential(ξ).Among them,ε-polylysinefunctionalized sepharose(SA-EPL,ξ=9.31 m V)showed high immobilization yield(78.8%),which was4.9-fold than that of nitrilotriacetic acid functionalized sepharose(SA-NTA,ξ=-12.6 m V).The residual activity of affinity co-immobilized enzyme(EPL-Ni/EPL@Ac K-UCK)was higher than 70.6%after recycled 10 times.Thus,this study provides an effective approach for the production of 5'-CMP with the advantages of low adenosine 5'-triphosphate(ATP)consumption,reduced side reactions,and improved reusability by co-immobilized UCK and Ac K on the functionalized Sepharose.展开更多
Multi-drug resistance(MDR)has become the largest obstacle to the success of cancer patients receiving traditional chemotherapeutics or novel targeted drugs.Here,we developed a targeted nanoplatform based on biodegrada...Multi-drug resistance(MDR)has become the largest obstacle to the success of cancer patients receiving traditional chemotherapeutics or novel targeted drugs.Here,we developed a targeted nanoplatform based on biodegradable boronic acid modifiedε-polylysine to co-deliver P-gp siRNA,Bcl-2 siRNA,and doxorubicin for overcoming the challenge.The targeted nanoplatform showed a robust suppressing efficiency for the invasion,proliferation,and colony formation of adriamycin(ADR)resistant breast cancer cell line(MCF-7/ADR)cells in vitro.The ATP responsiveness of the nanoplatform was also proved in the research.In the in vivo antitumor experiment,the targeted nanoplatform showed a significant inhibition of tumor growth with good biocompatibility.The goal of this study is to develop a novel and facile strategy to prepare a highly efficient and safe gene and drug delivery system for MDR breast cancer based on biocompatibleε-polylysine polymers.展开更多
基金Funded by the National Major Science & Technology Specific Projects (2009ZX10004-703)
文摘A novel antibacterial material (L-PET) was prepared by immobilizing ε-polylysine on polyethylene terephthalate (PET) nonwoven fabrics. Surface modifications of the fabric were performed by using a chemical modification procedure where carboxyl groups were prepared on the PET surface, a coupling agent was grafted, and the ε-polylysine was immobilized. Scanning electron microscopy (SEM) was used to analyze the surface morphology of the fabrics, while the toluidine blue method and X-ray photoelectron spectroscopy (XPS) were used to evaluate the grafting densities. The antibacterial activities of the L-PET were investigated by using the shaking-flask method. The electron micrographs showed that the surface of the blank PET and the modified fabrics did not change. The results of XPS analysis confirmed that ε-polylysine was successfully grafted onto the surface of PET. The results of the antibacterial experiments showed that L-PET fabrics had excellent antibacterial activity against Escherichia coli and Staphylococcus aureus, and that L-PET fabrics were stable in storage for at least two years.
基金supported by grants from the National Key Research and Development Program of China(2021YFC2102805,2019YFD1101204)the National Natural Science Foundation of China(21878142,21776132)+3 种基金Key Research and Development Plan of Jiangsu Province(BE2020712)Key Research and Development Plan of Jiangsu Province(BE2019001)Jiangsu Natural Science Fund for Distinguished Young Scholars(BK20190035)the Priority Academic Program Development of Jiangsu Higher Education Institutions(PAPD)。
文摘Cytidine 5'-monophosphate(5'-CMP)is an essential nucleotide for additives.In this study,enhanced production of 5'-CMP was realized by the transformation of cytidine using co-immobilized di-enzymes,uridine-cytidine kinase(UCK)and acetate kinase(AcK).The immobilization yield of the enzyme had a clear correlation with the surface charges as zeta potential(ξ).Among them,ε-polylysinefunctionalized sepharose(SA-EPL,ξ=9.31 m V)showed high immobilization yield(78.8%),which was4.9-fold than that of nitrilotriacetic acid functionalized sepharose(SA-NTA,ξ=-12.6 m V).The residual activity of affinity co-immobilized enzyme(EPL-Ni/EPL@Ac K-UCK)was higher than 70.6%after recycled 10 times.Thus,this study provides an effective approach for the production of 5'-CMP with the advantages of low adenosine 5'-triphosphate(ATP)consumption,reduced side reactions,and improved reusability by co-immobilized UCK and Ac K on the functionalized Sepharose.
基金the National Natural Science Foundation of China(Nos.81771968,82003166,and 21704061)the Natural Science Foundation of Shanghai(No.21ZR1439200)+3 种基金Shanghai Sailing Program(No.17YF1411000)Shanghai Municipal Education Commission-Gaofeng Clinical Grant Support(No.20181705)Shanghai Municipal Commission of Health and Family Planning(No.201840020)the Medical-Engineering Joint Funds from the Shanghai Jiao Tong University(Nos.ZH2018ZDA05 and YG2016QN54)on this work.
文摘Multi-drug resistance(MDR)has become the largest obstacle to the success of cancer patients receiving traditional chemotherapeutics or novel targeted drugs.Here,we developed a targeted nanoplatform based on biodegradable boronic acid modifiedε-polylysine to co-deliver P-gp siRNA,Bcl-2 siRNA,and doxorubicin for overcoming the challenge.The targeted nanoplatform showed a robust suppressing efficiency for the invasion,proliferation,and colony formation of adriamycin(ADR)resistant breast cancer cell line(MCF-7/ADR)cells in vitro.The ATP responsiveness of the nanoplatform was also proved in the research.In the in vivo antitumor experiment,the targeted nanoplatform showed a significant inhibition of tumor growth with good biocompatibility.The goal of this study is to develop a novel and facile strategy to prepare a highly efficient and safe gene and drug delivery system for MDR breast cancer based on biocompatibleε-polylysine polymers.
