Yi-Feng Zhang, Kun Chen, Yu-Qing Zhu, Lin Liu, Xiang-Tao Kong, Yan Dai, Xiu-Juan Fu, Ya-Ling Li, Ming-Hua Liu, Dan Zhang
{"title":"癌细胞膜包被含硫麻酸ph敏感脂质体的制备及靶向抗肝癌作用的研究。","authors":"Yi-Feng Zhang, Kun Chen, Yu-Qing Zhu, Lin Liu, Xiang-Tao Kong, Yan Dai, Xiu-Juan Fu, Ya-Ling Li, Ming-Hua Liu, Dan Zhang","doi":"10.1007/s13346-025-01949-y","DOIUrl":null,"url":null,"abstract":"<p><p>Hepatocellular carcinoma has an insidious onset, and therefore, most patients are already in the middle or advanced stage once diagnosed, which seriously affects the prognosis of the patients. For a long time, it has been difficult to achieve the expected effect of the treatment that can effectively deal with the middle-or-late -stage liver cancer. Gambogic acid (GA), a dry resin secreted by the Garcinia hanbaryi Hook.f., is a natural active ingredient with various biological activities, especially the strong anti-hepatocellular carcinoma activity. However, the drawbacks such as high toxicity to the liver and kidney and low solubility have greatly limited its application. Therefore, it is necessary to develop suitable Gambogic acid formulations to overcome these disadvantages. In this study, injectable HepG2 cell membrane-modified pH-responsive liposomes (PEOz/GA@HepG2m) were prepared for active targeted delivery of Gambogic acid for the treatment of hepatocellular carcinoma. The physicochemical properties of PEOz/GA@HepG2m were evaluated in terms of the drug loading efficiency, particle size, morphology and drug release. The inhibitory effect of PEOz/GA@HepG2m on the proliferation of hepatocellular carcinoma cells was assessed by CCK8 assay and calcein-AM/PI assay in vitro. The effect of unloaded liposome PEOz@HepG2m on cellular internalization was assessed in different cell lines and it's in vivo biodistribution was analyzed by near-infrared (NIR) fluorescence imaging. The antitumor effect of PEOz/GA@HepG2m in vivo was evaluated in HepG2 tumor-bearing nude mice. The PEOz@HepG2m liposomes exhibit excellent targeting ability toward HepG2 cells. PEOz/GA@HepG2m possesses high delivery efficiency and a remarkably therapeutic effect both in vitro and vivo. The coating HepG2 cell membrane could significantly enhance the tumor-targeting effect of the liposomes and improve the antitumor effect of the loaded drug GA in vivo, indicating that the active-targeting biomimetic liposome, PEOz/GA@HepG2m, is a promising nanoplatform for delivery of drugs to hepatocellular carcinoma.</p>","PeriodicalId":11357,"journal":{"name":"Drug Delivery and Translational Research","volume":" ","pages":""},"PeriodicalIF":5.5000,"publicationDate":"2025-08-17","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"Preparation of cancer cell membrane-coated Gambogic acid-loaded pH-sensitive liposomes to enhance targeted anti-hepatocellular carcinoma effect.\",\"authors\":\"Yi-Feng Zhang, Kun Chen, Yu-Qing Zhu, Lin Liu, Xiang-Tao Kong, Yan Dai, Xiu-Juan Fu, Ya-Ling Li, Ming-Hua Liu, Dan Zhang\",\"doi\":\"10.1007/s13346-025-01949-y\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<p><p>Hepatocellular carcinoma has an insidious onset, and therefore, most patients are already in the middle or advanced stage once diagnosed, which seriously affects the prognosis of the patients. For a long time, it has been difficult to achieve the expected effect of the treatment that can effectively deal with the middle-or-late -stage liver cancer. Gambogic acid (GA), a dry resin secreted by the Garcinia hanbaryi Hook.f., is a natural active ingredient with various biological activities, especially the strong anti-hepatocellular carcinoma activity. However, the drawbacks such as high toxicity to the liver and kidney and low solubility have greatly limited its application. Therefore, it is necessary to develop suitable Gambogic acid formulations to overcome these disadvantages. In this study, injectable HepG2 cell membrane-modified pH-responsive liposomes (PEOz/GA@HepG2m) were prepared for active targeted delivery of Gambogic acid for the treatment of hepatocellular carcinoma. The physicochemical properties of PEOz/GA@HepG2m were evaluated in terms of the drug loading efficiency, particle size, morphology and drug release. The inhibitory effect of PEOz/GA@HepG2m on the proliferation of hepatocellular carcinoma cells was assessed by CCK8 assay and calcein-AM/PI assay in vitro. The effect of unloaded liposome PEOz@HepG2m on cellular internalization was assessed in different cell lines and it's in vivo biodistribution was analyzed by near-infrared (NIR) fluorescence imaging. The antitumor effect of PEOz/GA@HepG2m in vivo was evaluated in HepG2 tumor-bearing nude mice. The PEOz@HepG2m liposomes exhibit excellent targeting ability toward HepG2 cells. PEOz/GA@HepG2m possesses high delivery efficiency and a remarkably therapeutic effect both in vitro and vivo. 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Preparation of cancer cell membrane-coated Gambogic acid-loaded pH-sensitive liposomes to enhance targeted anti-hepatocellular carcinoma effect.
Hepatocellular carcinoma has an insidious onset, and therefore, most patients are already in the middle or advanced stage once diagnosed, which seriously affects the prognosis of the patients. For a long time, it has been difficult to achieve the expected effect of the treatment that can effectively deal with the middle-or-late -stage liver cancer. Gambogic acid (GA), a dry resin secreted by the Garcinia hanbaryi Hook.f., is a natural active ingredient with various biological activities, especially the strong anti-hepatocellular carcinoma activity. However, the drawbacks such as high toxicity to the liver and kidney and low solubility have greatly limited its application. Therefore, it is necessary to develop suitable Gambogic acid formulations to overcome these disadvantages. In this study, injectable HepG2 cell membrane-modified pH-responsive liposomes (PEOz/GA@HepG2m) were prepared for active targeted delivery of Gambogic acid for the treatment of hepatocellular carcinoma. The physicochemical properties of PEOz/GA@HepG2m were evaluated in terms of the drug loading efficiency, particle size, morphology and drug release. The inhibitory effect of PEOz/GA@HepG2m on the proliferation of hepatocellular carcinoma cells was assessed by CCK8 assay and calcein-AM/PI assay in vitro. The effect of unloaded liposome PEOz@HepG2m on cellular internalization was assessed in different cell lines and it's in vivo biodistribution was analyzed by near-infrared (NIR) fluorescence imaging. The antitumor effect of PEOz/GA@HepG2m in vivo was evaluated in HepG2 tumor-bearing nude mice. The PEOz@HepG2m liposomes exhibit excellent targeting ability toward HepG2 cells. PEOz/GA@HepG2m possesses high delivery efficiency and a remarkably therapeutic effect both in vitro and vivo. The coating HepG2 cell membrane could significantly enhance the tumor-targeting effect of the liposomes and improve the antitumor effect of the loaded drug GA in vivo, indicating that the active-targeting biomimetic liposome, PEOz/GA@HepG2m, is a promising nanoplatform for delivery of drugs to hepatocellular carcinoma.
期刊介绍:
The journal provides a unique forum for scientific publication of high-quality research that is exclusively focused on translational aspects of drug delivery. Rationally developed, effective delivery systems can potentially affect clinical outcome in different disease conditions.
Research focused on the following areas of translational drug delivery research will be considered for publication in the journal.
Designing and developing novel drug delivery systems, with a focus on their application to disease conditions;
Preclinical and clinical data related to drug delivery systems;
Drug distribution, pharmacokinetics, clearance, with drug delivery systems as compared to traditional dosing to demonstrate beneficial outcomes
Short-term and long-term biocompatibility of drug delivery systems, host response;
Biomaterials with growth factors for stem-cell differentiation in regenerative medicine and tissue engineering;
Image-guided drug therapy,
Nanomedicine;
Devices for drug delivery and drug/device combination products.
In addition to original full-length papers, communications, and reviews, the journal includes editorials, reports of future meetings, research highlights, and announcements pertaining to the activities of the Controlled Release Society.
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