The phenomenon has been used widely to explain the efficiency of nanoparticle and macromolecular drug accumulation in tumours [27]. Unfortunately, knowledge of LNP biokinetics, metabolism, and clearance is otherwise poor since too few LNP products have been clinically tested. This is a major limitation
in the growth of the field of cancer nanotechnology. Nevertheless, cancer nanotechnology is a fast developing field and new data is arriving all the time. In the following sections, the status of LNP use in cancer diagnosis and therapy will be surveyed. 2. Prototype Drug Nanoparticles for Cancer Therapy The capacity of LNPs Inhibitors,research,lifescience,medical to be prepared by reliable, spontaneous self-assembly from purpose designed chemical components (most of which are lipids either natural or synthetic) is due to the Imatinib Mesylate 220127-57-1 unrivalled capacity of structural lipids
in aqueous solution to undergo association and controlled assembly into potentially vast three-dimensional Inhibitors,research,lifescience,medical macromolecular assemblies. Inhibitors,research,lifescience,medical Selected structural lipids self-assemble into liposomes that are typically approximately 100nm in diameter and consist of a lipid bilayer surrounding an aqueous cavity [28–30]. This cavity can be used to entrap water-soluble drugs in an enclosed volume resulting in a drug-AB nanoparticle [31, 32]. The first drug-AB nanoparticles reported were designed to selleck chem inhibitor improve the pharmacokinetics and biodistribution of the Inhibitors,research,lifescience,medical anthracycline
drug doxorubicin. Doxorubicin is a potent anticancer agent but is cardiotoxic. In order to minimize cardiotoxicity, doxorubicin was initially encapsulated in anionic liposomes giving anionic doxorubicin-AB nanoparticles that enabled improved drug accumulation in tumours and increased antitumour activity Inhibitors,research,lifescience,medical while diminishing side effects of cardiotoxicity [33, 34]. Such drug formulations have been used efficiently in clinic for the treatment of ovarian and breast cancer [35, 36]. Thereafter, Brefeldin_A Doxil was devised corresponding to a drug-ABC nanoparticle system (PEGylated drug nanoparticle system), comprising PEGylated liposomes with encapsulated doxorubicin. These Doxil drug nanoparticles were designed to improve drug pharmacokinetics and reduce toxicity further by maximizing RES avoidance [37–39], making use of the PEG layer to reduce uptake by RES macrophages of the mononuclear phagocyte system (MPS) [40, 41]. In more recent times, prototype nucleic acid-AB, -ABC, or -ABCD nanoparticles have been tested for functional delivery of therapeutic nucleic acids to target cells in animal models of human disease (to liver for treatment of hepatitis B and C virus infection, to ovarian cancer lesions for cancer therapy) and to target cells in murine lungs [42–47].