This is particularly problematic as it is imperative that these Wee1 inhibitor systems remain in circulation long enough such that they can accumulate within tumor tissue at levels great enough to have the intended cytotoxic effect. One obvious method for overcoming this obstacle involves the overall size reduction of the nanocarrier, which as mentioned
Inhibitors,research,lifescience,medical earlier also has the unfortunate effect of translating into less drug being delivered by the nanocarrier. Another proven method for overcoming this obstacle without compromising the amount of chemotherapeutic being delivered to tumors is the surface coating of these drug delivery vehicles with polymers, particularly polyethylene glycol (PEG). This generates “Stealth” liposomes, which is a name Inhibitors,research,lifescience,medical given to them based on their ability to evade the immune system resulting in significant increases in circulations
times in vivo [14, 19, 20]. In fact, the benefit of pegylation is quite apparent when comparing the relative half-lives of nonpegylated and pegylated liposomes which increases from just a few hours to as much as 45 hours, respectively [9]. Therefore, it is not surprising to note that the clinically approved drug Doxil is in fact pegylated (Mr 2000) in order to improve tumor site accumulation of the drug [14]. However, while surface Inhibitors,research,lifescience,medical coating liposomes with PEG achieve desirable circulation times in vivo, Inhibitors,research,lifescience,medical it also negatively influences tumor cellular uptake of these systems as the presence of the PEG moiety presents a steric barrier between the drug and cancer cells [10]. Therefore, while pegylation does not eliminate cellular uptake entirely, delivery of pegylated liposome-based chemotherapeutics is in large part based on the ability of the encapsulated drug to escape or be released from the nanocarrier
Inhibitors,research,lifescience,medical via leakage in the tumor microenvironment prior to tumor cellular uptake of the free drug. Therefore, future strategies involving the improved delivery efficiency of pegylated liposome-based drugs, particularly in the treatment of breast cancer, are aimed at various enhanced triggered release techniques to facilitate this process. One such method involves the heat-triggered release of pegylated thermosensitive liposomes. 2.1. Hyperthermia and Improved Liposome-Based Drug Delivery While liposome-based drugs of the appropriate size MycoClean Mycoplasma Removal Kit retain the ability to extravasate out of circulation at tumor sites, various challenges remain involving release of the encapsulated drug from the nanocarrier. Therefore, one aspect with respect to the future design of these drugs involves the incorporation of various molecules within liposomal formulations that respond to external stimuli in a manner that disrupts liposomes to allow for the delivery of encapsulated material.