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Drug resistance uptake proteins

The proteins whose abundances are altered in the plasma membrane in drug-resistant cells (Table 13.2) include those involved in increased amino acid uptake (4F2 cell-surface antigen heavy chain, large neutral amino acids transporter small subunit-1), reduced glucose uptake (stomatin, facilitated glucose transport... [Pg.252]

Liposomes The pH-sensitive liposomes so developed were able 56 to overcome the three main problems associated with liposomes, i.e., low stability, slow drug release and accumulation In liver/spleen. The ECM targeting liposome could prevent protein adsorption and drug leakage from liposome due to the biotin 2-PEG cross-linker located on interface of liposome. The uptake within the cancer cell is improved and could actively target tumor in tumor ECM to increase tumor accumulation. Also the drug release was enhanced at low pH, thus the potential bioavailability and drug resistance problem are also avoided. [Pg.762]


See other pages where Drug resistance uptake proteins is mentioned: [Pg.322]    [Pg.180]    [Pg.213]    [Pg.287]    [Pg.371]    [Pg.43]    [Pg.506]    [Pg.30]    [Pg.7]    [Pg.42]    [Pg.206]    [Pg.22]    [Pg.86]    [Pg.582]    [Pg.254]    [Pg.109]    [Pg.150]    [Pg.276]    [Pg.76]    [Pg.53]    [Pg.242]    [Pg.552]    [Pg.281]    [Pg.212]    [Pg.1333]    [Pg.254]    [Pg.122]    [Pg.350]    [Pg.365]    [Pg.2290]    [Pg.276]    [Pg.59]    [Pg.325]    [Pg.213]    [Pg.1777]    [Pg.225]    [Pg.22]    [Pg.366]    [Pg.214]    [Pg.246]    [Pg.204]    [Pg.212]    [Pg.278]    [Pg.618]    [Pg.596]    [Pg.144]    [Pg.759]    [Pg.254]   
See also in sourсe #XX -- [ Pg.375 ]




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