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nanocarrier (Hu, 2010; Kratz, 2012; Zhang, 2011), and even more
challenging to deliver such cargos in vivo, where it is absolutely
necessary to supply the proper drug ratio at the tumor level (Mayer,
2006). Several nanoparticulate systems such as lipid-based, inorganic
and polymeric nanoparticles, among other types, have been used to co-
load two or more different payloads adopting different strategies (Hu,
2010). Some include the physical adsorption of drugs to the nanovector,
with the disadvantage that only drugs with similar physicochemical
properties can be loaded simultaneously (Herranz-Blanco, 2014; Liu,
2012; 2014a). It is also possible to co-load molecules with different
physicochemical properties via a sequential adsorption procedure (Liu,
2013a). Others have followed the incorporation of therapeutics into the
particle matrix during particle preparation (Doane, 2013), and covalently
bonded the drug molecules to the polymeric backbone after particle
preparation (Aryal, 2011).
Despite the obstacles encountered in cancer therapy, extensive
progress has been made so far and nowadays there are several
nanoformulations that combine two or more different anticancer drugs
(Liao, 2014; Tardi, 2009) or even two different classes of therapeutics
(Deng, 2013; Liu, 2014b; Saad, 2008). For example, a nanoparticulate
system was developed by Deng using a layer-by-layer deposition
approach (Deng, 2013). Liposomes were chosen to be encapsulated by
polycationic PLA through the layer-by-layer deposition, and finally
coated by a layer of hyaluronic acid that enhances the in vivo stability of
the nanosystem (Poon, 2011). This system co-delivered siRNA molecules
and doxorubicin loaded in the core of the liposomes, which were able to
knockdown a drug resistance pathway in tumor cells (Whitehead, 2009).
This means they can be applied in the treatment of triple-negative breast
cancer form, which is an estrogen, progesterone and human epidermal
growth factor receptor 2 (HER2)-negative cancer type with a more
aggressive effect than other breast cancers (Kassam, 2009; Livasy,
2006). The successful co-delivery of both siRNA and doxorubicin was
achieved, as well as significantly enhanced DXR efficacy by 4-fold in
vitro (Fig. 3.5.6). The in vivo results showed an 8-fold decrease in tumor
volume compared to the control treatments, with no observed toxicity to
the animals. An ultimate outer layer of hyaluronic acid (HA) was
Biomedical Chemistry: Current Trends and Developments
- Titel
- Biomedical Chemistry: Current Trends and Developments
- Autor
- Nuno Vale
- Verlag
- De Gruyter Open Ltd
- Datum
- 2016
- Sprache
- englisch
- Lizenz
- CC BY-NC-ND 4.0
- ISBN
- 978-3-11-046887-8
- Abmessungen
- 21.0 x 29.7 cm
- Seiten
- 427
- Schlagwörter
- Physical Sciences, Engineering and Technology, Chemistry, Organic Chemistry, Green Chemistry
- Kategorien
- Naturwissenschaften Chemie