| Literature DB >> 29196043 |
Pilar de la Puente1, Micah J Luderer1, Cinzia Federico1, Abbey Jin2, Rebecca C Gilson3, Christopher Egbulefu3, Kinan Alhallak1, Shruti Shah1, Barbara Muz1, Jennifer Sun1, Justin King4, Daniel Kohnen4, Noha Nabil Salama5, Samuel Achilefu3, Ravi Vij4, Abdel Kareem Azab6.
Abstract
The establishment of more effective treatments that can circumvent chemoresistance in Multiple Myeloma (MM) is a priority. Although bortezomib (BTZ) is one of the most potent proteasome inhibitors available, still possesses limitations related to dose limiting side effects. Several strategies have been developed to improve the delivery of chemotherapies to MM by targeting different moieties expressed on MM cells to nanoparticle delivery systems (NPs), which have failed mainly due to their heterogeneous expression on these cells. Our goal was to test CD38 targeted chitosan NPs as novel targeting moiety for MM to improve the potency and efficacy of BTZ in MM cells and reduce the side effects in healthy tissue. We have showed preferential BTZ release in tumor-microenvironment, specific binding to MM cells, and an improved drug cellular uptake through BTZ diffusion from the surface and endocytosed NPs, which translated in enhanced proteasome inhibition and robust cytotoxic effect on MM cells when BTZ was administered through anti-CD38 chitosan NPs. Furthermore, the anti-CD38 chitosan NPs specifically delivered therapeutic agents to MM cells improving therapeutic efficacy and reducing side effects in vivo. The anti-CD38 chitosan NPs showed low toxicity profile allowing enhancement of proteasome-inhibitory activity and specificity of BTZ by endocytosis-mediated uptake of CD38 representing a promising therapy in MM.Entities:
Keywords: Bortezomib; CD38; Endocytosis; Nanoparticles, multiple myeloma
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Year: 2017 PMID: 29196043 PMCID: PMC6056271 DOI: 10.1016/j.jconrel.2017.11.045
Source DB: PubMed Journal: J Control Release ISSN: 0168-3659 Impact factor: 9.776