Investigating the optimal size of anticancer nanomedicine

Li Tang(Division of Materials Science and Engineering), Xujuan Yang, Qian Yin(Division of Materials Science and Engineering), Kaimin Cai(Division of Materials Science and Engineering), Hua Wang(Division of Materials Science and Engineering), Isthier Chaudhury(Division of Materials Science and Engineering), Catherine Yao(Division of Materials Science and Engineering), Qin Zhou(Guangdong Pharmaceutical University), Mincheol Kwon(Division of Materials Science and Engineering), James A. Hartman, Iwona T. Dobrucki(University of Illinois Urbana-Champaign), Lawrence W. Dobrucki(Bioengineering Center), Luke B. Borst(North Carolina State University), Stéphane Lezmi, William G. Helferich(Unité de Nutrition Humaine), Andrew L. Ferguson(Division of Materials Science and Engineering), Timothy M. Fan(University of Veterinary Medicine), Jianjun Cheng(Division of Materials Science and Engineering)
Proceedings of the National Academy of Sciences
October 14, 2014
Cited by 659Open Access
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Abstract

Nanomedicines (NMs) offer new solutions for cancer diagnosis and therapy. However, extension of progression-free interval and overall survival time achieved by Food and Drug Administration-approved NMs remain modest. To develop next generation NMs to achieve superior anticancer activities, it is crucial to investigate and understand the correlation between the physicochemical properties of NMs (particle size in particular) and their interactions with biological systems to establish criteria for NM optimization. Here, we systematically evaluated the size-dependent biological profiles of three monodisperse drug-silica nanoconjugates (NCs; 20, 50, and 200 nm) through both experiments and mathematical modeling and aimed to identify the optimal size for the most effective anticancer drug delivery. Among the three NCs investigated, the 50-nm NC shows the highest tumor tissue retention integrated over time, which is the collective outcome of deep tumor tissue penetration and efficient cancer cell internalization as well as slow tumor clearance, and thus, the highest efficacy against both primary and metastatic tumors in vivo.


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