Gdowski Andrew S, Lampe Jana B, Lin Victor J T, Joshi Rohan, Wang Yu-Chieh, Mukerjee Anindita, Vishwanatha Jamboor K, Ranjan Amalendu P
University of North Texas Health Science Center, 3500 Camp Bowie Boulevard, Fort Worth, Texas 76107, United States.
ACS Appl Nano Mater. 2019 Oct 25;2(10):6249-6257. doi: 10.1021/acsanm.9b01226. Epub 2019 Sep 17.
Targeting therapeutic agents to specific organs in the body remains a challenge despite advances in the science of systemic drug delivery. We have engineered a programmable-bioinspired nanoparticle (P-BiNP) delivery system to simultaneously target the bone and increase uptake in homotypic tumor cells by coating polymeric nanoparticles with programmed cancer cell membranes. This approach is unique in that we have incorporated relevant clinical bioinformatics data to guide the design and enhancement of biological processes that these nanoparticles are engineered to mimic. To achieve this, an analysis of RNA expression from metastatic prostate cancer patients identified ITGB3 (a subunit of integrin ) as overexpressed in patients with bone metastasis. Cancer cells were stimulated to increase this integrin expression on the cell surface, and these membranes were subsequently used to coat cargo carrying polymeric nanoparticles. Physicochemical optimization and characterization of the P-BiNPs showed desirable qualities regarding size, potential, and stability. testing confirmed enhanced homotypic binding and uptake in cancer cells. P-BiNPs also demonstrated improved bone localization with a murine model. This novel approach of identifying clinically relevant targets for dual homotypic and bone targeting has potential as a strategy for treatment and imaging modalities in diseases that affect the bone as well as broader implications for delivering nanoparticles to other organs of interest.
尽管全身给药科学取得了进展,但将治疗药物靶向输送至体内特定器官仍然是一项挑战。我们设计了一种可编程生物启发纳米颗粒(P-BiNP)递送系统,通过用编程癌细胞膜包裹聚合物纳米颗粒,同时靶向骨骼并增加同型肿瘤细胞的摄取。这种方法的独特之处在于,我们纳入了相关临床生物信息学数据,以指导这些纳米颗粒模拟的生物过程的设计和优化。为此,对转移性前列腺癌患者的RNA表达分析确定ITGB3(整合素的一个亚基)在骨转移患者中过表达。刺激癌细胞增加细胞表面这种整合素的表达,随后用这些细胞膜包裹携带药物的聚合物纳米颗粒。P-BiNP的物理化学优化和表征显示其在尺寸、电位和稳定性方面具有理想的特性。体外测试证实癌细胞中的同型结合和摄取增强。在小鼠模型中,P-BiNP还显示出改善的骨定位。这种识别双重同型和骨靶向临床相关靶点的新方法,作为一种治疗和成像策略,在影响骨骼的疾病中具有潜力,并且对于将纳米颗粒递送至其他感兴趣的器官具有更广泛的意义。