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Systemic Delivery of Gemcitabine Triphosphate via LCP Nanoparticles for NSCLC and Pancreatic Cancer Therapy

机译:通过LCP纳米粒子通过LCP纳米粒子进行全身递送NSCLC和胰腺癌治疗

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摘要

Nucleoside analogues are a significant class of anticancer agent. As prodrugs, they terminate the DNA synthesis upon transforming to their active triphosphate metabolites. We have encapsulated a biologically activate nucleotide analogue (i.e. gemcitabine triphosphate (GTP)), instead of the nucleoside (i.e. gemcitabine) derivative, into a novel Lipid/Calcium/Phosphate nanoparticle (LCP) platform. The therapeutic efficacy of LCP-formulated GTP was evaluated in a panel of human non-small-cell lung cancer (NSCLC) and human pancreatic cancer models after systemic administrations. GTP-loaded LCPs induced cell death and arrested the cell cycle in the S phase. In vivo efficacy studies showed that intravenously injected GTP-loaded LCPs triggered effective apoptosis of tumor cells, significant reduction of tumor cell proliferation and cell cycle progression, leading to dramatic inhibition of tumor growth, with little in vivo toxicity. Broadly speaking, the current study offers preclinical proof-of-principle that many active nucleotide or phosphorylated nucleoside analogues could be encapsulated in the LCP nanoplatform and delivered systemically for a wide variety of therapeutic applications.
机译:核苷类似物是一类重要的抗癌药。作为前药,它们在转化为活性三磷酸代谢物后终止DNA合成。我们已经将一种生物活化的核苷酸类似物(即吉西他滨三磷酸(GTP))而不是核苷(即吉西他滨)衍生物封装到新型脂质/钙/磷酸盐纳米颗粒(LCP)平台中。在系统性给药后,在一组人非小细胞肺癌(NSCLC)和人胰腺癌模型中评估了LCP配制的GTP的治疗效果。装载GTP的LCP诱导细胞死亡,并使细胞周期停滞在S期。体内功效研究表明,静脉注射负载GTP的LCP可以触发肿瘤细胞的有效凋亡,显着降低肿瘤细胞的增殖和细胞周期进程,从而导致对肿瘤生长的显着抑制,而几乎没有体内毒性。从广义上讲,当前的研究提供了临床前的原理证明,即许多活性核苷酸或磷酸化的核苷类似物都可以封装在LCP纳米平台中,并系统地交付用于各种治疗应用。

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