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在斑马鱼胚胎中纳米 ZIF-8 的溶解和生物评估

Dissolution and Biological Assessment of Cancer-Targeting Nano-ZIF-8 in Zebrafish Embryos.

机构信息

Integrated Chemical BioPhysics Research, Faculty of Science, Universiti Putra Malaysia (UPM), Serdang 43400, Selangor, Malaysia.

UPM-MAKNA Cancer Laboratory, Institute of Bioscience, Universiti Putra Malaysia, Serdang 43400, Selangor, Malaysia.

出版信息

ACS Biomater Sci Eng. 2022 Jun 13;8(6):2445-2454. doi: 10.1021/acsbiomaterials.2c00186. Epub 2022 May 18.

DOI:10.1021/acsbiomaterials.2c00186
PMID:35583465
Abstract

Cancer-targeting nanotherapeutics offer promising opportunities for selective delivery of cytotoxic chemotherapeutics to cancer cells. However, the understanding of dissolution behavior and safety profiles of such nanotherapeutics is scarce. In this study, we report the dissolution profile of a cancer-targeting nanotherapeutic, gemcitabine (GEM) encapsulated within RGD-functionalized zeolitic imidazolate framework-8 (GEM⊂RGD@nZIF-8), in dissolution media having pH = 6.0 and 7.4. GEM⊂RGD@nZIF-8 was not only responsive in acidic media (pH = 6.0) but also able to sustain the dissolution rate (57.6%) after 48 h compared to non-targeting nanotherapeutic GEM⊂nZIF-8 (76%). This was reflected by the value of 36.1, which indicated a difference in the dissolution behaviors of GEM⊂RGD@nZIF-8 and GEM⊂nZIF-8 in acidic media compared to those in neutral media (pH = 7.4). A dissolution kinetic study showed that the GEM release mechanism from GEM⊂RGD@nZIF-8 followed the Higuchi model. In comparison to a non-targeting nanotherapeutic, the cancer-targeting nanotherapeutic exhibited an enhanced permeability rate in healthy zebrafish embryos but did not induce lethality to 50% of the embryos (LC > 250 μg mL) with significantly improved survivability (75%) after 96 h of incubation. Monitoring malformation showed minimal adverse effects with only 8.3% of edema at 62.5 μg mL. This study indicates that cancer-targeting GEM⊂RGD@nZIF, with its pH-responsive behavior for sustaining chemotherapeutic dissolution in a physiologically relevant environment and its non-toxicity toward the healthy embryos within the tested concentrations, has considerable potential for use in cancer treatment.

摘要

癌症靶向纳米治疗为细胞毒性化疗药物向癌细胞的选择性输送提供了有前景的机会。然而,对于这种纳米治疗的溶解行为和安全性概况的了解甚少。在这项研究中,我们报告了癌症靶向纳米治疗药物,即包裹在 RGD 功能化沸石咪唑骨架-8(GEM⊂RGD@nZIF-8)中的吉西他滨(GEM)在 pH 值为 6.0 和 7.4 的溶解介质中的溶解情况。GEM⊂RGD@nZIF-8 不仅在酸性介质(pH = 6.0)中具有响应性,而且在 48 小时后与非靶向纳米治疗药物 GEM⊂nZIF-8(76%)相比,能够维持溶解速率(57.6%)。这反映在 值为 36.1,这表明与中性介质(pH = 7.4)相比,GEM⊂RGD@nZIF-8 和 GEM⊂nZIF-8 在酸性介质中的溶解行为存在差异。溶解动力学研究表明,GEM 从 GEM⊂RGD@nZIF-8 的释放机制遵循 Higuchi 模型。与非靶向纳米治疗药物相比,该癌症靶向纳米治疗药物在健康斑马鱼胚胎中表现出增强的渗透性,但对 50%的胚胎没有致死性(LC > 250 μg mL),在孵育 96 小时后具有显著提高的存活率(75%)。监测畸形显示,只有在 62.5 μg mL 时才有 8.3%的水肿,副作用极小。这项研究表明,具有 pH 响应行为的癌症靶向 GEM⊂RGD@nZIF 在生理相关环境中维持化疗溶解,并在测试浓度内对健康胚胎无毒,具有在癌症治疗中应用的巨大潜力。

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