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Convertible MRI contrast: Sensing the delivery and release of anti-glioma nano-drugs

机译:可转换MRI对比:感知抗神经胶质瘤纳米药物的传递和释放

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There is considerable interest in developing nanohybrids of imaging contrast agents and drugs for image-guided drug delivery. We have developed a strategy of utilizing manganese (Mn) to enhance the nano-encapsulation of arsenic trioxide (ATO). Formation of arsenite (As3+)-Mn precipitates in liposomes generates magnetic susceptibility effects, reflected as dark contrast on T2-weighted MRI. Intriguingly, following cell uptake, the As-Mn complex decomposes in response to low pH in endosome-lysosome releasing ionic As3+, the active form of ATO, and Mn2+, the T1 contrast agent that gives a bright signal. Glioblastoma (GBM) is well known for its high resistance to chemotherapy, e.g., temozolomide (TMZ). Building upon the previously established phosphatidylserine (PS)-targeted nanoplatform that has excellent GBM-targeting specificity, we now demonstrate the effectiveness of the targeted nanoformulated ATO for treating TMZ-resistant GBM cells and the ability of the convertible Mn contrast as a surrogate revealing the delivery and release of ATO.
机译:开发成像造影剂和用于图像引导药物递送的药物的纳米杂交体引起了相当大的兴趣。我们已经开发出一种利用锰(Mn)增强三氧化二砷(ATO)纳米封装的策略。脂质体中砷(As 3 + )-Mn沉淀的形成会产生磁化率效应,在T 2 加权MRI上表现为暗对比度。有趣的是,细胞摄取后,As-Mn复合物在低pH下分解,释放释放的离子型As 3 + ,ATO活性形式和Mn 2 + ,T 1 造影剂,发出明亮的信号。胶质母细胞瘤(GBM)以其对化疗的高耐药性而闻名,例如替莫唑胺(TMZ)。建立在先前建立的具有出色的GBM靶向特异性的磷脂酰丝氨酸(PS)靶向纳米平台的基础上,我们现在证明靶向纳米制剂ATO治疗TMZ耐药性GBM细胞的有效性以及可转换的Mn对比剂替代物的揭示能力ATO的交付和发布。

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