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首页> 外文期刊>Biomaterials Science >A drug formulation using an alginate hydrogel matrix for efficient oral delivery of the manganese porphyrin-based superoxide dismutase mimic
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A drug formulation using an alginate hydrogel matrix for efficient oral delivery of the manganese porphyrin-based superoxide dismutase mimic

机译:使用藻酸盐水凝胶基质的药物制剂,可有效地口服递送基于锰卟啉的超氧化物歧化酶模拟物

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摘要

In order for patients to avail of the therapeutic benefits of antioxidant drugs efficiently and conveniently, a robust oral delivery system needs to be developed. However, a common problem in oral drug delivery is ensuring that the drug remains functionally intact even after it has passed through the acidic environment of the gastrointestinal (GI) tract. To protect drugs within the GI environment, we formulated a design based on encapsulating liposomal drugs by using an alginate matrix as a carrier. The liposomal drug was composed of manganese porphyrin (Mn-por), which has been developed as a mimic of superoxide dismutase (SOD), as the therapeutic agent based on the antioxidative effect, namely superoxide (O-2(center dot-)) inhibitory activity. A cytochrome c assay revealed that the O-2(center dot-) inhibitory activity of Mn-por could be maintained even after treatment with simulated gastric and intestinal fluids. We demonstrated that oral administration of the formulated drug significantly inhibited the growth of transplanted tumors in mice. The drug formulation presented in this study would be a good candidate for orally available systems, which can effectively deliver SOD mimics.
机译:为了使患者有效和方便地利用抗氧化剂的治疗益处,需要开发一种健壮的口服递送系统。但是,口服药物输送中的一个普遍问题是即使在通过胃肠道(GI)的酸性环境后,也要确保药物保持功能完整。为了在GI环境中保护药物,我们制定了一种设计方法,该方法以藻酸盐基质为载体,封装脂质体药物。脂质体药物由锰卟啉(Mn-por)组成,锰卟啉已被开发为模仿超氧化物歧化酶(SOD),作为基于抗氧化作用的治疗剂,即超氧化物(O-2(中心点-))抑制活性。细胞色素c分析显示,即使用模拟的胃液和肠液治疗,Mn-por的O-2(中心点)抑制活性也可以保持。我们证明了口服配制的药物显着抑制了小鼠移植肿瘤的生长。这项研究中提出的药物配方将是口服可用系统的良好候选者,该系统可以有效地提供SOD模拟物。

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