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原位凝胶化氧化柑橘果胶用于局部递抗癌药物和防止同种癌细胞聚集。

In situ gellable oxidized citrus pectin for localized delivery of anticancer drugs and prevention of homotypic cancer cell aggregation.

机构信息

Department of Chemical Engineering, Graduate School of Engineering, Kyushu University, 744 Motooka, Nishi-ku, Fukuoka 819-0385, Japan.

出版信息

Biomacromolecules. 2010 Dec 13;11(12):3525-30. doi: 10.1021/bm1010068. Epub 2010 Oct 28.

Abstract

The aim of this study was to develop in situ gellable hydrogels composed of periodate oxidized citrus pectin (OP) for localized anticancer drug delivery and evaluate the potential of OP to inhibit cancer metastasis. Doxorubicin (Dox) was coupled to OP by imine bonds. Adipic dihydrazide (ADH) was used for cross-linking of the Dox-OP conjugates. The Dox-OP conjugate solution gelled within 2 min after addition of ADH. The release rate of Dox from the hydrogels was controllable by an additive amount of ADH. The released Dox retained anticancer activity. OP was shown to have a potency to prevent homotypic cancer cell aggregation compared to unmodified citrus pectin, strongly suggesting that OP released from hydrogels in vivo will inhibit cancer metastasis. These results indicate that OP hydrogels have the potential to prevent progression of primary cancer by the released Dox and generation of metastatic cancer by the released OP.

摘要

本研究旨在开发原位可凝胶化的水凝胶,由高碘酸盐氧化柑橘果胶(OP)组成,用于局部抗癌药物输送,并评估 OP 抑制癌症转移的潜力。阿霉素(Dox)通过亚胺键偶联到 OP 上。己二酰肼(ADH)用于交联 Dox-OP 缀合物。Dox-OP 缀合物溶液在加入 ADH 后 2 分钟内凝胶化。通过添加 ADH 的量可控制 Dox 从水凝胶中的释放速率。从水凝胶中释放的 Dox 保留了抗癌活性。与未改性的柑橘果胶相比,OP 显示出抑制同源癌细胞聚集的能力,这强烈表明体内从水凝胶中释放的 OP 将抑制癌症转移。这些结果表明,OP 水凝胶具有通过释放 Dox 预防原发性癌症进展和通过释放 OP 产生转移性癌症的潜力。

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