D-arginine-loaded metal-organic frameworks nanoparticles sensitize osteosarcoma to radiotherapy

C Du, M Zhou, F Jia, L Ruan, H Lu, J Zhang, B Zhu… - Biomaterials, 2021 - Elsevier
C Du, M Zhou, F Jia, L Ruan, H Lu, J Zhang, B Zhu, X Liu, J Chen, Z Chai, Y Hu
Biomaterials, 2021Elsevier
Osteosarcoma is a common type of bone cancers with a high rate of pulmonary recurrence.
High-dose radiation therapy is useful for the ablation of unresectable osteosarcoma.
However, it may cause severe adverse effects. To address this problem, we developed D-
arginine-loaded metal-organic frameworks (MOF) nanoparticles for improving the
radiosensitivity of osteosarcoma. D-arginine, a metabolically inert enantiomer of L-arginine,
could produce nitric oxide and down-regulate hypoxia-inducible factor-1alpha (HIF-1α) to …
Abstract
Osteosarcoma is a common type of bone cancers with a high rate of pulmonary recurrence. High-dose radiation therapy is useful for the ablation of unresectable osteosarcoma. However, it may cause severe adverse effects. To address this problem, we developed D-arginine-loaded metal-organic frameworks (MOF) nanoparticles for improving the radiosensitivity of osteosarcoma. D-arginine, a metabolically inert enantiomer of L-arginine, could produce nitric oxide and down-regulate hypoxia-inducible factor-1alpha (HIF-1α) to alleviate tumor hypoxia. In addition, MOF could also generate free radicals to kill the tumor cells. Results demonstrate that D-arginine-loaded nanoparticles enhanced tumor ablation and prevented the lung metastasis in mice upon radiation therapy. Furthermore, the nanoparticles or radiation alone had relatively low toxicity in cells and mice. Therefore, D-arginine-loaded MOF nanoparticles are relatively safe and highly effective in sensitizing osteosarcoma to radiotherapy.
Elsevier
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