Jiawei Xiang scite author profile

Galactosyl-terminated drug carriers are known to enhance drug accumulation in the liver, while possible accompanying hepatic toxicity is usually not clarified. This study developed a galactosyl-α,β-poly[(2-hydroxyethyl)-L-aspartamide]-doxorubicin conjugate (Gal-PHEA-DOX) and investigated its therapeutic efficacy and safety in orthotopic hepatocellular carcinoma-bearing mice. Gal-PHEA-DOX had a galactosylation degree of 7.5 mol% and a DOX content of 8.9 wt%. A biodistribution study showed that Gal-PHEA-DOX sustainedly circulated in the plasma and highly accumulated in hepatocarcinoma. Free drug liberated from Gal-PHEA-DOX was relatively low in the liver and heart as compared with that of the DOX administration. The Gal-PHEA-DOX conjugate showed superior cytotoxicity against the hepatocellular carcinoma cell line HepG2 as compared with the nongalactosylated PHEA-DOX conjugate. Gal-PHEA-DOX exhibited comparable antitumor activity with PHEA-DOX in the S180-bearing mice, but more effective than PHEA-DOX or DOX in the Heps-bearing mice with negligible detrimental effect in the liver remnant. A systemic toxicity study showed that this conjugate did not show either cytotoxicity or hepatotoxicity at a relatively high dose, which would be harmful for free DOX. These results suggest that the Gal-PHEA-DOX conjugate has great potential for use in hepatocellular carcinoma chemotherapy because of its enhanced antitumor effect with reduced systemic toxicity including hepatotoxicity.

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Design and biological evaluation of tetrahydropyridine derivatives as novel human GPR119 agonists

Zuo

Chen

Shao

et al. 2020

Bioorganic & Medicinal Chemistry Letters

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Synthesis and biological evaluation of innovative thiourea derivatives as PHGDH inhibitors

Xiang

Tao²,

Zhou

et al. 2020

Chem. Pap.

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Jiawei Xiang

Localized Delivery of Antisense Oligonucleotides by Cationic Hydrogel Suppresses TNF-α Expression and Endotoxin-Induced Osteolysis

Galactosylated α,β-poly[(2-hydroxyethyl)-L-aspartamide]-bound doxorubicin

Design and biological evaluation of tetrahydropyridine derivatives as novel human GPR119 agonists

Synthesis and biological evaluation of innovative thiourea derivatives as PHGDH inhibitors

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