Synthesis and antiviral evaluation of novel heteroarylpyrimidines analogs as HBV capsid effectors

新型杂芳基嘧啶类似物作为乙型肝炎病毒衣壳效应物的合成及抗病毒活性评价

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Abstract

New modifications to the scaffold of previously reported HBV capsid assembly effectors such as BAY 41-4109, HAP-12 and GLS4 were explored. The anti-HBV activity in the HepAD38 system, and cytotoxicity profiles of each of the new compounds has been assessed. Among them, five new iodo- and bromo-heteroarylpyrimidines analogs displayed anti-HBV activity in the low micromolar range.

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