Center for Drug Design, College of Pharmacy, University of Minnesota, Minneapolis, MN 55455, USA.
ChemMedChem. 2022 Sep 5;17(17):e202200334. doi: 10.1002/cmdc.202200334. Epub 2022 Aug 10.
Human cytomegalovirus (HCMV) replication requires a metal-dependent endonuclease at the C-terminus of pUL89 (pUL89-C) for viral genome packaging and cleavage. We have previously shown that pUL89-C can be pharmacologically inhibited with designed metal-chelating compounds. We report herein the synthesis of a few 8-hydroxy-1,6-naphthyridine subtypes, including 5-chloro (subtype 15), 5-aryl (subtype 16), and 5-amino (subtype 17) variants. Analogs were studied for the inhibition of pUL89-C in a biochemical endonuclease assay, a biophysical thermal shift assay (TSA), in silico molecular docking, and for the antiviral potential against HCMV in cell-based assays. These studies identified eight analogs of 8-hydroxy-1,6-naphthyridine-7-carboxamide subtypes for further characterization, most of which inhibited pUL89-C with single-digit μM IC values, and conferred antiviral activity in μM range. TSA and molecular modeling of selected analogs corroborate their binding to pUL89-C. Collectively, our biochemical, antiviral, biophysical and in silico data suggest that 8-hydroxy-1,6-naphthyridine-7-carboxamide subtypes can be used for designing inhibitors of HCMV pUL89-C.
人巨细胞病毒(HCMV)复制需要 pUL89(pUL89-C)C 端的金属依赖性内切核酸酶进行病毒基因组包装和切割。我们之前已经证明,pUL89-C 可以用设计的金属螯合化合物进行药理学抑制。我们在此报告几种 8-羟基-1,6-萘啶的合成,包括 5-氯(亚型 15)、5-芳基(亚型 16)和 5-氨基(亚型 17)变体。在生化内切核酸酶测定、生物物理热转移测定(TSA)、计算机分子对接以及基于细胞的测定中针对 HCMV 的抗病毒潜力方面研究了类似物对 pUL89-C 的抑制作用。这些研究确定了 8-羟基-1,6-萘啶-7-甲酰胺亚型的八种类似物用于进一步表征,其中大多数类似物以单位数 μM IC 值抑制 pUL89-C,并在 μM 范围内具有抗病毒活性。TSA 和选定类似物的分子建模证实了它们与 pUL89-C 的结合。总的来说,我们的生化、抗病毒、生物物理和计算机数据表明,8-羟基-1,6-萘啶-7-甲酰胺亚型可用于设计 HCMV pUL89-C 的抑制剂。
