Kuhelj R, Rizzo C J, Chang C H, Jadhav P K, Towler E M, Korant B D
Department of Virology, Experimental Station, DuPont Pharmaceuticals, Wilmington, Delaware 19880, USA.
J Biol Chem. 2001 May 18;276(20):16674-82. doi: 10.1074/jbc.M008763200. Epub 2001 Feb 21.
A full-length and C-terminally truncated version of human endogenous retrovirus (HERV)-K10 protease were expressed in Escherichia coli and purified to homogeneity. Both versions of the protease efficiently processed HERV-K10 Gag polyprotein substrate. HERV-K10 Gag was also cleaved by human immunodeficiency virus, type 1 (HIV-1) protease, although at different sites. To identify compounds that could inhibit protein processing dependent on the HERV-K10 protease, a series of cyclic ureas that had previously been shown to inhibit HIV-1 protease was tested. Several symmetric bisamides acted as very potent inhibitors of both the truncated and full-length form of HERV-K10 protease, in subnanomolar or nanomolar range, respectively. One of the cyclic ureas, SD146, can inhibit the processing of in vitro translated HERV-K10 Gag polyprotein substrate by HERV-K10 protease. In addition, in virus-like particles isolated from the teratocarcinoma cell line NCCIT, there is significant accumulation of Gag and Gag-Pol precursors upon treatment with SD146, suggesting the compound efficiently blocks HERV-K Gag processing in cells. This is the first report of an inhibitor able to block cell-associated processing of Gag polypeptides of an endogenous retrovirus.
人内源性逆转录病毒(HERV)-K10蛋白酶的全长和C末端截短版本在大肠杆菌中表达并纯化至均一性。这两个版本的蛋白酶都能有效地加工HERV-K10 Gag多聚蛋白底物。HERV-K10 Gag也能被1型人类免疫缺陷病毒(HIV-1)蛋白酶切割,尽管切割位点不同。为了鉴定能够抑制依赖HERV-K10蛋白酶的蛋白质加工的化合物,测试了一系列先前已被证明能抑制HIV-1蛋白酶的环脲。几种对称双酰胺分别在亚纳摩尔或纳摩尔范围内,对截短型和全长型HERV-K10蛋白酶均表现出非常有效的抑制作用。其中一种环脲SD146能够抑制HERV-K10蛋白酶对体外翻译的HERV-K10 Gag多聚蛋白底物的加工。此外,在用SD146处理从畸胎瘤细胞系NCCIT分离的病毒样颗粒时,Gag和Gag-Pol前体有显著积累,这表明该化合物能有效阻断细胞内HERV-K Gag的加工。这是关于一种能够阻断内源性逆转录病毒Gag多肽细胞相关加工的抑制剂的首次报道。
