CMX001 (1-O-Hexadecyloxypropyl-Cidofovir) Inhibits Polyomavirus JC Replication in Human Brain Progenitor-Derived Astrocytes

被引:41
作者
Gosert, Rainer [1 ]
Rinaldo, Christine Hanssen [2 ]
Wernli, Marion [1 ]
Major, Eugene O. [3 ]
Hirsch, Hans H. [1 ,4 ]
机构
[1] Univ Basel, Inst Med Microbiol, Dept Biomed, CH-4003 Basel, Switzerland
[2] Univ Hosp N Norway, Dept Microbiol & Infect Control, Tromso, Norway
[3] NINDS, Nihon Univ, Bethesda, MD 20892 USA
[4] Univ Basel Hosp, CH-4031 Basel, Switzerland
关键词
PROGRESSIVE MULTIFOCAL LEUKOENCEPHALOPATHY; ACYCLIC NUCLEOSIDE PHOSPHONATES; ACTIVE ANTIRETROVIRAL THERAPY; EARLY GENE-EXPRESSION; IN-VITRO; BK REPLICATION; VIRUS MULTIPLICATION; CIDOFOVIR; CELLS; AIDS;
D O I
10.1128/AAC.00046-11
中图分类号
Q93 [微生物学];
学科分类号
071005 ; 100705 ;
摘要
Polyomavirus JC (JCV) replication causes progressive multifocal leukoencephalopathy (PML), a frequently fatal brain disease in immunodeficient patients, yet antiviral drugs are lacking. We characterized the lipid conjugate 1-O-hexadecyloxypropyl-cidofovir (CMX001) regarding JCV (Mad-4) replication in human brain progenitor-derived astrocytes (PDA) and the simian virus 40 (SV40) large-T-antigen-expressing COS-7 cells up to 7 days postinfection (dpi). We examined JCV loads by PCR, the infection rate by immunofluorescence, and host cell toxicity by WST-1 and BrdU incorporation assays. Supernatants from CMX001-treated PDA demonstrated a drug concentration-dependent decrease in JCV loads and infectivity. CMX001 had only a modest effect on host cell metabolism but reduced overall BrdU incorporation. In PDA at 7 dpi, the CMX001 50% effective concentration (EC50) was 5.55 nM, the 50% cytotoxic concentration (CC50) was 184.6 nM, and the 50% selectivity index (SI50) was 33.3. The EC90 was 19.7 nM, the CC90 was 5,054 nM, and the SI90 was 256.1. In COS-7 cells, JCV replication was faster and the EC50 and EC90 were 18-and 37-fold higher than those in PDA, i.e., 0.1 mu M and 0.74 mu M (CC50, 0.67 mu M; SI50, 6.7; CC90, 12.2 mu M; SI90, 16.5) at 5 dpi. We conclude that CMX001 inhibits JCV replication at concentrations in vitro that can be attained by oral administration without significant side effects in clinical studies.
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收藏
页码:2129 / 2136
页数:8
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