FREQUENCY OF UL97 PHOSPHOTRANSFERASE MUTATIONS RELATED TO GANCICLOVIR RESISTANCE IN CLINICAL CYTOMEGALOVIRUS ISOLATES

被引：159

作者：

CHOU, SW

GUENTZEL, S

MICHELS, KR

MINER, RC

DREW, WL

机构：

[1] VET ADM MED CTR,RES SERV,PORTLAND,OR 97201

[2] OREGON HLTH SCI UNIV,PORTLAND,OR 97201

[3] UNIV CALIF SAN FRANCISCO,MT ZION MED CTR,DEPT CLIN MICROBIOL,SAN FRANCISCO,CA 94120

[4] UNIV CALIF SAN FRANCISCO,MT ZION MED CTR,DEPT INFECT DIS,SAN FRANCISCO,CA 94120

来源：

JOURNAL OF INFECTIOUS DISEASES | 1995年 / 172卷 / 01期

关键词：

D O I：

10.1093/infdis/172.1.239

中图分类号：

R392 [医学免疫学]; Q939.91 [免疫学];

学科分类号：

100102 ;

摘要：

Cytomegalovirus (CMV) isolates from subjects who received ganciclovir therapy were tasted for susceptibility to ganciclovir by a plaque reduction assay. Results were correlated with restriction enzyme and sequence analysis of the CMV UL97 phosphotransferase gene. Of the 30 isolates, 20 had one or more mutations in UL97 affecting amino acid encoding at codons 460, 520, or 591-596. All 20 were resistant to ganciclovir, with an IC50 of >6.0 mu M (range, 6.7-50.0). The remaining 10 isolates had no mutations at these loci; 8 were susceptible to ganciclovir while the other 2 were borderline resistant (IC(50)s, 6.6 and 7.2 mu M). None of 40 control CMV isolates from untreated subjects contained any amino acid changes at these loci. The three most common mutations at codons 460, 594, and 595 were detected by restriction digest analysis in 16 (80%) of 20 isolates and in 16 (73%) of 22 isolates with ganciclovir IC(50)s >6.0 mu M. These results indicate that the majority of ganciclovir-resistant clinical isolates contain diagnostically useful mutations in UL97.

引用

页码：239 / 242

页数：4

共 8 条

[1] ANALYSIS OF THE UL97 PHOSPHOTRANSFERASE CODING SEQUENCE IN CLINICAL CYTOMEGALOVIRUS ISOLATES AND IDENTIFICATION OF MUTATIONS CONFERRING GANCICLOVIR RESISTANCE
CHOU, SW
ERICE, A
JORDAN, MC
VERCELLOTTI, GM
MICHELS, KR
TALARICO, CL
STANAT, SC
BIRON, KK
[J]. JOURNAL OF INFECTIOUS DISEASES, 1995, 171 (03) : 576 - 583
[2] Drew W L, 1993, Clin Diagn Virol, V1, P179
[3] PREVALENCE OF RESISTANCE IN PATIENTS RECEIVING GANCICLOVIR FOR SERIOUS CYTOMEGALOVIRUS-INFECTION
DREW, WL
MINER, RC
BUSCH, DF
FOLLANSBEE, SE
GULLETT, J
MEHALKO, SG
GORDON, SM
OWEN, WF
MATTHEWS, TR
BUHLES, WC
DEARMOND, B
[J]. JOURNAL OF INFECTIOUS DISEASES, 1991, 163 (04) : 716 - 719
[4] HANSON MN, 1995, IN PRESS ANTIMICROB
[5] HUMAN CYTOMEGALOVIRUS UL97 OPEN READING FRAME ENCODES A PROTEIN THAT PHOSPHORYLATES THE ANTIVIRAL NUCLEOSIDE ANALOG GANCICLOVIR
LITTLER, E
STUART, AD
CHEE, MS
[J]. NATURE, 1992, 358 (6382) : 160 - 162
[6] MUTATION IN THE UL97 OPEN READING FRAME OF HUMAN CYTOMEGALOVIRUS STRAINS RESISTANT TO GANCICLOVIR
LURAIN, NS
SPAFFORD, LE
THOMPSON, KD
[J]. JOURNAL OF VIROLOGY, 1994, 68 (07) : 4427 - 4431
[7] GANCICLOVIR-RESISTANT CYTOMEGALOVIRUS CLINICAL ISOLATES - MODE OF RESISTANCE TO GANCICLOVIR
STANAT, SC
REARDON, JE
ERICE, A
JORDAN, MC
DREW, WL
BIRON, KK
[J]. ANTIMICROBIAL AGENTS AND CHEMOTHERAPY, 1991, 35 (11) : 2191 - 2197
[8] A PROTEIN-KINASE HOMOLOG CONTROLS PHOSPHORYLATION OF GANCICLOVIR IN HUMAN CYTOMEGALOVIRUS-INFECTED CELLS
SULLIVAN, V
TALARICO, CL
STANAT, SC
DAVIS, M
COEN, DM
BIRON, KK
[J]. NATURE, 1992, 358 (6382) : 162 - 164

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