The Hepatitis B Virus Ribonuclease H Is Sensitive to Inhibitors of the Human Immunodeficiency Virus Ribonuclease H and Integrase Enzymes

A Agrawal; A Monto; Aleem Siddiqui; AM Woltman; B Werle-Lapostolle; C Chang; CA Shaw-Reid; CS Coffin; CW Shepard; D Ganem; D Lavanchy; DK Wong; DM Himmel; DM Himmel; E Michailidis; E. Jon Jacobsen; Eleftherios Michailidis; ER Goedken; F Cao; F Dyda; F Kurbanov; F van Bommel; F Zoulim; F Zoulim; F Zoulim; Feng Cao; G Radziwill; G Radziwill; G Woo; GJ Klarmann; GK Lau; GM Di; GR Foster; H Fuji; H Kwon; H Pelletier; H Wang; HP Su; HR Bokesch; J Beck; J Cheng; J Choi; J Didierjean; J Hu; J Hu; J Wu; J zu Putlitz; JE Tavis; JE Tavis; JJ Arnold; JJ Song; JL Keck; John E. Tavis; JS Tuttleman; JT Edward; K Katayanagi; K Klumpp; K Klumpp; K Takada; K Wursthorn; L Lin; LJ Chang; M Ariyoshi; M Billamboz; M Billamboz; M Buti; M Chen; M Ghany; M Levrero; M Nowotny; M Nowotny; M Ruggeri; M Sturmer; M Wendeler; M Wu; Marvin J. Meyers; MD Li; Michael A. Parniak; Michael Totten; ML Op den Brouw; MT Chen; N Cox; N Potenza; O Poch; P Frank; P Frank; P Marcellin; P Vanlandschoot; PA Rice; PD Williams; PN Cheng; Q Gong; Rajeev Aurora; RP Perrillo; S Chung; S Chung; SR Budihas; Stefan G. Sarafianos; T Gerelsaikhan; TA Kirschberg; V Suchaud; W Yang; WF Lima; WF Lima; X Wei; Xiaohong Cheng; Y Chen; Y Gong; Y Wei; Y Xu; YF Liaw; YI Lee; Yuan Hu

research

The Hepatitis B Virus Ribonuclease H Is Sensitive to Inhibitors of the Human Immunodeficiency Virus Ribonuclease H and Integrase Enzymes

Authors: A Agrawal
A Monto
Aleem Siddiqui
AM Woltman
B Werle-Lapostolle
C Chang
CA Shaw-Reid
CS Coffin
CW Shepard
D Ganem
D Lavanchy
DK Wong
DM Himmel
DM Himmel
E Michailidis
E. Jon Jacobsen
Eleftherios Michailidis
ER Goedken
F Cao
F Dyda
F Kurbanov
F van Bommel
F Zoulim
F Zoulim
F Zoulim
Feng Cao
G Radziwill
G Radziwill
G Woo
GJ Klarmann
GK Lau
GM Di
GR Foster
H Fuji
H Kwon
H Pelletier
H Wang
HP Su
HR Bokesch
J Beck
J Cheng
J Choi
J Didierjean
J Hu
J Hu
J Wu
J zu Putlitz
JE Tavis
JE Tavis
JJ Arnold
JJ Song
JL Keck
John E. Tavis
JS Tuttleman
JT Edward
K Katayanagi
K Klumpp
K Klumpp
K Takada
K Wursthorn
L Lin
LJ Chang
M Ariyoshi
M Billamboz
M Billamboz
M Buti
M Chen
M Ghany
M Levrero
M Nowotny
M Nowotny
M Ruggeri
M Sturmer
M Wendeler
M Wu
Marvin J. Meyers
MD Li
Michael A. Parniak
Michael Totten
ML Op den Brouw
MT Chen
N Cox
N Potenza
O Poch
P Frank
P Frank
P Marcellin
P Vanlandschoot
PA Rice
PD Williams
PN Cheng
Q Gong
Rajeev Aurora
RP Perrillo
S Chung
S Chung
SR Budihas
Stefan G. Sarafianos
T Gerelsaikhan
TA Kirschberg
V Suchaud
W Yang
WF Lima
WF Lima
X Wei
Xiaohong Cheng
Y Chen
Y Gong
Y Wei
Y Xu
YF Liaw
YI Lee
Yuan Hu
Publication date: 1 January 2013
Publisher: 'Public Library of Science (PLoS)'
Doi

Abstract

Nucleos(t)ide analog therapy blocks DNA synthesis by the hepatitis B virus (HBV) reverse transcriptase and can control the infection, but treatment is life-long and has high costs and unpredictable long-term side effects. The profound suppression of HBV by the nucleos(t)ide analogs and their ability to cure some patients indicates that they can push HBV to the brink of extinction. Consequently, more patients could be cured by suppressing HBV replication further using a new drug in combination with the nucleos(t)ide analogs. The HBV ribonuclease H (RNAseH) is a logical drug target because it is the second of only two viral enzymes that are essential for viral replication, but it has not been exploited, primarily because it is very difficult to produce active enzyme. To address this difficulty, we expressed HBV genotype D and H RNAseHs in E. coli and enriched the enzymes by nickel-affinity chromatography. HBV RNAseH activity in the enriched lysates was characterized in preparation for drug screening. Twenty-one candidate HBV RNAseH inhibitors were identified using chemical structure-activity analyses based on inhibitors of the HIV RNAseH and integrase. Twelve anti-RNAseH and anti-integrase compounds inhibited the HBV RNAseH at 10 μM, the best compounds had low micromolar IC50 values against the RNAseH, and one compound inhibited HBV replication in tissue culture at 10 μM. Recombinant HBV genotype D RNAseH was more sensitive to inhibition than genotype H. This study demonstrates that recombinant HBV RNAseH suitable for low-throughput antiviral drug screening has been produced. The high percentage of compounds developed against the HIV RNAseH and integrase that were active against the HBV RNAseH indicates that the extensive drug design efforts against these HIV enzymes can guide anti-HBV RNAseH drug discovery. Finally, differential inhibition of HBV genotype D and H RNAseHs indicates that viral genetic variability will be a factor during drug development. © 2013 Tavis et al