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 HIV and Hepatitis.com Coverage of the
49th Interscience Conference on Antimicrobial Agents and Chemotherapy (ICAAC 2009)
September 12-15, 2009, San Francisco, CA
 The material posted on HIV and Hepatitis.com about the 49th ICAAC is not approved by the American Society for Microbiology
Experimental Agent ATI-0810 Appears to Have Novel Mechanism of Action against Hepatitis C Virus

A set of investigational small molecule inhibitors of hepatitis C virus (HCV) replication, including ATI-0810, work by a novel mechanism and appear to have different resistance profiles than other anti-HCV therapies, according to a poster presented at the 49th Interscience Conference on Antimicrobial Agents and Chemotherapy (ICAAC 2009) this week in San Francisco.

By Liz Highleyman

As background, researchers from ImQuest Biosciences noted that the experimental agents have antiviral activity that results in a significant reduction of viral RNA synthesis not related to known mechanisms including inhibition of viral entry into cells, initiation of IRES translation, inhibition of the HCV NS2/3 or NS3/4A HCV protease enzyme, or interference with the HCV NS5B viral RNA-dependent RNA polymerase.

In previous laboratory studies, ATI-0810 was 100- to 200-fold less toxic than ribavirin, and in fact appeared to reduce the toxicity of ribavirin when the drugs were administered together. ATI-0810 was shown to be non-toxic to fresh human hepatocytes (liver cells) at the highest concentration tested (1.33 mM). Furthermore, serial passage of cells infected with a virus related to HCV (bovine viral diarrhea virus) in the presence of escalating doses of ATI-0810 failed to select for drug-resistant virus, suggesting a high genetic barrier to resistance.

In the present study, an HCV replicon system was used to analyze the activity of ATI-0810 and 10 chemically related compounds (PG204057, PG702253, PG702273, PG702306, PG702307, PG702379, PG702532, PG702548, PG702617, and PG703010), and to generate ATI-0810 resistant HCV replicons. The investigators examined cellular gene expression in the presence and absence of ATI-0810.

Results

In vitro antiviral activity of ATI-0810 and the related compounds ranged from 0.21 to 3.4 mcM.
Selection of ATI-0810 resistant replicons revealed potential resistance-conferring mutations in the HCV NS3 and NS5A enzymes.
A single NS5A mutation, C446R, conferred a 21-fold decrease in sensitivity to ATI-0810.
This mutation is the P2 proximal amino acid at the NS5A/NS5B junction.
Sensitivity testing of ATI-0810 in replicons cells expanded after selection for this mutation revealed an approximately 17- to 20-fold increase in the drug's EC50 value (50% effective concentration).
The C446R mutation and 3 others -- NS3 D168N, NS5A L199F, and V296 -- emerged in replicons cultured with ATI-0810, but not those grown without the agent.
Differential gene expression revealed no significant changes in cellular RNA accumulation in the presence of ATI-0810.

Based on these data, the researchers hypothesized that ATI-0810 inhibits HCV replication through a novel mechanism of action.

"ATI-0810 does not inhibit viral protease or polymerase activity and does not appear to inhibit IRES-mediated translation or NS2 protease activity," they stated.

They added that in tests combining ATI-0810 with other anti-HCV agents, the new agent "reduces the toxicity of ribavirin and interferon and is additive with interferon and additive/slightly synergistic with ribavirin."

ImQuest BioSci., Frederick, MD.

9/15/09

Reference
TB Parsley, l Yang, and RW Buckheit. ATI-0810 is a Novel Late Stage Inhibitor of HCV Replicon Replication. 49th Interscience Conference on Antimicrobial Agents and Chemotherapy (ICAAC 2009). San Francisco. September 12-15, 2009. Abstract H-215.


 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 



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