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A combination of two oral drugs for reducing viral load in hepatitis C patients had good safety and tolerability in a small, phase I study.
The finding, published online Oct. 15 in the Lancet, points the way toward an alternative to the current standard of care – subcutaneous pegylated interferon-alfa plus oral ribavirin – which has limited tolerability and efficacy.
The novel therapies that were tested in this study are RG7128, a nucleoside polymerase inhibitor, and danoprevir, a protease inhibitor, wrote Dr. Edward J. Gane of Auckland (New Zealand) Clinical Studies Ltd., an early-phase clinical pharmacology unit, and his colleagues.
Both compounds have potent in vitro and in vivo activity against HCV, and at the time of this study, each was in phase I development, wrote the authors. Both agents are made by Roche, which funded the study and employed several of the researchers.
The study, known as INFORM-1 (Interferon-Free Regimen for the Management of HCV) was a randomized, double-blind, placebo-controlled, dose-escalation trial. Eligible patients were aged 18-65 years and had been chronically infected with HCV genotype 1, with a minimum HCV RNA of 105 IU/mL.
Patients with cirrhosis, other hepatic or renal failure, and comorbid HIV were not included in this study – a potential limitation, the authors wrote (Lancet 2010 Oct. 14 [doi:10.1016/S0140-6736(10)61384-0]).
In all, 88 patients from six centers in New Zealand and Australia were randomized into seven groups, to receive either placebo or various doses of the novel treatment. Most were white (90%), male (80%), and infected with genotype 1a (79%). The mean age was roughly 47 years.
Overall, 73 patients were ultimately given at least one dose of the assigned treatment, and 14 received placebo.
The investigators found that among patients who received the highest doses of treatment (1,000 mg RG7128 twice daily plus 900 mg of danoprevir twice daily), “five of eight treatment-naive patients and two of eight [previous] null responders [to standard HCV therapy] had HCV RNA concentrations below the limit of detection (less than 15 IU/mL),” according to the authors.
Additionally, “seven of eight treatment-naive patients and four of eight null responders had HCV RNA concentrations below the limit of quantification (43 IU/mL).”
The median reduction in HCV RNA concentrations among the treatment-naive patients was 5.1 log10 IU/mL, and among the previous null responders it was 4.9 log10 IU/mL. In comparison, the mean baseline log10 plasma HCV RNA concentration was 6.4 IU/mL.
The treatment group who received the lowest dose (500 mg RG7128 twice daily, plus 100 mg danoprevir every 8 hours) also saw a median reduction in viral load of 3.7 log10 IU/mL. Of the eight patients in this low-dose cohort, one patient achieved viral levels below the level of detection at 14 days.
“No evidence of treatment-emergent resistance to either compound was identified during the study, and 72 of 73 patients in the treatment groups had a continuous decline in viral load, which was maintained throughout dosing,” wrote the investigators.
The authors noted that they did not find many serious adverse events during treatment. There was one case of severe back pain, and one instance of severe influenzalike illness. However, many patients experienced headache, lethargy, rash, gastrointestinal disorder, and nausea.
At 14 days – the study’s completion – patients continued therapy by switching to standard of care treatment with pegylated interferon alfa-2a and ribavirin.
“The INFORM-1 study provides proof of concept for an oral approach to the treatment of HCV, in which a combination of direct-acting antiviral drugs is safely coadministered without pegylated interferon,” wrote the investigators.
The study treatment “marks a major shift in the future management of HCV infection and the biggest development in treatment of the disease” for the past 2 decades, they added.
The study was funded by Roche, which developed RG7128 and recently bought the worldwide development and commercialization rights to danoprevir from InterMune Inc. Several investigators, including Dr. Gane, have received grants, travel fees, advisory board fees, and other support from Roche and other drug makers; several are employees of Roche or InterMune and have stock options in Roche.
In an editorial accompanying the article, Dr. David L. Thomas wrote that “we are on the eve of a new era in hepatitis C virus treatment.”
Indeed, he added, for the first 2 decades after the virus was discovered, “only ribavirin and interferon-alfa–related compounds were approved for HCV treatment, and nearly a decade has passed since the last substantive upgrade.”
“The long wait for new HCV treatments is about to end,” Dr. Thomas wrote.
However, he pointed out some “important limitations” to early-phase trials such as this. For example, although the study met its safety objectives, “the goal of HCV treatment is to eradicate infection,” an end point that is achieved when HCV RNA cannot be detected in blood at the end of treatment and 6 months later.
Because patients in Dr. Gane and colleagues’ study rolled over to pegylated interferon-alfa and ribavirin after completion of study drug treatment, “the study will never tell us about the ultimate efficacy of the combined use of the two direct-acting agents.”
Moreover, “long-term risk of viral resistance with a two-drug direct-acting regimen cannot be confidently assessed, because drug use was directly observed in a clinical trial unit, and only limited resistance testing was presented.”
In any case, he argued, there is an even bigger problem with HCV treatment: “Most HCV-infected individuals are not patients. Only a small fraction of the estimated 170 million individuals with chronic hepatitis C infection know they are infected; far fewer ever start treatment.”
Even if a treatment with 100% efficacy is ultimately developed, “what is unclear at this stage is whether HCV testing and treatment will penetrate to the prisons, drug-treatment centres, and other venues where many HCV infected individuals are found and unknowingly harbour the virus,” he wrote.
“It will take both safe, effective drugs and a coordinated, well-resourced response to achieve major global impact.”
David L. Thomas, M.D., is a professor at Johns Hopkins University in Baltimore. He disclosed that he has been supplied with drugs for phase IV studies with Merck & Co. and Gilead Sciences Inc., and has received an honorarium from Merck, and payment for development of educational materials from companies who in turn receive support from drug companies.
In an editorial accompanying the article, Dr. David L. Thomas wrote that “we are on the eve of a new era in hepatitis C virus treatment.”
Indeed, he added, for the first 2 decades after the virus was discovered, “only ribavirin and interferon-alfa–related compounds were approved for HCV treatment, and nearly a decade has passed since the last substantive upgrade.”
“The long wait for new HCV treatments is about to end,” Dr. Thomas wrote.
However, he pointed out some “important limitations” to early-phase trials such as this. For example, although the study met its safety objectives, “the goal of HCV treatment is to eradicate infection,” an end point that is achieved when HCV RNA cannot be detected in blood at the end of treatment and 6 months later.
Because patients in Dr. Gane and colleagues’ study rolled over to pegylated interferon-alfa and ribavirin after completion of study drug treatment, “the study will never tell us about the ultimate efficacy of the combined use of the two direct-acting agents.”
Moreover, “long-term risk of viral resistance with a two-drug direct-acting regimen cannot be confidently assessed, because drug use was directly observed in a clinical trial unit, and only limited resistance testing was presented.”
In any case, he argued, there is an even bigger problem with HCV treatment: “Most HCV-infected individuals are not patients. Only a small fraction of the estimated 170 million individuals with chronic hepatitis C infection know they are infected; far fewer ever start treatment.”
Even if a treatment with 100% efficacy is ultimately developed, “what is unclear at this stage is whether HCV testing and treatment will penetrate to the prisons, drug-treatment centres, and other venues where many HCV infected individuals are found and unknowingly harbour the virus,” he wrote.
“It will take both safe, effective drugs and a coordinated, well-resourced response to achieve major global impact.”
David L. Thomas, M.D., is a professor at Johns Hopkins University in Baltimore. He disclosed that he has been supplied with drugs for phase IV studies with Merck & Co. and Gilead Sciences Inc., and has received an honorarium from Merck, and payment for development of educational materials from companies who in turn receive support from drug companies.
In an editorial accompanying the article, Dr. David L. Thomas wrote that “we are on the eve of a new era in hepatitis C virus treatment.”
Indeed, he added, for the first 2 decades after the virus was discovered, “only ribavirin and interferon-alfa–related compounds were approved for HCV treatment, and nearly a decade has passed since the last substantive upgrade.”
“The long wait for new HCV treatments is about to end,” Dr. Thomas wrote.
However, he pointed out some “important limitations” to early-phase trials such as this. For example, although the study met its safety objectives, “the goal of HCV treatment is to eradicate infection,” an end point that is achieved when HCV RNA cannot be detected in blood at the end of treatment and 6 months later.
Because patients in Dr. Gane and colleagues’ study rolled over to pegylated interferon-alfa and ribavirin after completion of study drug treatment, “the study will never tell us about the ultimate efficacy of the combined use of the two direct-acting agents.”
Moreover, “long-term risk of viral resistance with a two-drug direct-acting regimen cannot be confidently assessed, because drug use was directly observed in a clinical trial unit, and only limited resistance testing was presented.”
In any case, he argued, there is an even bigger problem with HCV treatment: “Most HCV-infected individuals are not patients. Only a small fraction of the estimated 170 million individuals with chronic hepatitis C infection know they are infected; far fewer ever start treatment.”
Even if a treatment with 100% efficacy is ultimately developed, “what is unclear at this stage is whether HCV testing and treatment will penetrate to the prisons, drug-treatment centres, and other venues where many HCV infected individuals are found and unknowingly harbour the virus,” he wrote.
“It will take both safe, effective drugs and a coordinated, well-resourced response to achieve major global impact.”
David L. Thomas, M.D., is a professor at Johns Hopkins University in Baltimore. He disclosed that he has been supplied with drugs for phase IV studies with Merck & Co. and Gilead Sciences Inc., and has received an honorarium from Merck, and payment for development of educational materials from companies who in turn receive support from drug companies.
A combination of two oral drugs for reducing viral load in hepatitis C patients had good safety and tolerability in a small, phase I study.
The finding, published online Oct. 15 in the Lancet, points the way toward an alternative to the current standard of care – subcutaneous pegylated interferon-alfa plus oral ribavirin – which has limited tolerability and efficacy.
The novel therapies that were tested in this study are RG7128, a nucleoside polymerase inhibitor, and danoprevir, a protease inhibitor, wrote Dr. Edward J. Gane of Auckland (New Zealand) Clinical Studies Ltd., an early-phase clinical pharmacology unit, and his colleagues.
Both compounds have potent in vitro and in vivo activity against HCV, and at the time of this study, each was in phase I development, wrote the authors. Both agents are made by Roche, which funded the study and employed several of the researchers.
The study, known as INFORM-1 (Interferon-Free Regimen for the Management of HCV) was a randomized, double-blind, placebo-controlled, dose-escalation trial. Eligible patients were aged 18-65 years and had been chronically infected with HCV genotype 1, with a minimum HCV RNA of 105 IU/mL.
Patients with cirrhosis, other hepatic or renal failure, and comorbid HIV were not included in this study – a potential limitation, the authors wrote (Lancet 2010 Oct. 14 [doi:10.1016/S0140-6736(10)61384-0]).
In all, 88 patients from six centers in New Zealand and Australia were randomized into seven groups, to receive either placebo or various doses of the novel treatment. Most were white (90%), male (80%), and infected with genotype 1a (79%). The mean age was roughly 47 years.
Overall, 73 patients were ultimately given at least one dose of the assigned treatment, and 14 received placebo.
The investigators found that among patients who received the highest doses of treatment (1,000 mg RG7128 twice daily plus 900 mg of danoprevir twice daily), “five of eight treatment-naive patients and two of eight [previous] null responders [to standard HCV therapy] had HCV RNA concentrations below the limit of detection (less than 15 IU/mL),” according to the authors.
Additionally, “seven of eight treatment-naive patients and four of eight null responders had HCV RNA concentrations below the limit of quantification (43 IU/mL).”
The median reduction in HCV RNA concentrations among the treatment-naive patients was 5.1 log10 IU/mL, and among the previous null responders it was 4.9 log10 IU/mL. In comparison, the mean baseline log10 plasma HCV RNA concentration was 6.4 IU/mL.
The treatment group who received the lowest dose (500 mg RG7128 twice daily, plus 100 mg danoprevir every 8 hours) also saw a median reduction in viral load of 3.7 log10 IU/mL. Of the eight patients in this low-dose cohort, one patient achieved viral levels below the level of detection at 14 days.
“No evidence of treatment-emergent resistance to either compound was identified during the study, and 72 of 73 patients in the treatment groups had a continuous decline in viral load, which was maintained throughout dosing,” wrote the investigators.
The authors noted that they did not find many serious adverse events during treatment. There was one case of severe back pain, and one instance of severe influenzalike illness. However, many patients experienced headache, lethargy, rash, gastrointestinal disorder, and nausea.
At 14 days – the study’s completion – patients continued therapy by switching to standard of care treatment with pegylated interferon alfa-2a and ribavirin.
“The INFORM-1 study provides proof of concept for an oral approach to the treatment of HCV, in which a combination of direct-acting antiviral drugs is safely coadministered without pegylated interferon,” wrote the investigators.
The study treatment “marks a major shift in the future management of HCV infection and the biggest development in treatment of the disease” for the past 2 decades, they added.
The study was funded by Roche, which developed RG7128 and recently bought the worldwide development and commercialization rights to danoprevir from InterMune Inc. Several investigators, including Dr. Gane, have received grants, travel fees, advisory board fees, and other support from Roche and other drug makers; several are employees of Roche or InterMune and have stock options in Roche.
A combination of two oral drugs for reducing viral load in hepatitis C patients had good safety and tolerability in a small, phase I study.
The finding, published online Oct. 15 in the Lancet, points the way toward an alternative to the current standard of care – subcutaneous pegylated interferon-alfa plus oral ribavirin – which has limited tolerability and efficacy.
The novel therapies that were tested in this study are RG7128, a nucleoside polymerase inhibitor, and danoprevir, a protease inhibitor, wrote Dr. Edward J. Gane of Auckland (New Zealand) Clinical Studies Ltd., an early-phase clinical pharmacology unit, and his colleagues.
Both compounds have potent in vitro and in vivo activity against HCV, and at the time of this study, each was in phase I development, wrote the authors. Both agents are made by Roche, which funded the study and employed several of the researchers.
The study, known as INFORM-1 (Interferon-Free Regimen for the Management of HCV) was a randomized, double-blind, placebo-controlled, dose-escalation trial. Eligible patients were aged 18-65 years and had been chronically infected with HCV genotype 1, with a minimum HCV RNA of 105 IU/mL.
Patients with cirrhosis, other hepatic or renal failure, and comorbid HIV were not included in this study – a potential limitation, the authors wrote (Lancet 2010 Oct. 14 [doi:10.1016/S0140-6736(10)61384-0]).
In all, 88 patients from six centers in New Zealand and Australia were randomized into seven groups, to receive either placebo or various doses of the novel treatment. Most were white (90%), male (80%), and infected with genotype 1a (79%). The mean age was roughly 47 years.
Overall, 73 patients were ultimately given at least one dose of the assigned treatment, and 14 received placebo.
The investigators found that among patients who received the highest doses of treatment (1,000 mg RG7128 twice daily plus 900 mg of danoprevir twice daily), “five of eight treatment-naive patients and two of eight [previous] null responders [to standard HCV therapy] had HCV RNA concentrations below the limit of detection (less than 15 IU/mL),” according to the authors.
Additionally, “seven of eight treatment-naive patients and four of eight null responders had HCV RNA concentrations below the limit of quantification (43 IU/mL).”
The median reduction in HCV RNA concentrations among the treatment-naive patients was 5.1 log10 IU/mL, and among the previous null responders it was 4.9 log10 IU/mL. In comparison, the mean baseline log10 plasma HCV RNA concentration was 6.4 IU/mL.
The treatment group who received the lowest dose (500 mg RG7128 twice daily, plus 100 mg danoprevir every 8 hours) also saw a median reduction in viral load of 3.7 log10 IU/mL. Of the eight patients in this low-dose cohort, one patient achieved viral levels below the level of detection at 14 days.
“No evidence of treatment-emergent resistance to either compound was identified during the study, and 72 of 73 patients in the treatment groups had a continuous decline in viral load, which was maintained throughout dosing,” wrote the investigators.
The authors noted that they did not find many serious adverse events during treatment. There was one case of severe back pain, and one instance of severe influenzalike illness. However, many patients experienced headache, lethargy, rash, gastrointestinal disorder, and nausea.
At 14 days – the study’s completion – patients continued therapy by switching to standard of care treatment with pegylated interferon alfa-2a and ribavirin.
“The INFORM-1 study provides proof of concept for an oral approach to the treatment of HCV, in which a combination of direct-acting antiviral drugs is safely coadministered without pegylated interferon,” wrote the investigators.
The study treatment “marks a major shift in the future management of HCV infection and the biggest development in treatment of the disease” for the past 2 decades, they added.
The study was funded by Roche, which developed RG7128 and recently bought the worldwide development and commercialization rights to danoprevir from InterMune Inc. Several investigators, including Dr. Gane, have received grants, travel fees, advisory board fees, and other support from Roche and other drug makers; several are employees of Roche or InterMune and have stock options in Roche.