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Investigational HCV drug combo yields high SVR12 rates in compensated cirrhosis

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The next generation of HCV drugs

In phase II and III clinical trials of direct-acting antivirals (DAAs), sustained viral response (SVR) rates over 90% were achieved in most patient groups and the combinations were well tolerated, results confirmed in real-world studies. However, a number of patients remain “difficult to cure.” Among them, patients infected with genotype 3, especially those with advanced liver disease, do not respond as well as patients infected with other genotypes and often need ribavirin.
In this study, a combination of two “next- generation” drugs with potent pangenotypic antiviral activity and a high barrier to resistance was administered to patients infected with HCV genotype 1 or 3 with compensated cirrhosis. Overall, 96% of patients infected with geno­type 1 and 98% of patients infected with genotype 3 achieved SVR, with no apparent effect of ribavirin. The combination was well tolerated. Pending confirmation in phase III trials, these results suggest that pangenotypic combination regimens will be available in the very near future (approval expected in 2017) and that genotype 3 will become as easy to cure as other genotypes, while less ribavirin will be used. Unfortunately, patients with decompensated cirrhosis will not benefit from these advances, as protease inhibitors such as ABT-493 cannot be used in this population. This pangenotypic regimen may also prove particularly useful in patients with severe or end-stage kidney disease who should not receive the nucleotide analogue sofosbuvir. High SVR rates appear to be achievable when retreating patients who failed a prior DAA-based treatment with this combination, but relapses may still occur with highly resistant viruses. This next generation of HCV drugs will be the last generation. With this armamentarium, it will be technically possible to cure the vast majority of HCV-infected patients. Thus, screening and diagnosing HCV-infected patients are now mandatory in order to provide them with efficient care and make the world almost free of hepatitis C by 2030.

Jean-Michel Pawlotsky, MD, PhD, director of the National Reference Center for Viral Hepatitis B, C, and D, and professor of medicine in the department of virology, Hôpital Henri Mondor, Université Paris-Est, Créteil, France. He has received research grants from Gilead and Abbvie and has served as an adviser for Abbvie, Bristol-Myers Squibb, Gilead, Janssen, and Merck.


 

FROM GASTROENTEROLOGY

A once-daily regimen of two investigational, direct-acting anti-HCV agents, ABT-493 and ABT-530, was well tolerated and achieved sustained viral response at 12 weeks (SVR12) for nearly all patients with compensated cirrhosis and chronic genotype (GT) 1 or 3 hepatitis C virus infection, according to open-label phase II studies.

“The unique potency of these agents against all genotypes, even in the presence of common NS3 and/or NS5A baseline substitutions that confer resistance to most contemporary NS3/4A protease inhibitors and NS5A inhibitors, offers the potential for pangenotypic [HCV] therapy without ribavirin,” Edward J. Gane, MD, of the University of Auckland, New Zealand, and his associates wrote in the October issue of Gastroenterology. Phase III trials are now testing this hypothesis by focusing on cohorts of treatment-experienced, genotype 3–infected patients, on patients with renal impairment, and on patients who failed earlier-generation direct-acting antiviral regimens, they said.

Dr. Edward J. Gane

Dr. Edward J. Gane

The prevalence of HCV-related cirrhosis has yet to peak, and gold standard therapies for GT3 and GT1a infections can take weeks of treatment and the use of ribavirin, which causes undesirable side effects, the investigators noted. Attempts to surmount these residual barriers led to the development of ABT-493, an HCV nonstructural (NS) protein 3/4A protease inhibitor, and ABT-530, an HCV NS5A inhibitor. During in vitro studies, both agents showed “potent” activity against all major HCV genotypes, including variants with mutations that confer resistance to earlier, direct-acting antivirals, the researchers said (Gastroenterology. 2016 Jul 22. doi: 10.1053/j.gastro.2016.07.020). Their two open-label phase II studies enrolled adults with compensated cirrhosis and chronic GT3 (55 patients) or GT1 (27 patients) infection. Among GT1 patients, 41% had baseline NS3 substitutions conferring resistance to earlier-generation drugs, 19% had NS5A substitutions, and 11% had both mutations. The GT1-infected patients received 200 mg ABT-493 and 120 mg of ABT-530. The GT3-infected patients received 300 mg ABT-493 and 120 mg ABT-530, and half (27 patients) also received ribavirin. Most patients were treatment-naive, male, and white, with Child-Pugh scores of 5 and HCV RNA levels averaging about 6.2-6.6 log10 IU/mL.

In all, 26 patients with GT1 infection (96%) achieved SVR12 (95% confidence interval, 82% to 99%). The remaining patient relapsed after completing treatment. All treatment-naive GT3 patients achieved SVR12 whether or not they received ribavirin. However, one treatment-experienced GT3 patient who did not receive ribavirin relapsed after 16 weeks of treatment. Thus, rates of SVR12 were 96% (95% confidence interval, 82%-99%) for GT3 patients who did not receive ribavirin and 100% (95% CI, 88%-100%) for those who did. Notably, 94% of patients with baseline substitutions in NS3 and NS5A achieved SVR12, and there was no apparent link between treatment failure and any demographic or clinical characteristics, the investigators wrote.

Adverse events affected about 74% of patients and were usually mild or moderate in severity. Patients who did not receive ribavirin were most likely to report headache (15%), diarrhea (13%), and fatigue (11%). Only 4% of GT1 patients and 7% of the GT3 cohorts developed serious adverse events, and the only serious adverse event considered possibly treatment related involved a delusional disorder in a 57-year-old male who was receiving ribavirin and admitted amphetamine and alcohol use on the day it occurred. Treatment-related laboratory abnormalities were uncommon, no patients stopped treatment because of adverse events, and there were no deaths. “The rates of some adverse events were numerically higher with the higher ABT-493 dose, though the sample sizes are small and this was a cross-study comparison,” the investigators added. “Though not included in this study, patients with severe or end-stage kidney disease are predicted to be able to be treated with ABT-493 and ABT-530 because both agents have negligible renal excretion. These drugs were well tolerated in HCV-uninfected patients with renal impairment and can be administered without dose adjustment.”AbbVie funded the study and makes ABT-493 and ABT-530. Dr. Gane disclosed ties to AbbVie, Achillion Pharmaceuticals, Alnylam, Janssen, Merck, Novartis, and Novira.

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