Funny (not) how "real world" data takes so long to "come out"! Here is a recent publication (2018), all about "Viekirax" (ombitasvir/paritaprevir/ritonavir) and "Exviera" (dasabuvir) - also known as "OPrD" (similar to later and further formulations named Viekira Pak and then Viekira XR).

Below is not trial data but "real world" data, after Viekirax/Exviera was approved for use in Israel in Feb 2015. Between Feb 2015 and Dec 2015 the "real world" data compiled (on how well it did in that population, within that limited time period) is just being published recently!

J Viral Hepat. 2018 Feb;25(2):144-151. doi: 10.1111/jvh.12800. Epub 2017 Nov 7.

Sustained virological response to ombitasvir/paritaprevir/ritonavir and dasabuvir treatment for hepatitis C: Real-world data from a large healthcare provider.

Weil C¹, Mehta D^2,3, Koren G¹, Pinsky B², Samp JC², Chodick G^1,4, Shalev V^1,4.

Author information

Abstract

Treatment with ombitasvir/paritaprevir/ritonavir and dasabuvir, with or without ribavirin (OPrD ± RBV), was the first interferon-free direct-acting antiviral for hepatitis C virus (HCV) introduced to Israel's national basket of health services in February 2015. Patients with HCV genotype 1 (GT1) and advanced fibrosis (F3-F4) were eligible for treatment in 2015. This study aimed to characterize patients initiating OPrD ± RBV and assess sustained virological response (SVR). A retrospective cohort study was performed using the database of Maccabi Healthcare Services (MHS), a 2-million-member health plan in Israel. The study population included adults who initiated OPrD ± RBV through December 2015 per health basket criteria. A gap in medication fills (>14 days between a fill's run-out and the next fill) was used to estimate adherence. SVR was defined by the viral tests at least 12-week post-treatment. The study population consisted of 403 patients (56.3% male), with a mean age of 60.7 years (SD 11.0). Overall, 71.0% were naïve to prior HCV treatment, and 95.6% were treated with a 12-week regimen. A total of 348 patients (86.4%) completed the regimen in the usual time frame (highly adherent), whereas 8.2% completed with a gap, and 4.7% purchased less than the recommended dose. SVR rates overall and among highly adherent patients were 395/403 (98.0%; 95% CI 96.1-99.1) and 346/348 (99.4%; 95% CI 97.9-99.9), respectively. GT1b patients on 12-week regimens attained SVR rates of 194/196 (fibrosis F3) and 170/176 (cirrhosis). After a first year of provision of OPrD ± RBV with good adherence, high SVR rates were achieved in various patient subgroups and comorbidities.

PMID: 28984012   DOI:  10.1111/jvh.12800

(Continued) - "Discussion" via a Medscape article on the data presentation

Discussion

The study results indicate high rates of adherence and high SVR rates with OPrD + RBV in the first year of its provision in the Israeli health basket, among HCV patients in a large health plan. The SVR-12 rate in the present study population of 403 patients was 98.0% (95% CI: 96.1-99.1). These results are consistent with the SVR rates found in the clinical trials,^[10,11] as well as recently published real-world data. A meta-analysis of 5726 patients treated in several countries reported an SVR-12 rate of 97%,^[12] and early evidence of OPrD + RBV use in Poland indicated a rate of 207/209 (99.0%), ranging from 96.4% to 100.0% across subgroups.^[13] 

In line with these findings, results from an early US Veterans Affairs study indicate SVR rates of 98.0% (248/253) and 95.5% (705/738) with 12 weeks of OPrD without or with RBV, respectively.^[14]

Cirrhotic patients in our study population had very high rates of SVR-12, similar rate to noncirrhotic patients, which supports currently available real-world data.^[12] As shown previously, SVR-12 can be attained in GT1b patients with compensated cirrhosis and early HCC that has been eradicated.^[23] In our study, all 5 patients with a definite history of HCC achieved SVR-12. In this population, OPrD is contraindicated for patients with moderate and severe hepatic impairment (for Child-Pugh B, treatment was not recommended and then contraindicated following the FDA safety warning in October 2015). Although data were not readily available to confirm Child-Pugh A in all the early OPrD users in this study, upon review of gastroenterologists' summaries in the medication approval records of 50 randomly sampled patients with an ICD-9 code for cirrhosis, we found confirmation of Child-Pugh A in 76% of cases, with no mention of Child-Pugh or decompensation in the remaining records.

Studies suggest that HCV infection may be associated with a more rapid decline in renal function^[24,25] and increased risk of CKD,^[26,27] and more studies are needed to show that clearance of HCV can improve outcomes in CKD patients. Clinical trial results have demonstrated high SVR-12 rates with OPrD + RBV among GT1 patients with advanced CKD (stages 4-5).^[28] This real-world study suggests that high SVR rates can be achieved among CKD patients. More information is needed on the subpopulation with advanced stages of CKD, and this should be confirmed in larger studies and with different stages. While concomitant medications that increase gastric pH can alter the bioavailability of antiviral drugs, data from Phase 3 trials indicate that HCV-GT1 patients who use acid-reducing agents or proton pump inhibitors attained high SVR-12 rates with OBV/PTV/r+DSV and RBV in clinical trial setting.^[29] Our data are consistent with this trend, where 108/110 of our patients receiving acid-reducing or proton pump inhibitors achieved SVR-12.

Given the challenges to adherence in real-world settings, the results of the present early study are encouraging, demonstrating high rates of adherence and SVR in different HCV patient subgroups, including patients with advanced fibrosis combined with chronic comorbidities. These results stand in contrast to our previous study of interferon-based therapy for HCV in the same healthcare setting, which showed substantially lower adherence and SVR rates.^[30]

Studies of interferon-based therapy have demonstrated that failure to achieve SVR is strongly associated with nonadherence,^[30] often due to lack of treatment effect or occurrence of adverse events.^[6] Failure to reach SVR-12 with OPrD in our study could potentially also be related to a lower actual consumption of dispensed medication (ie missed doses), or to potential resistance to DAAs.^[31]

The health plan members have similar demographics to the general population of Israel, and the results can therefore be generalizable to the national level.^[32] By establishing an open cohort in the second largest Israeli health plan, real-world evidence will continue to be updated in future studies to monitor a growing cohort and assess the long-term effectiveness and safety of OPrD + RBV. In the present analyses, 1% of patients had a record of on-treatment decompensation and nonetheless achieved SVR-12. Early real-world data suggest that 2%-5.4% of patients experience a serious adverse event, while less than 3% discontinue due to an adverse event.^[12] Future studies can utilize MHS' comprehensive databases to investigate adverse events and assess broader outcomes such as healthcare resource utilization. Treated patients will continue to be monitored for long-term outcomes, such as liver progression or regression.

In summary, this large early real-world cohort of HCV GT1 patients with advanced fibrosis treated with the new regimen of OPrD + RBV showed high efficacy on par with that in the clinical trials. After the first year of its provision in the Israeli health basket, high rates of adherence and SVR were achieved. The high effectiveness of this new regimen was independent of patient characteristics and underscores the potential for improving outcomes of HCV patients in a new era of HCV treatment.