A real-life study of the positive response to DAA-based therapies for hepatitis C in Brazil

Vivaldini, Simone Monzani; Ribeiro, Rachel Abraão; Mosimann Júnior, Gláucio; Tonini, Karen Cristine; Pereira, Gerson Fernando Mendes; Araújo, Wildo Navegantes de

doi:10.1016/j.bjid.2021.101573

ABSTRACT

A retrospective cohort of 11,308 chronic hepatitis C infected patients treated with regimens that included Sofosbuvir (SOF), Daclatasvir (DCV), Simeprevir (SMV), or an association of Ombitasvir, Veruprevir/Ritonavir and Dasabuvir (3D) with or without Ribavirin (RBV) were assessed for sustained virologic response (SVR) or viral cure after a 12-week treatment. Logistic regression analyses were used to identify factors independently associated with positive response to direct-acting antivirals (DAA)-based therapies.Overall 57.1% were male; 48.3% self-identified as white; 78.3% were over 50 years old; 44.1% were from the Southeast region; 47.7% had genotype 1b; and 84.5% were treated for 12 weeks. The SVR rates with DAAs ranged from 87% to 100%. Genotypes 1 and 4 had higher SVR rates (96.3–100%), and genotypes 2 and 3 had SVR of 90.6–92.2%, respectively. Treatment durations of 12 and 24 weeks were associated with an average SVR of 95.0% and 95.9%, respectively. Females were half as likely (OR 0.5; 95% CI 0.4−0.6) to have a negative response to therapy compared to males, and those with genotypes 2 and 3 were one and half fold more likely (OR 1.5–2.2; 95 CI% 0.7–2.9; 1.2–3.6 and OR 2.7–2.8; 95% CI 2.0–3.8, respectively) to not have SVR compared to genotype 1. Patients in the age-range of 50–69 years old were 1.2-fold (OR 1.2; 95% CI 0.7–1.9) more likely to not have SVR compared to other age groups, although not statistically significant.This study is the first of this magnitude to be held in a Latin-American country with high SVR results, supported by a free-of-charge universal and public health system. The high performance found in this study gives support to the Brazilian public health policy decision of adopting DAA-based therapies as a strategy to eliminate HCV by 2030.

Keywords:
Hepatitis C; Treatment; Direct-acting antivirals; Health policy

Introduction

Globally, in 2016 there were an estimated 71 million people with chronic hepatitis C virus (HCV) infection and only a small minority were able to access curative treatment.¹1 World Health Organization, Available: http://apps.who.int/iris/bitstream/handle/10665/255016/9789241565455-eng.pdf?sequence=1, 2017.
http://apps.who.int/iris/bitstream/handl... ^,²2 Blach S, Zeuzem S, Manns M, Altraif I, Duberg AS, Muljono DH, et al. Global prevalence and genotype distribution of hepatitis C virus infection in 2015: a modelling study. Lancet Gastroenterol Hepatol. 2017;2:161-76. Due to the substantial impact of HCV infection on patients, their families, public health systems, and the World Health Organization (WHO) has set HCV elimination goals that include reduction of HCV incidence by 80% and HCV-related mortality by 65% before 2030.¹1 World Health Organization, Available: http://apps.who.int/iris/bitstream/handle/10665/255016/9789241565455-eng.pdf?sequence=1, 2017.
http://apps.who.int/iris/bitstream/handl... ^,³3 World Health Organization, Available: https://www.who.int/hepatitis/publications/hep-c-access-report-2018/en/, 2018.
https://www.who.int/hepatitis/publicatio... As part of the strategy to achieve these goals, WHO included all-oral, interferon-free, direct-acting antiviral (DAA) regimens in the 2017 edition of the treatment guidelines.¹1 World Health Organization, Available: http://apps.who.int/iris/bitstream/handle/10665/255016/9789241565455-eng.pdf?sequence=1, 2017.
http://apps.who.int/iris/bitstream/handl... ^,³3 World Health Organization, Available: https://www.who.int/hepatitis/publications/hep-c-access-report-2018/en/, 2018.
https://www.who.int/hepatitis/publicatio... ^,⁴4 Spearman CW, Dusheiko GM, Hellard M, Sonderup M. Hepatitis C. Lancet. 2019;394:1451-66.

About 632,000 people in Brazil are infected with HCV, with seroprevalence of 0.70% in the population aged between 15 and 69 years.⁵5 Benzaken AS, Girade R, Catapan E, Pereira GFM, de Almeida EC, Vivaldini S, et al. Hepatitis C disease burden and strategies for elimination by 2030 in Brazil. A mathematical modeling approach. Braz J Infect Dis. 2019;23:182-90. Most HCV-infected people are unaware of their status until the virus has caused serious liver damage.³3 World Health Organization, Available: https://www.who.int/hepatitis/publications/hep-c-access-report-2018/en/, 2018.
https://www.who.int/hepatitis/publicatio... ^,⁵5 Benzaken AS, Girade R, Catapan E, Pereira GFM, de Almeida EC, Vivaldini S, et al. Hepatitis C disease burden and strategies for elimination by 2030 in Brazil. A mathematical modeling approach. Braz J Infect Dis. 2019;23:182-90.^,⁶6 Brasil. Ministério da Saúde, Protocolo Clínico e Diretrizes Terapêuticas para Hepatite C e Coinfecções. Brasília, 2011. The introduction of DAAs in 2015 has changed the landscape of treatment and its associated outcomes in the Brazilian Unified National Health System (SUS).⁷7 Ministério da Saúde-Brasil, Available: Protocolo Clínico e Diretrizes Terapêuticas para Hepatite C e Coinfecções; 2015. p. 1–98 http://bvsms.saude.gov.br/bvs/publicacoes/protocolo_clinicodiretrizeshepatite_co_coinfeccoes.pdf
http://bvsms.saude.gov.br/bvs/publicacoe... Despite the high potency of DAAs, their high cost initially represented a serious barrier, leading to the rationing of HCV treatment for patients with high risk of disease progression and development of complications.⁶6 Brasil. Ministério da Saúde, Protocolo Clínico e Diretrizes Terapêuticas para Hepatite C e Coinfecções. Brasília, 2011.^,⁸8 Id WL, Lin Y, Chang C, Chang C. Impact of direct-acting antiviral therapy for hepatitis C – related hepatocellular carcinoma. PLoS One J. 2020;:80-90.^–¹¹11 Juanbeltz R, Martínez-Baz I, San Miguel R, Goñi-Esarte S, Cabasés JM, Castilla J. Impact of successful treatment with directacting antiviral agents on health-related quality of life in chronic hepatitis C patients. PLoS One. 2018;13:1-15. However, today all Brazilian patients have access to these therapies.

Brazil’s National Treatment Guidelines for HCV was launched in 2015, elaborated by the Brazilian Ministry of Health (MoH-Brazil), and adopted by SUS.⁷7 Ministério da Saúde-Brasil, Available: Protocolo Clínico e Diretrizes Terapêuticas para Hepatite C e Coinfecções; 2015. p. 1–98 http://bvsms.saude.gov.br/bvs/publicacoes/protocolo_clinicodiretrizeshepatite_co_coinfeccoes.pdf
http://bvsms.saude.gov.br/bvs/publicacoe... In 2018, the MoH-Brazil took a step forward to supporting the development and implementation of national multi-sector policies and strategies for hepatitis prevention and control in Brazil, for all HCV-infected patients, regardless of the degree of liver fibrosis.¹²12 Roche B, Coilly A, Duclos-Vallee JC, Samuel D. The impact of treatment of hepatitis C with DAAs on the occurrence of HCC. Liver Int. 2018;38:139-45. Since many countries are working on action plans to address HCV, different methodologies, processes, and ways to move forward have been identified. Therefore, the analysis and comparison of Brazil’s policies may offer an opportunity to accelerate the development and implementation of new national plans.¹³13 Ministério da Saúde. B, Brasília Protocolo Clínico E Diretrizes Terapêuticas Para Hepatite C e Coinfecções; 2018. SUS supported the annual cost per capita of US$ 6,152.85 on average for DAA-based therapies from 2015 to 2018.¹⁴14 Brasil. Ministério da Saúde, Available: www.aids.gov.br, 2018.
www.aids.gov.br... The MOH has developed a mathematical model to better understand the national prevalence data and establish its own elimination goals, including an estimation of the number of people to be treated.⁵5 Benzaken AS, Girade R, Catapan E, Pereira GFM, de Almeida EC, Vivaldini S, et al. Hepatitis C disease burden and strategies for elimination by 2030 in Brazil. A mathematical modeling approach. Braz J Infect Dis. 2019;23:182-90.^,¹⁵15 Castelo A, Brandão Mello CE, Teixeira R, Madruga JVR, Reuter T, Pereira LMMB, et al. Hepatitis C in the Brazilian public health care system: burden of disease. Arq Gastroenterol. 2018;55:329-37.

The purpose of this study was to determine the impact of DAA regimens within all 27 Brazilian states and to identify the factors associated with SVR.

Materials and methods

A retrospective cohort study was conducted using different national databases of the Brazilian Public Health System, including diagnostic information system (GAL), hospital information system (SIH), and treatment information system (HORUS). The sample for this study included people with acute or chronic hepatitis C. They were part of the first groups treated at the SUS network with therapeutic regimens which sometimes included Ribavirin (RBV) ]but, in most cases, consisted of only direct-acting antivirals: Sofosbuvir (SOF), Daclatasvir (DCV), Simeprevir (SMV) or Ombitasvir/Veruprevir/Ritonavir + Dasabuvir (3D). These drugs were used in different therapeutic combinations: SOF + DCV ± RBV; SOF + SMV ± RBV; SOF + RBV; 3D ± RBV; SOF + PEG + RBV.

To obtain the final database with the selected population, two steps were developed. The first step consisted of identifying a probabilistic relationship among the following databases: (i) Laboratory Environment Management System (GAL) – which contains data from the Central Laboratories of Public Health (LACEN); (ii) Ambulatory Information System (SIA/SUS) – which includes records from the High Complexity Procedures Authorization (APAC) database; and (iii) Individual Outpatient Production Bulletins (BPAI) – which contain information recorded by states concerning requests and delivery of medication. From this relationship, a unique numeric code (ID) was attributed to each patient and this code was replicated in the different databases to allow the connection of the information taken from different sources. Later, patients’ personal data were suppressed to maintain anonymity. This step was developed by the SUS Department of Information Technology (DATASUS) through a project called “VinculaSUS”,¹⁶16 Departamento de Informática do SUS/DATASUS-Ministério da Saúde [cited 8 Jun 2020]. Available: http://datasus1.saude.gov.br/noticias/atualizacoes/1167-datasus-demas-e-hospital-albert-einstein-promovem-workshop-vinculasus, 2020.
http://datasus1.saude.gov.br/noticias/at... whose objective is to facilitate researchers’ analyses of policies developed by the Brazilian MOH while maintaining ethical commitments and the confidentiality of personal data.

The second step consisted of selecting patients with at least one viral load measurement by quantitative real-time qPCR-HCV test from the GAL database and some record of treatment for HCV in the SIA/SUS database, filtering patients who had detectable qPCR-HCV following 12 weeks of treatment and assessing how many of these patients presented SVR to HCV. Fig. 1 details the procedures and quantifies the results of the first and second steps.

Fig. 1
Relationship information from the databases used and final identification of 11,308 patients with post-treatment investigation (quantitative qPCR-HCV test).

From the final database, descriptive analyses were performed with the objective of understanding the studied population and the procedures of interest that were adopted. All available sociodemographic, clinical, and laboratory variables were analyzed: sex, age, race/color, place of residence, genotype, time of treatment, therapeutic scheme, start and end date of treatment, date of laboratory tests, and respective results of qPCR-HCV tests. Trend and dispersion measures were used for numerical variables, and rates or proportions were utilized for categorical variables.

Patients were spatially distributed into three groups: 1) those registered in the APAC database who had at least one exam registered in the GAL database; 2) those registered in the APAC database who had at least one exam 12 weeks after the end of treatment registered in GAL; and 3) those registered in the APAC database who had at least one exam 12 weeks after the end of the treatment registered in GAL and who had reached SVR.

Some criteria were used to make the analyzed groups more homogeneous and to promote greater internal validity: analyses separated by genotypes; evaluation of therapeutic schemes; treatment time; and results of qPCR-HCV tests evaluated after 12 weeks of treatment completion. We compared the proportions to assess whether the results were statistically significant. Pearson's chi-squared test was applied with a significance level of α = 5%. We used the odds ratio (OR) and confidence interval (CI) of 95% to identify the factors associated with SVR.

A univariate analysis was conducted to assess the relationships between positive and negative responses to therapy and the available sociodemographic data. For the multivariate analysis, we used the variables that presented a p-value <0.2 in the bivariate analysis. We identified collinearity in two variables using a correlation matrix, and variables that presented R² > 0.5 were selected. Three different models were evaluated through the Akaike Information Criterion (AIC), and a multivariate model of logistic regression was defined to determine the independent association between SVR responses to therapy (cure vs no cure). These responses were defined by the results of the qPCR-HCV test as undetectable (SVR) or detectable (not SVR).

All statistical analyses were conducted using SPSS 20.0 for Windows, with a significance level of 0.05 (Table 2). Statistical analyses and graphical representations were performed using the IBM-PASW Statistics version 18 and Microsoft Excel^® 2013 programs. Analysis and maps were developed utilizing RStudio, a free software program for an integrated development environment for R, version 1.2.5019-6.¹⁷17 R Foundation for Statistical, Viena/Autria Available: https://www.r-project.org/, 2015.
https://www.r-project.org/...

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Table 1
Sociodemographic, clinical, and laboratory characteristics of patients who underwent hepatitis C treatment, from October 2015 to July 2018 in Brazil.

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Table 2
Demographic, clinical, and laboratory characteristics of patients, and factors associated with SVR, bivariate and multivariate analyzes.

As mentioned before, this study utilized a historical database, and participants' names and personal information were kept confidential by substituting these data for an identification number (ID). As a result, the National Committee for Ethics in Research (CONEP) waived the requirement to obtain patients' informed written consent and approved the research, which is registered in Brazil under number 2,872,543.

Results

The SUS Department of Information Technology (DATASUS), through a project called VinculaSUS,¹⁸18 Im GY, Dieterich DT. Direct-acting antiviral agents in patients with hepatitis C cirrhosis. Gastroenterol Hepatol. 2012;8. worked on establishing a relationship among the various Ministry of Health’s databases by providing a numeric identification key (ID) which enables locating patients in these various information systems and facilitates researchers’ analyses of policies adopted by the MoH-Brazil, while maintaining ethical commitments and the confidentiality of personal data. From this relationship, a unique numeric code (ID) was attributed to each patient and this code was replicated in the different databases to allow connecting the information taken from different sources.

During the analyzed period, five million ambulatory procedures were recorded in the SIA/SUS databases, including 30,423 patients treated for hepatitis C, of which 19,100 patients were registered with laboratory tests related to hepatitis C in the GAL database. Only 11,308 of these patients had a viral load test performed 12 weeks after the end of treatment, allowing the assessment of SVR and confirming the cure of hepatitis C. Of these 11,308 patients, 10,758 had a sustained virologic response and 550 individuals continued to present detectable qPCR-HCV following treatment (Fig. 1).

The states of the North, Northeast and Southeast regions presented the same proportion of cases (about 30%) in the three groups of patients mentioned above (p-value > 0.05). The other states showed significant differences among the three groups (p-value < 0.05). This was due to the high concentration of patients in the first group from the Southeast region, primarily from the state of São Paulo, which represented 21.3% of the total number of patients. Although the other two groups represent the majority of cases in the Southeast region, the final analyzed group showed a higher concentration of treatments for the states along the South-Southeast axis, translating into a more heterogeneous group.

Georeferencing of the treated and cured cases was carried out and can be seen in Fig. 2, which shows the concentration of treatments in the South and Southeastern states.

Fig. 2
Georeferencing of cases according to patients treated for hepatitis C, and patients who achieved viral cure, Brazil, 2015 to 2018.

Among the evaluated patients (n = 11,308), 6459 (57.1%) were male, 4,847 (42.9%) self-identified as white, 13,046 (65.8%) were between 50 and 69 years of age at the beginning of treatment, 8,686 (43.8%) lived in the Southeast region of the country, 4,983 (44.1%) had genotype 1b, 9494 (84.0%), and 1810 (16.0%) underwent treatment for 12 weeks and 24 weeks, respectively. More details are available in Table 1.

Among those with undetectable qPCR-HCV at the end of treatment (SVR), 6060 (56.3%) were male; 5179 (48.1%) identified as white; 3759 (34.9%) had initiated treatment at the age range of 50–59 years; 4777 (44.4%) lived in the Southeast region; 5215 (48.15%) carried genotype 1b; and 9075 (84,3%) and 1681 (15,7%) underwent treatment for 12 weeks and 24 weeks, respectively. Treatment regimens for each of the different genotypes identified in the study were compared. Genotypes 1 (without subtype results), 1a, 1b, 2, 3, 4 and some mixed genotypes were present in the analyses. The average rate of SVR with the use of DAAs was 95.0% and 95.9% for 12 and 24 weeks after treatment, respectively (Table 2).

In the odds ratio (OR) assessment, we verified that females are half as likely to have a negative response to therapy when compared to males (Table 2). In relation to the variable race/color, the rates did not present significantly different values for DAA-based therapies, with positive responses between 94.8 and 100%. The age group variable presented positive responses to treatment, varying from 94.7% to 100%; however, the p-value indicated no significant differences among the groups (Table 2).

The positive response rate for the five Brazilian regions ranged from 94.0 to 96.7%, being significantly better in the Center-West and Southeast with an OR of 0.5 and 0.7, respectively (p < 0,05). SVR proportion ranged from 90.6% (genotype 3) to 100% (genotype 1). Some patients (12) were classified as infected by two different genotypes (mixed genotypes) and the SVR proportion was 100%. Patients with genotypes 2 and 3 obtained the lowest SVR proportion: 92.2% and 90.6%, respectively. When results were assessed according to genotypes, patients with genotypes 2 and 3 were 1.5 and 2.8 more likely to not have SVR, respectively, when compared to genotype 1a and 1b (Table 2). These results were confirmed by the bivariate and multivariate analyses (Table 2).

The treatment of genotype 1a and 1b reached results of 96.3 and 96.7%, respectively. For 56 patients with genotype 1, there were no records of the subgenotype (1a and 1b). These patients had a 100% positive response rate to therapy (Table 2).

The least efficient regimen was SOF + SMV, with an OR of 1.4. We found no differences between treatment time of 12 and 24 weeks (Table 2). When observing the data by therapeutic scheme, the results of SVR after 12 weeks of DAA-based treatment ranged from 92.2% (Sofosbuvir + RBV) to 100% (3D + Ribavirin) (Table 2).

Bivariate and multivariate analyses showed that genotypes 1a and 1b presented significantly different results when compared to others, responding better to therapeutic schemes. Genotypes 2 and 3, on the other hand, responded less to treatments when compared to genotype 1a and 1b. Genotype 4 had an SVR of 97.6%, but presented no significant difference due to the small number of cases. In the evaluation, it was observed that the SOF + RBV scheme had a significantly lower response to HCV (SVR 92.2%; OR 1.6; IC 95% 1,1–2.5) along with PEG + RBV (SVR 72.4%; OR 7.4; CI 5.1–10.8). We also verified that the SOF + DCV + RBV scheme yielded a higher response than the other antivirals (SVR 96%; OR 0.8; CI 0.6–1.0). The SVR of 3D + RBV was 100% (Table 2b).

Table 3 shows the SVR rates according to the various therapeutic regimens and genotypes (1, 1a, 1b, 2, 3, and 4).

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Table 3
HCV qPCR results following 12 weeks of treatment for hepatitis C for 11,308 patients in Brazil, according to the therapeutic scheme and patients' genotype.

When the results of treatments for each genotype were analyzed, we confirmed that the best SVR rates were reached by using SOF + DAC (±) RBV therapeutic regimens. The same was true for patients carrying genotypes 1a and 1b, whose SVR rates ranged from 96.5 to 97.7% (IC 95–98.2%).

Discussion

A total of 11,308 patients had a viral load test performed 12 weeks after the end of treatment. The average rate of SVR with the use of DAAs was 95.0% and 95.9% for 12 and 24 weeks after treatment, respectively. It is important to highlight that the study cohort had a large number of patients with advanced fibrosis, cirrhosis, which is consistent with the treatment protocol used from 2015 to 2018. The rates of SVR were very satisfactory, demonstrating that the treatment reached a high cure rate with an average of 95.5% with DAA incorporated into SUS (87–100%), being the largest study carried out to date in Latin America. Similar data were found in other studies.⁹9 Gallach M, Vergara M, da Costa JP, Miquel M, Casas M, Sanchez-Delgado J, et al. Impact of treatment with direct-acting antivirals on anxiety and depression in chronic hepatitis C. PLoS One. 2018;13:1-15.^,¹⁸18 Im GY, Dieterich DT. Direct-acting antiviral agents in patients with hepatitis C cirrhosis. Gastroenterol Hepatol. 2012;8.^,¹⁹19 Daniel KE, Saeian K, Rizvi S. Real-world experiences with direct-acting antiviral agents for chronic hepatitis C treatment. J Viral Hepat. 2020;27:195-204.

Treatment schemes in each of the different genotypes identified in the study were evaluated to compare whether the different responses were statistically significant. Among those with sustained virologic responses (SVR), 56.3% were male; 48.1% identified as white; 34.9% had initiated treatment between 50–59 years of age; 44.4% lived in the Southeast region; 48.15% carried genotype 1b; and 85.5% underwent treatment for 12 weeks. Genotypes 1 (without subtype results) 1a, 1b, 2, 3, 4 and some mixed genotypes were present in the analyses. Patients with genotypes 1a and 1b showed better cure rates than others (Table 2). We also verified that treatments utilizing DAA-based, such as 3D + RBV; SOFO + DCV ± RBV; SOFO + PEG + RBV; SOF + RBV; SOF + SMV ± RBV, obtained SVR rates ranging from 92.2 to 100%.

The analyses of the sociodemographic data showed that being a woman aged between 20 and 49 years and residing in the Southeast and Center-West regions were predictors of a better response to DAA-based therapies (Table 2). The age range 50–69 years yielded a slightly lower response to DAAs when compared to other age groups (SVR of 94.8%), although this finding was not confirmed in the bivariate analysis, and the multivariate model could not be conducted (Table 2a). A large retrospective cohort study with about 17,500 patients with HCV, grouped into six age groups (<55 years of age, 55–59, 60–64, 65–69, 70–74, 75 years of age) and treated with DAA-based therapies in 2014/2015 found high SVR rates ranging from 90 to 94%, similar to those found in our study. It is worth highlighting that advanced age was not a predictor for a negative response, but rather the presence of cirrhosis. It is probable that in our cohort, people of more advanced age – being the largest group – had cirrhosis or neoplasms and that may have influenced the relatively lower SVR rates for this age group. However, when the factor age was analyzed independently, it was not a predictor of a lower SVR in relation to other age groups, according to other published studies.²⁰20 Reid M, Price JC, Tien PC. Hepatitis C virus infection in the older patient. Infect Dis Clin North Am. 2017;31:827-38.^–²²22 Su F, Beste LA, Green PK, Berry K, Ioannou GN. Direct-acting antivirals are effective for chronic hepatitis C treatment in elderly patients: a real-world study of 17 487 patients. Eur J Gastroenterol Hepatol. 2017;29:686-93. The positive response rate in the five regions of the country ranged from 94.0 to 96.7%, being significantly better in the Center-West and Southeast, with an OR of 0.5 and 0.7, respectively. These finding are difficult to interpret, although quality of life and access to healthcare in these regions may contribute to a better regional response to DAAs. The state of São Paulo accounts for a large representation of patients in the Southeast region and this state is known as having a good public healthcare system. On the other hand, other conditions influencing the achievement or not of SVR are discussed in depth throughout this study.

The best therapeutic results for genotype 1a and 1b, utilizing these regimens, ranged from 96.3 to 96.7%, respectively. Patients with genotypes 2 and 3 obtained the lowest SVR rates (92.2% and 90.6%, respectively) and were 1.5 and 2.8 more likely to not have SVR, respectively, when compared to genotype 1a and 1b, a finding that has been confirmed in other studies.¹⁸18 Im GY, Dieterich DT. Direct-acting antiviral agents in patients with hepatitis C cirrhosis. Gastroenterol Hepatol. 2012;8.^–²⁴24 Holzmann I, Tovo CV, Minmé R, Leal MP, Kliemann MP, Ubirajara C, et al. Effectiveness of chronic hepatitis C treatment with direct-acting antivirals in the Public Health System in Brazil. Braz J Infect Dis. 2018;22:317-22. Genotype 4 had an SVR of 97.6%, an excellent result, but the difference cannot be established as significant due to the small number of cases. Ferreira and collaborators evaluated 296 patients in the South region, obtaining SVR rates of 92%.²⁵25 Perazzo H, Jorge MJ, Silva JC, Avellar AM, Silva PS, Romero C, et al. Micro-costing analysis of guideline-based treatment by direct-acting agents: the real-life case of hepatitis C management in Brazil. BMC Gastroenterol. 2017;17:1-11. Another study including 1002 patients treated for HCV, with genotypes 1, 2 and 3, also carried out in the South region by Holzmann et al., found that even patients with liver cirrhosis achieved SVR rates ranging from 88.5% to 100%.²⁴24 Holzmann I, Tovo CV, Minmé R, Leal MP, Kliemann MP, Ubirajara C, et al. Effectiveness of chronic hepatitis C treatment with direct-acting antivirals in the Public Health System in Brazil. Braz J Infect Dis. 2018;22:317-22. In another study, in which 219 patients underwent therapy with DAAs, a high rate of SVR and excellent drug tolerability were found. Failure to achieve SVR was observed mainly among patients with at least one negative response predictor: cirrhosis and/or genotypes 2 or 3.²⁵25 Perazzo H, Jorge MJ, Silva JC, Avellar AM, Silva PS, Romero C, et al. Micro-costing analysis of guideline-based treatment by direct-acting agents: the real-life case of hepatitis C management in Brazil. BMC Gastroenterol. 2017;17:1-11. Other studies carried out in the Southeast region yielded similar data.¹⁷17 R Foundation for Statistical, Viena/Autria Available: https://www.r-project.org/, 2015.
https://www.r-project.org/... ^–²⁰20 Reid M, Price JC, Tien PC. Hepatitis C virus infection in the older patient. Infect Dis Clin North Am. 2017;31:827-38.^,²⁶26 Wang GP, Terrault N, Reeves JD, Liu L, Li E, Zhao L, et al. Prevalence and impact of baseline resistance-associated substitutions on the efficacy of ledipasvir/sofosbuvir or simeprevir/sofosbuvir against GT1 HCV infection. Sci Rep. 2018;8:1-14.^,²⁷27 Das C, Hansen KC, Tyler JKLMS. 乳鼠心肌提取 HHS Public Access. Physiol Behav. 2017;176:139-148.

This study showed that the SOF + RBV scheme had a significantly lower response to HCV (SVR 92.2%; OR 1.6; CI 95% 1.1–2.5). We also verified a higher response for the SOF + DCV + RBV scheme than for other antivirals (SVR 96%; OR 0.8; CI 0.6–1.0). The SOF + SMV regimen, with an SVR of 95.6%, yielded values that were very similar to SOF + DCV (95.1%); The addition of RBV to both schemes increased the rates to 96.7% and 96%, respectively (Table 2b). However, in the multivariate analyses, the SOF + SMV scheme proved to be less effective than SOF + DCV (OR 1.3), results that have also been corroborated in other studies.²⁶26 Wang GP, Terrault N, Reeves JD, Liu L, Li E, Zhao L, et al. Prevalence and impact of baseline resistance-associated substitutions on the efficacy of ledipasvir/sofosbuvir or simeprevir/sofosbuvir against GT1 HCV infection. Sci Rep. 2018;8:1-14.^,²⁷27 Das C, Hansen KC, Tyler JKLMS. 乳鼠心肌提取 HHS Public Access. Physiol Behav. 2017;176:139-148.

Although the SVR of 3D + RBV was 100%, we were not able to verify whether this result was significant due to the small number of treated patients (Table 2).

The high cure rate after using the therapeutic schemes considered in this study, with data from all Brazilian states, has great relevance to demonstrate that public policies developed by the Brazilian Ministry of Health, including the incorporation of therapies requiring large investments, providing cure for thousands of hepatitis C patients, has brought Brazil closer to the goal of eliminating the disease as a public health hazard, and over 140,000 people have been treated to date. This study can help to understand the dynamics of response to therapy in the Brazilian population. The average positive response with the use of DAAs ranged from 95.0% to 95.9%, demonstrating that it is possible to obtain good results with therapies for hepatitis C in the public health system.

Limitations

This study was conducted using, initially, secondary data collected from the Ministry of Health’s information systems (DATASUS). However, in order to collect data, it was necessary to work with several independent areas of that institution, as there is no interface between the different systems. Therefore, investments to increase the performance of the Ministry’s systems – in charge of so many diseases – would facilitate research and permit more efficient analyses of data by managers at all levels (municipalities, states, and the federal government).

Although around 80,000 treatments were distributed throughout the period of this study, when the databases were merged, only 29,033 patients were found in the GAL database for undergoing some hepatitis C exam while also being registered in other databases related to the treatment of Hepatitis C (SIASUS - BPAI and APAC). Of these, 19,100 (66%) had qPCR-HCV in the GAL, but only 11,308 (∼60%) had qPCR-HCV after 12 weeks of treatment for hepatitis C (Fig. 2). Therefore, it can be inferred that most patients may have undergone testing through Supplementary Health Care (Health Insurance Plans) or bore the costs of laboratory tests themselves, and therefore, were not included in the GAL system database.

Among the main limitations to this study, the incompleteness of data in all systems stands out. The main data refer to results of viral genotype; race/color (Tables 1 and 2). The study was conducted with secondary data that did not always adequately control confounding factors. The absence of sociodemographic data (resulting from poorly filled out forms), such as information about race/color (27%) is common in the various SUS databases (e.g.: GAL and Sinan- Notifiable Diseases Information System).

In the evaluated age groups, we found some differences in the SVR rate, but this was not confirmed by the bivariate analyses. SVR rates varied from 98.6 to 100% in the age group between 10 and 29 years. This indicates that there is a better response to therapy among younger populations; however, the number of patients assessed was small (73) and this positive difference in SVR could not be confirmed in the statistical models.

Conclusion

Even without obtaining data for all patients initially located in the SIA/SUS, it is possible to conclude that the data in this study obtained excellent results, consistent with the study performed. Brazil is also a signatory to the World Health Organization resolution and has a National Plan for the Elimination of Hepatitis C as a public health hazard by 2030. One of the main goals of this plan is to offer more diagnosis and treatment for 50,000 people annually, by 2025.¹³13 Ministério da Saúde. B, Brasília Protocolo Clínico E Diretrizes Terapêuticas Para Hepatite C e Coinfecções; 2018.^,²⁸28 Cooke GS, Andrieux-Meyer I, Applegate TL, Atun R, Burry JR, Cheinquer H, et al. Accelerating the elimination of viral hepatitis: a lancet gastroenterology & hepatology commission. Lancet Gastroenterol Hepatol. 2019;4:135-84.

Our work shows that the incorporation of DAAs was of prime importance to achieve high cure rates in the studied population and highlights the importance of monitoring treatments and achieving virologic cure. The Brazilian Public Health System must be included among the public institutions that offer treatments to its population in a universal and egalitarian way.

Currently, new treatments are being incorporated into SUS, with other drugs that are as good or better than the ones we studied. Our study demonstrates that the excellent results obtained in curing patients with hepatitis C may have even better results in the future. This is significantly important, confirming the excellent results of the treatment of hepatitis C in the national territory and the need to maintain treatment for the elimination of hepatitis C as a public health problem by 2030.⁵5 Benzaken AS, Girade R, Catapan E, Pereira GFM, de Almeida EC, Vivaldini S, et al. Hepatitis C disease burden and strategies for elimination by 2030 in Brazil. A mathematical modeling approach. Braz J Infect Dis. 2019;23:182-90.^,¹⁴14 Brasil. Ministério da Saúde, Available: www.aids.gov.br, 2018.
www.aids.gov.br... ^,²⁸28 Cooke GS, Andrieux-Meyer I, Applegate TL, Atun R, Burry JR, Cheinquer H, et al. Accelerating the elimination of viral hepatitis: a lancet gastroenterology & hepatology commission. Lancet Gastroenterol Hepatol. 2019;4:135-84.

Funding sources

University of Brasília (UnB), Faculty of Medicine, Center for Tropical Medicine, Brasília, DF, Brazil

Acknowledgements

We would like to acknowledge all of the support provided in the preparation and publication of this study, Brazil’s Ministry of Health, DATASUS and the Department of Chronic Conditions Diseases, and other Sexually Transmitted Infections/the Ministry of Health, teams who made this study possible.

References

¹
World Health Organization, Available: http://apps.who.int/iris/bitstream/handle/10665/255016/9789241565455-eng.pdf?sequence=1, 2017.
» http://apps.who.int/iris/bitstream/handle/10665/255016/9789241565455-eng.pdf?sequence=1
²
Blach S, Zeuzem S, Manns M, Altraif I, Duberg AS, Muljono DH, et al. Global prevalence and genotype distribution of hepatitis C virus infection in 2015: a modelling study. Lancet Gastroenterol Hepatol. 2017;2:161-76.
³
World Health Organization, Available: https://www.who.int/hepatitis/publications/hep-c-access-report-2018/en/, 2018.
» https://www.who.int/hepatitis/publications/hep-c-access-report-2018/en/
⁴
Spearman CW, Dusheiko GM, Hellard M, Sonderup M. Hepatitis C. Lancet. 2019;394:1451-66.
⁵
Benzaken AS, Girade R, Catapan E, Pereira GFM, de Almeida EC, Vivaldini S, et al. Hepatitis C disease burden and strategies for elimination by 2030 in Brazil. A mathematical modeling approach. Braz J Infect Dis. 2019;23:182-90.
⁶
Brasil. Ministério da Saúde, Protocolo Clínico e Diretrizes Terapêuticas para Hepatite C e Coinfecções. Brasília, 2011.
⁷
Ministério da Saúde-Brasil, Available: Protocolo Clínico e Diretrizes Terapêuticas para Hepatite C e Coinfecções; 2015. p. 1–98 http://bvsms.saude.gov.br/bvs/publicacoes/protocolo_clinicodiretrizeshepatite_co_coinfeccoes.pdf
» http://bvsms.saude.gov.br/bvs/publicacoes/protocolo_clinicodiretrizeshepatite_co_coinfeccoes.pdf
⁸
Id WL, Lin Y, Chang C, Chang C. Impact of direct-acting antiviral therapy for hepatitis C – related hepatocellular carcinoma. PLoS One J. 2020;:80-90.
⁹
Gallach M, Vergara M, da Costa JP, Miquel M, Casas M, Sanchez-Delgado J, et al. Impact of treatment with direct-acting antivirals on anxiety and depression in chronic hepatitis C. PLoS One. 2018;13:1-15.
¹⁰
Gastaldi G, Gomes D, Schneiter P, Montet X, Tappy L, Clément S, et al. Treatment with direct-acting antivirals improves peripheral insulin sensitivity in nondiabetic, lean chronic hepatitis C patients. PLoS One. 2019;14:1-17.
¹¹
Juanbeltz R, Martínez-Baz I, San Miguel R, Goñi-Esarte S, Cabasés JM, Castilla J. Impact of successful treatment with directacting antiviral agents on health-related quality of life in chronic hepatitis C patients. PLoS One. 2018;13:1-15.
¹²
Roche B, Coilly A, Duclos-Vallee JC, Samuel D. The impact of treatment of hepatitis C with DAAs on the occurrence of HCC. Liver Int. 2018;38:139-45.
¹³
Ministério da Saúde. B, Brasília Protocolo Clínico E Diretrizes Terapêuticas Para Hepatite C e Coinfecções; 2018.
¹⁴
Brasil. Ministério da Saúde, Available: www.aids.gov.br, 2018.
» www.aids.gov.br
¹⁵
Castelo A, Brandão Mello CE, Teixeira R, Madruga JVR, Reuter T, Pereira LMMB, et al. Hepatitis C in the Brazilian public health care system: burden of disease. Arq Gastroenterol. 2018;55:329-37.
¹⁶
Departamento de Informática do SUS/DATASUS-Ministério da Saúde [cited 8 Jun 2020]. Available: http://datasus1.saude.gov.br/noticias/atualizacoes/1167-datasus-demas-e-hospital-albert-einstein-promovem-workshop-vinculasus, 2020.
» http://datasus1.saude.gov.br/noticias/atualizacoes/1167-datasus-demas-e-hospital-albert-einstein-promovem-workshop-vinculasus
¹⁷
R Foundation for Statistical, Viena/Autria Available: https://www.r-project.org/, 2015.
» https://www.r-project.org/
¹⁸
Im GY, Dieterich DT. Direct-acting antiviral agents in patients with hepatitis C cirrhosis. Gastroenterol Hepatol. 2012;8.
¹⁹
Daniel KE, Saeian K, Rizvi S. Real-world experiences with direct-acting antiviral agents for chronic hepatitis C treatment. J Viral Hepat. 2020;27:195-204.
²⁰
Reid M, Price JC, Tien PC. Hepatitis C virus infection in the older patient. Infect Dis Clin North Am. 2017;31:827-38.
²¹
Ioannou GN, Beste LA, Chang MF, Green PK, Lowy E, Tsui JI, et al. Effectiveness of sofosbuvir, ledipasvir/sofosbuvir, or paritaprevir/ritonavir/ombitasvir and dasabuvir regimens for treatment of patients with hepatitis C in the Veterans affairs national health care system. Gastroenterology. 2016;151:457-471.e5.
²²
Su F, Beste LA, Green PK, Berry K, Ioannou GN. Direct-acting antivirals are effective for chronic hepatitis C treatment in elderly patients: a real-world study of 17 487 patients. Eur J Gastroenterol Hepatol. 2017;29:686-93.
²³
Ferreira VL, Borba HHL, Wiens A, Pedroso MLA, Radunz VF de C, Ivantes CAP, et al. Effectiveness and tolerability of direct-acting antivirals for chronic hepatitis C patients in a Southern state of Brazil. Braz J Infect Dis. 2018;22:186-92.
²⁴
Holzmann I, Tovo CV, Minmé R, Leal MP, Kliemann MP, Ubirajara C, et al. Effectiveness of chronic hepatitis C treatment with direct-acting antivirals in the Public Health System in Brazil. Braz J Infect Dis. 2018;22:317-22.
²⁵
Perazzo H, Jorge MJ, Silva JC, Avellar AM, Silva PS, Romero C, et al. Micro-costing analysis of guideline-based treatment by direct-acting agents: the real-life case of hepatitis C management in Brazil. BMC Gastroenterol. 2017;17:1-11.
²⁶
Wang GP, Terrault N, Reeves JD, Liu L, Li E, Zhao L, et al. Prevalence and impact of baseline resistance-associated substitutions on the efficacy of ledipasvir/sofosbuvir or simeprevir/sofosbuvir against GT1 HCV infection. Sci Rep. 2018;8:1-14.
²⁷
Das C, Hansen KC, Tyler JKLMS. 乳鼠心肌提取 HHS Public Access. Physiol Behav. 2017;176:139-148.
²⁸
Cooke GS, Andrieux-Meyer I, Applegate TL, Atun R, Burry JR, Cheinquer H, et al. Accelerating the elimination of viral hepatitis: a lancet gastroenterology & hepatology commission. Lancet Gastroenterol Hepatol. 2019;4:135-84.

Publication Dates

Publication in this collection
16 June 2021
Date of issue
2021

History

Received
19 Nov 2020
Accepted
10 Feb 2021

This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial No Derivative License, which permits unrestricted non-commercial use, distribution, and reproduction in any medium provided the original work is properly cited and the work is not changed in any way.

[1] Funding sources

University of Brasília (UnB), Faculty of Medicine, Center for Tropical Medicine, Brasília, DF, Brazil

Characteristics	Patients
	Total (N = 11,308)
	N	%
Sex
Male	6,459	57.1
Female	4,847	42.9
Ignored	2	0.0
Race/Color
White	5,464	48.3
Black	598	5.3
Asian	965	8.5
Brown	1,217	10.8
Indigenous	5	0.0
Ignored	3,059	27.1
Age group
0 to 9	0	0.0
10 to 19	2	0.0
20 to 29	71	0.6
30 to 39	516	4.6
40 to 49	1,884	16.7
50 to 59	3,970	35.1
60 to 69	3,522	31.1
Above 70	1,343	11.9
Region of Residence
North	617	5.5
Northeast	825	7.3
Southeast	4,983	44.1
South	4,393	38.8
Center-West	490	4.3
Genotypes
Genotype 1	56	0.5
Genotype 1a	1,674	14.8
Genotype 1b	5,395	47.7
Genotype 2	282	2.5
Genotype 3	1,934	17.1
Genotype 4	42	0.4
Mixed Genotypes	12	0.1
Unknown	1,913	16.9
Treatment Time
12 weeks	9,554	84.5
24 weeks	1,752	15.5
Unknown	2	0.0

Characteristics	SVR
	No		Yes		Bivariate analysis			Multivariate analysis
	Total (N = 550)		Total (N = 10,758)		Odds Ratio	Confidence Interval (CI) 95%	p-Value	Odds Ratio	CI 95%	p-Value
	N	%	N	%
Sex
Male*	399	6.2	6,060	93.8	-	-	-	-	-	-
Female	151	3.1	4,696	96.9	0.5	(0.4 ; 0.6)	< 0.0001	0.5	(0.4 ; 0.6)	< 0.0001
Unknown	0	0.0	2	100.0	0.0	-	-	0.0	-	-
Race/color
White*	285	5.2	5,179	94.8	-	-	-	-	-	-
Black	23	3.8	575	96.2	0.7	(0.5 ; 1.1)	0.1492	0.8	(0.5 ; 1.3)	0.4599
Asian	50	5.2	915	94.8	1.0	(0.7 ; 1.4)	0.9644	1.0	(0.7 ; 1.5)	0.8774
Brown	60	4.9	1,157	95.1	0.9	(0.7 ; 1.3)	0.6837	1.0	(0.7 ; 1.4)	0.8939
Indigenous	0	0.0	5	100.0	0.0	-	0.7350	0.0	-	0.9893
Unknown	132	4.3	2,927	95.7	0.8	(0.7 ; 1.0)	0.0648	0.9	(0.7 ; 1.1)	0.2054
Age range
10 to 19	0	0.0	2	100.0	0.0	-	0.3587	-	-	-
20 to 29	1	1.4	70	98.6	0.3	(0.0 ; 2.3)	0.2503	-	-	-
30 to 39*	23	4.5	493	95.5	-	-	-	-	-	-
40 to 49	83	4.4	1,801	95.6	1.0	(0.6 ; 1.6)	0.9595	-	-	-
50-59	211	5.3	3,759	94.7	1.2	(0.8 ; 1.9)	0.4105	-	-	-
60 to 69	182	5.2	3,340	94.8	1.2	(0.7 ; 1.8)	0.4929	-	-	-
Above 70	50	3.7	1,293	96.3	0.8	(0.5 ; 1.4)	0.4660	-	-	-
Region of Residence
North*	37	6.0	580	94.0	-	-	-	-	-	-
Northeast	48	5.8	777	94.2	1.0	(0.6 ; 1.5)	0.8867	0.9	(0.5 ; 1.4)	0.5730
Southeast	206	4.1	4,777	95.9	0.7	(0.5 ; 1.0)	0.0332	0.8	(0.6 ; 1.3)	0.3997
South	243	5.5	4,150	94.5	0.9	(0.6 ; 1.3)	0.6377	1.0	(0.6 ; 1.4)	0.8371
Center-West	16	3.3	474	96.7	0.5	(0.3 ; 1.0)	0.0372	0.7	(0.4 ; 1.3)	0.2121
Genotypes
1	0	0.0	56	100.0	0.0	-	0.3004	0.0	-	0.9666
1a*	62	3.7	1,612	96.3	-	-	-	-	-	-
1b	180	3.3	5,215	96.7	0.9	(0.7 ; 1.2)	0.4705	0.9	(0.6 ; 1.2)	0.3538
2	22	7.8	260	92.2	2.2	(1.2 ; 3.6)	0.0022	1.5	(0.7 ; 2.9)	0.2831
3	181	9.4	1,753	90.6	2.7	(2.0 ; 3.6)	< 0.0001	2.8	(2.0 ; 3.8)	< 0.0001
4	1	2.4	41	97.6	0.6	(0.1 ; 4.7)	0.6553	0.6	(0.1 ; 4.5)	0.6200
Mixed genotypes	0	0.0	12	100.0	0.0	-	0.9826	0.0	-	0.9844
Unknown	104	5.4	1,809	94.6	1.5	(1.1 ; 2.1)	0.0143	1.2	(0.9 ; 1.8)	0.1968
Therapeutic scheme
3D + RBV	0	0.0	30	100.0	0.0	-	0.4212	0.0	-	0.9757
SOFO + DCV*	199	4.9	3,859	95.1	-	-	-	-	-	-
SOF + DCV RBV	159	4.0	3,835	96.0	0.8	(0.6 ; 1.0)	0.0449	0.8	(0.6 ; 0.9)	0.0094
SOFO + PEG + RBV	9	4.9	175	95.1	1.0	(0.5 ; 2.0)	0.9938	0.5	(0.2 ; 1.0)	0.0369
SOF + RBV	29	7.8	342	92.2	1.6	(1.1 ; 2.5)	0.0161	1.4	(0.8 ; 2.5)	0.2218
SOF + SMV	79	4.6	1,649	95.4	0.9	(0.7 ; 1.2)	0.5888	1.3	(1.0 ; 1.8)	0.0484
SOF + SMV + RBV	13	3.3	377	96.7	0.7	(0.4 ; 1.2)	0.1671	1.0	(0.5 ; 1.7)	0.9092
Unknown	16	4.8	318	95.2	1.0	(0.6 ; 1.6)	0.9264	1.0	(0.6 ; 1.8)	0.8644
Others therapies DAA	3	4.8	60	95.2	1.0	(0.3 ; 3.1)	0.9587	1.2	(0.4 ; 3.9)	0.7585
Peg + RBV	43	27.6	113	72.4	7.4	(5.1 ; 10.8)	< 0.0001	7.5	(5.0 ; 11.2)	< 0.0001
Time of treatment
12 weeks*	479	5.0	9,075	95.0	-	-	-	-	-	-
24 weeks	71	4.1	1,681	95.9	0.8	(0.6 ; 1.0)	0.0862	0.8	(0.6 ; 1.1)	0.1973
Unknown	0	0.0	2	100.0	0.0	-	0.3904	0.0	-	0.9935
Fibrosis/Cirrhosis
Yes*	171	4.6	3,551	95.4	-	-	-	-	-	-
No	379	5.0	7,209	95.0	1.1	(0.9 ; 1.3)	0.3524	-	-	-

Therapeutic scheme	Patients (N)	%	Genotypes	SVR
				No (%)	Yes (%)
3D + RBV with DAA	4	0.0%	genotype 1a	-	100
3D + RBV with DAA	26	0.2%	genotype 1b	-	100
SOF + DAC	18	0.2%	genotype 1	-	100
	604	5.3%	genotype 1a	3.5	96.5
	1,899	16.8%	genotype 1b	2.5	97.5
	20	0.2%	genotype 2	5	95
	782	6.9%	genotype 3	11.9	88.1
	31	0.3%	genotype 4	3.2	96.8
	6	0.1%	Mixed genotypes	-	100
	698	6.2%	ignored	5	95
SOF + DAC + RBV	18	0.2%	genotype 1	-	100
	610	5.4%	genotype 1a	2.3	97.7
	1,753	15.5%	genotype 1b	2.7	97.3
	9	0.1%	genotype 2	-	100
	893	7.9%	genotype 3	7.3	92.7
	8	0.1%	genotype 4	-	100
	4	0.0%	Mixed genotypes	-	100
	699	6.2%	ignored	4.6	95.4
SOF + PEG-RBV	8	0.1%	genotype 2	12.5	87.5
	146	1.3%	genotype 3	4.1	95.9
	30	0.3%	ignored	6.7	93.3
SOF + RBV	14	0.1%	genotype 1a	7.1	92.9
	60	0.5%	genotype 1b	3.3	96.7
	225	2.0%	genotype 2	7.6	92.4
	26	0.2%	genotype 3	11.5	88.5
	46	0.4%	ignored	13	87
SOF + SMV	10	0.1%	genotype 1	-	100
	289	2.6%	genotype 1a	5.5	94.5
	1,147	10.1%	genotype 1b	4.4	95.6
	3	0.0%	genotype 2	-	100
	3	0.0%	genotype 3	-	100
	2	0.0%	Mixed genotypes	-	100
	274	2.4%	ignored	4.7	95.3
SOF + SMV + RBV	6	0.1%	genotype 1	-	100
	84	0.7%	genotype 1a	3.6	96.4
	246	2.2%	genotype 1b	4.1	95.9
	54	0.5%	ignored	-	100
Unknown therapy	3	0.0%	genotype 1	-	100
	36	0.3%	genotype 1a	-	100
	197	1.7%	genotype 1b	4.1	95.9
	11	0.1%	genotype 2	-	100
	51	0.5%	genotype 3	11.8	88.2
	1	0.0%	genotype 4	-	100
	35	0.3%	ignored	5.7	94.3
Other DAA therapies	1	0.0%	genotype 1	-	100
	15	0.1%	genotype 1a	-	100
	27	0.2%	genotype 1b	-	100
	1	0.0%	genotype 2	100
	8	0.1%	genotype 3	-	100
	2	0.0%	genotype 4	-	100
	9	0.1%	ignored	22.2	77.8
Other non-DAA therapy	18	0.2%	genotype 1a	38.9	61.1
	40	0.4%	genotype 1b	35	65
	5	0.0%	genotype 2	40	60
	25	0.2%	genotype 3	32	68
	68	0.6%	ignored	17.6	82.4