Hepatitis C Infection and Treatment among Injecting Drug Users Attending General Practice: A Systematic Review and Meta-Analysis
Abstract
:1. Introduction
2. Materials and Methods
2.1. Data Source and Search Strategy
2.2. Screening and Eligibility
2.3. Inclusion and Exclusion Criteria
2.4. Quality Assessment
2.5. Study Outcomes
2.6. Data Extraction and Analysis
3. Results
3.1. Selection of Included Studies
3.2. Characteristics of the 18 Included Studies
3.3. Prevalence of HCV among Patients with a History of Intravenous Drug Use
3.4. HCV Diagnosis, Treatment, and Cure Rates
3.5. Opiate Substitution Therapy (OST)
3.6. Chronic Conditions
3.7. Risk of Bias Assessment
4. Discussion
4.1. Summary
4.2. Strengths and Limitations
4.3. Comparison with the Literature
5. Conclusions
Supplementary Materials
Author Contributions
Funding
Institutional Review Board Statement
Informed Consent Statement
Conflicts of Interest
References
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Study ID | Study Design | # of GP Sites | Are All Practices OST Centres? | Sample (Participants) | Study Period (Duration) | Sex (M/F) | Age (years) | Country | Main Outcome of the Study |
---|---|---|---|---|---|---|---|---|---|
Crofts et al. 1997 [34] | Retrospective cohort review | 1 | Yes | 1741 | January 1991–December 1995 (73 months) | 1010/730 | Mean 32.5 | Australia | HCV seroprevalence and effect of methadone maintenance therapy on HCV control |
Peat et al. 2000 [35] | Retrospective cohort review | 1 | NR | 115 | October 1999–February 2000 (5 months) | NR | NR | UK (Scotland) | HCV prevalence and referral to specialist treatment for infection |
Denis et al. 2000 [37] | Cross-sectional, comparative | 10 | Yes | 329 | 1995–June 1998 (NR) | 224/85 | Mean 25.9 Range 16–45 | Belgium | HCV seroprevalence—associated risk factors and feasibility of treatment |
Pradat et al. 2001 [38] | Cross-sectional | 271 * | NR | 11,804 | May–October 1997 (6 months) | NR | NR | France | HCV seroprevalence |
Budd et al. 2002 [32] | Cross-sectional | 1 | NR | 619 | January–May 2000 (5 months) | NR | NR | UK (Scotland) | HCV prevalence and associated risk factors |
Cullen et al. 2003 [13] | Retrospective record review | 42 | Yes | 571 | NR (NR) | 409/162 | Mean 28 | Ireland | HCV seroprevalence and associated factors |
Cullen 2005 [27] | Cross-sectional | 1 | Yes | 25 | 2002 (1 months and 2 weeks) | 14/11 | Mean 32 | Ireland | Awareness and experience of HCV infection, investigation, and treatment |
Cullen et al. 2006 [28] | Cluster randomized controlled trial | 26 | Yes | 196 | NR (6 months) | 142/54 | Mean 32.5 | Ireland | HCV screening and evaluation of clinical guideline implementation and treatment outcome |
Cullen et al. 2007 [30] | Cross-sectional | 25 | Yes | 196 | Early 2002 (NR) | 142/54 | Mean 32.2 Range 19–65 | Ireland | HCV infection care process—testing, hepatology referral, HCV treatment, alcohol consumption |
Jack et al. 2008 [36] | Clinical trial | 2 | Yes | 353 | February 2005–January 2008 (36 months) | 256/26 | Mean 34.7 Range 21–53 | UK (England) | HCV diagnosis, feasibility of antiviral treatment and outcome |
Anderson et al. 2009 [33] | Controlled intervention | 2 | Yes | 117 | November 2003–April 2004 (6 months) | 180/241 | NR | UK (Scotland) | HCV screening evaluation—test offer, uptake, and diagnosis |
Senn et al. 2009 [25] | Retrospective cohort review | 1 | Yes | 387 | January 2002–May 2008 (89 months) | 268/119 | Median 38.5 | Switzerland | Assessment of chronic HCV infection—viral load, genotypes |
Cullen et al. 2011 [29] | Controlled intervention | 16 | Yes | 422 | February–October 2007 (9 months) | NR | Range 30–54 | UK (Scotland) | HCV seroprevalence—test uptake, referral, management of PCR in intervention and control sites |
Seidenberg et al. 2013 [16] | Retrospective cohort | 1 | Yes | 85 | January 2002–May 2008 (89 months) | 52/33 | Median 38.8 | Switzerland | HCV treatment rate and sustained virological response rates between patients with and without drug dependency |
Datta et al. 2014 [12] | Cross-sectional | 6 | NR | 3765 | August 2012–January 2013 (6 months) | NR | NR | UK (England) | HCV seroprevalence |
Murtagh et al. 2018 [14] | Retrospective cohort-feasibility study | 14 | Yes | 134 | NR (NR) | 96/38 | Mean 43 Range 27–71 | Ireland | HCV management—process and outcomes |
Wade et al. 2019 [31] | Randomized controlled trial | 13 | Yes | 70 | November 2015–June 2018 (32 months) | 52/18 | Mean 47 | Australia and New Zealand | HCV treatment: direct-acting antiviral treatment uptake and sustained virological response |
Heard et al. 2020 [26] | Cross-sectional qualitative | 7 | No, only 5 out of 7 | 27 | NR (NR) | 18/9 | Range 33–65 | Australia | HCV management—barriers and enablers of direct-acting antiviral treatment |
Total | 440 | 20,956 | 2863/1580 |
Study ID | Study Reported HCV Treatment | Number Treated | Genotypes Detected (Treated) | Drugs by Genotypes and Duration |
---|---|---|---|---|
Denis et al. 2000 [37] | Yes | 10 | NR | Interferon |
Cullen 2005 [27] | Yes | 1 | NR | Interferon |
Cullen et al. 2006 [28] | Yes | 6 | NR | NR |
Cullen et al. 2007 [30] | Yes | 3 | NR | NR |
Jack et al. 2008 [36] | Yes | 30 | Genotype 1 (7), Genotype 3 (14), Genotype unknown (9) | NR |
Anderson et al. 2009 [33] | Yes | 2 | NR | NR |
Senn et al. 2009 [25] * | NR | Genotype 1 (43), Genotype 3 (34), Genotype 4 (9) * | ||
Cullen et al. 2011 [29] | Yes | 4 | NR | NR |
Seidenberg et al. 2013 [16] | Yes | 35 | Genotype 1 (19), Genotype 3 (13), Genotype 4 (30) | Genotypes 1 and 4—once-weekly injections of peginterferon alfa-2a (180 μg) plus ribavirin (1000 mg or 1200 mg/day) for 48 weeks. Genotype 3—ribavirin 800 mg/day and peginterferon alfa-2a 180 μg/week subcutaneously for 24 weeks. |
Murtagh et al. 2018 [14] | Yes | 20 | NR | NR |
Wade et al. 2019 [31] | Yes | 43 | Genotype 1, Genotype 1a, and Genotype 3 | Genotype 1—co-formulated paritaprevir 75 mg, ritonavir 50 mg, and ombitasvir 12.5 mg in two tablets daily plus dasabuvir 250 mg one tablet twice daily for 12 weeks. Genotype 1a—weight-based ribavirin; patients ≤75 kg received 1000 mg and patients ≥75 kg received 1200 mg daily for 12 weeks. Genotype 3—sofosbuvir 400 mg and daclatasvir 60 mg one tablet daily for 12 weeks. |
Heard et al. 2020 [26] | Yes | 20 | NR | NR |
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Tandan, M.; Dunlea, S.; Bury, G. Hepatitis C Infection and Treatment among Injecting Drug Users Attending General Practice: A Systematic Review and Meta-Analysis. Int. J. Environ. Res. Public Health 2023, 20, 5569. https://doi.org/10.3390/ijerph20085569
Tandan M, Dunlea S, Bury G. Hepatitis C Infection and Treatment among Injecting Drug Users Attending General Practice: A Systematic Review and Meta-Analysis. International Journal of Environmental Research and Public Health. 2023; 20(8):5569. https://doi.org/10.3390/ijerph20085569
Chicago/Turabian StyleTandan, Meera, Shane Dunlea, and Gerard Bury. 2023. "Hepatitis C Infection and Treatment among Injecting Drug Users Attending General Practice: A Systematic Review and Meta-Analysis" International Journal of Environmental Research and Public Health 20, no. 8: 5569. https://doi.org/10.3390/ijerph20085569
APA StyleTandan, M., Dunlea, S., & Bury, G. (2023). Hepatitis C Infection and Treatment among Injecting Drug Users Attending General Practice: A Systematic Review and Meta-Analysis. International Journal of Environmental Research and Public Health, 20(8), 5569. https://doi.org/10.3390/ijerph20085569