Hepatitis C virus: Difference between revisions
From IDWiki
mNo edit summary |
(→: added info about serology in Ontario) |
||
(25 intermediate revisions by the same user not shown) | |||
Line 1: | Line 1: | ||
==Background== |
|||
= Microbiology = |
|||
===Microbiology=== |
|||
* Enveloped single-stranded RNA virus |
|||
* NS5A and NS5B |
|||
*Enveloped single-stranded RNA virus in the genus ''Hepacivirus'' and family ''[[Flaviviridae]]'' |
|||
= Life Cycle = |
|||
*NS5A and NS5B are important non-structural proteins |
|||
===Life Cycle=== |
|||
* NS5A…... |
|||
* NS5B |
|||
*Involves protease, polymerase, and non-structural proteins (NS5A/NS5B) |
|||
= Epidemiology = |
|||
===Epidemiology=== |
|||
* Worldwide about 170 million cases |
|||
* Genotype varies by geography |
|||
** Genotype 1a and 1b common in Canada |
|||
*** Disproportionate burden in Indigienous Canadian population |
|||
*** Very high burden of disease in Canada, causing more years of life lost in Ontario than any other infectious disease |
|||
** Genotype 3 more common in injection drug use and south-east Asia |
|||
** Genotype 4 common in Egypt (15% prevalence) |
|||
* Modes of transmission |
|||
** Injection drug use (most important population, highest risk) |
|||
** Tattoos |
|||
** Blood transfusions before 1992 |
|||
** Cocaine use from blood on the straws |
|||
** Rarely, sexual transmission especially HIV-infected MSM |
|||
** Vertical transmission rare (3-5%) |
|||
** Iatrogenic or medical transmission, from multi-use vials |
|||
* In Canada, about 245,000 chronic hepatitis C, about half are undiagnosed |
|||
** Risk factors: injection drug use (highest risk), prior transfusion, and hemophilia |
|||
** Increasing burden of disease as patients progress to cirrhosis |
|||
*Worldwide about 70 million cases |
|||
= Pathophysiology = |
|||
*'''Genotype''' varies by geography |
|||
**Genotype 1 most common worldwide |
|||
**Genotype 1a and 1b common in Canada |
|||
***Disproportionate burden in Indigienous Canadian population in the North |
|||
***Very high burden of disease in Canada, causing more years of life lost in Ontario than any other infectious disease |
|||
**Genotype 3 more common south-east Asia and in injection drug use |
|||
**Genotype 4 common in Egypt (15% prevalence); Egypt has the highest burden in the world |
|||
*In '''Canada''', about 245,000 chronic hepatitis C, about half are undiagnosed |
|||
**Risk factors: injection drug use (highest risk), prior transfusion, and hemophilia |
|||
**Increasing burden of disease as patients age and progress to cirrhosis |
|||
*Modes of transmission |
|||
**Injection drug use (most important population, highest risk) |
|||
**Tattoos |
|||
**Blood transfusions before 1992 |
|||
**Cocaine use from blood on the straws |
|||
**Rarely, sexual transmission especially HIV-infected MSM |
|||
**Vertical transmission rare (3-5%) |
|||
**Iatrogenic or medical transmission, from multi-use vials |
|||
===Pathophysiology=== |
|||
* In the acute phase, the viral load and liver enzymes fluctuate over months |
|||
** Anti-HCV-Ab develops at 12 weeks |
|||
** Acute phase lasts 6 months to 2 years |
|||
* Spontaneous clearance is rare after 2 years |
|||
** Anti-HCV-Ab positive and HCV RNA negative |
|||
** Repeat to confirm, but no need to follow it |
|||
** No complications, though it is a surrogate for risk behaviours |
|||
** ''Not'' protected from reinfection |
|||
* If it isn't cleared, it becomes chronic |
|||
** Lifetime risk of cirrhosis is 50-60%, with 20% having cirrhosis at 20 years |
|||
** Liver cancer develops in 1-4% |
|||
*In the acute phase, the viral load and liver enzymes fluctuate over months |
|||
= Clinical Presentation = |
|||
**Anti-HCV-Ab develops at 12 weeks |
|||
**Acute phase lasts 6 months to 2 years |
|||
*Spontaneous clearance is rare after 2 years |
|||
**Anti-HCV-Ab positive and HCV RNA negative |
|||
**Repeat to confirm, but no need to follow it |
|||
**No complications, though it is a surrogate for risk behaviours |
|||
**''Not'' protected from reinfection |
|||
*If it isn't cleared, it becomes chronic |
|||
**Lifetime risk of cirrhosis is 50-60%, with 20% having cirrhosis at 20 years |
|||
**Liver cancer develops in 1-4% |
|||
==Clinical Manifestations== |
|||
* After exposure, may clear infection, but 70-80% become chronically infected |
|||
* Progresses slowly and asymptomatically until they develop liver fibrosis, compensated cirrhosis, then decompensated cirrhosis |
|||
** ~20-25% progress to end-stage liver disease within 20 years |
|||
*After exposure, incubation period of [[Usual incubation period::5 to 12 weeks]] |
|||
= Management = |
|||
*Not all have symptoms of primary infection, but if they do they are typically non-specific fatigue and myalgias, and occasionally jaundice |
|||
**Lasts 2 to 12 weeks |
|||
*About 25% have spontaneous viral clearance within 6 to 12 months, with the rest progressing to chronic infection |
|||
*Chronic infection progresses slowly and asymptomatically until they develop liver fibrosis, compensated cirrhosis, and finally decompensated cirrhosis |
|||
**~20-25% progress to end-stage liver disease within 20 years |
|||
=== Extrahepatic Manifestations === |
|||
== Decision to treat == |
|||
* [[Vasculitis]] |
|||
* All individuals should be considered for antiretroviral treatment |
|||
** [[Mixed cryoglobulinemia]] |
|||
* Assess readiness for treatment, as good adherence is necessary |
|||
** [[Cryoglobulinemic vasculitis]] |
|||
* Alcohol, drug use, and mental health disorders are ''not'' containdications to treatment |
|||
** [[Sicca syndrome]] and [[Sjögren syndrome]] |
|||
** [[Polyarteritis nodosa]] |
|||
* Hematologic disorders |
|||
** [[B-cell lymphoma]] |
|||
** [[Monoclonal gammopathies]] |
|||
** [[Immune thrombocytopenia]] |
|||
** [[Autoimmune hemolytic anemia]] |
|||
* Endocrine diseases |
|||
** [[Type 2 diabetes mellitus]] |
|||
** [[Hypothyroidism]] |
|||
* Renal disease |
|||
** [[Membranoproliferative glomerulonephritis]] |
|||
** [[Chronic kidney disease]] |
|||
* Dermatologic findings |
|||
** [[Porphyria cutanea tarda]] |
|||
** [[Lichen planus]] |
|||
** [[Necrolytic acral erythema]] |
|||
** [[Leukocytoclastic vasculitis]] |
|||
* Other |
|||
** Arthralgias and myalgias are common |
|||
** [[Cardiovascular disease]] |
|||
** Neurologic disorders, including [[depression]], fatigue, and neurocognitive impairment, as well as [[neuropathy]] |
|||
* Autoantibodies, including [[rheumatoid factor]], [[ANA]], anticardiolipin antibody, anti-thyroid antibodies, and anti-smooth muscle antibody |
|||
==Diagnosis== |
|||
== Initial investigations == |
|||
*Screening with serology for anti-HCV antibodies followed by RNA PCR to confirm ongoing infection |
|||
* Confirm active infection with HCV RNA then get genotype and subtype |
|||
**The window period for serology is about 5 to 10 weeks before antibodies are detectable |
|||
** Two positive HCV RNA tests 6 months apart documents chronic infection |
|||
**Viral RNA detectable 2 to 14 days after exposure |
|||
** May need resistance testing |
|||
*Anti-HCV antibodies appear to be lifelong but not protective against reinfection, so need to check RNA PCR to rule out reinfection |
|||
* Baseline bloodwork, including CBC, liver enzymes, liver function, and creatinine |
|||
*In Ontario, serology is done with a two-tier algorithm (screening test and confirmatory test) |
|||
* Serology to exclude HIV and HBV |
|||
**Screening test is chemiluminescent microparticle immunoassay (CMIA) |
|||
* Transferrin saturation to exclude hemochromatosis, and IgG levels to exclude autimmune hepatitis |
|||
**Confirmatory test is a second chemiluminescence assay |
|||
* Baseline liver ultrasound |
|||
**Interpretation: |
|||
* If not clearly cirrhotic, assess liver fibrosis |
|||
***Screening and confirmatory reactive: positive test |
|||
** Bloodwork: AST:platelet ratio index (APRI), FIB-4, FibroTest |
|||
***Screening non-reactive: negative test |
|||
** Imaging: FibroScan |
|||
***Screening reactive (or indeterminate) and confirmatory non-reactive (or indeterminate): inconclusive |
|||
** Gold standard: biopsy |
|||
****Submit HCV RNA with repeat serology |
|||
****If RNA not detected, repeat serology at 6-8 weeks |
|||
****If repeatedly inconclusive, discuss with microbiologist |
|||
== |
==Management== |
||
===Decision to Treat=== |
|||
* Include nonstructural 3/4A (NS3/4A) serine protease (-previr), the NS5B RNA dependent RNA polymerase (-buvir) and the NS5A protein (-asvir) |
|||
* Assess drug-drug interactions with [[https://www.hepdruginteractions.org/|www.hepdruginteractions.org]] |
|||
** PPI and Epclusa/Harvoni |
|||
** Statins require dose reduction; atorvastatin and Maviret is no-no |
|||
** Anti-epileptics except leviteracetam |
|||
* Choice of treatment regimen depends on genotype, previously-failed treatments, and cirrhosis |
|||
** All protease inhibitors (-previr) are contraindicated in decompensated cirrhosis, which refers to ascites, esophageal variceal hemorrhage, jaundice, or hepatic encephalopathy |
|||
** Sofosbuvir/velpatasvir/voxilaprevir (Vosevi) is indicated for previously-treated patients |
|||
*All individuals should be considered for antiretroviral treatment |
|||
{| |
|||
*Assess readiness for treatment, as good adherence is necessary |
|||
! Regimen |
|||
*Alcohol, drug use, and mental health disorders are ''not'' containdications to treatment |
|||
! 1a |
|||
! 1b |
|||
===Initial Investigations=== |
|||
! 2 |
|||
! 3 |
|||
*Confirm active infection with HCV RNA then get genotype and subtype |
|||
! 4 |
|||
**Two positive HCV RNA tests 6 months apart documents chronic infection, only needed in Ontario |
|||
! 5 |
|||
**May need resistance testing |
|||
! 6 |
|||
**Genotype only actually matters for cirrhosis (since we can otherwise pick a pan-genotypic regimen) |
|||
*Baseline bloodwork, including CBC, liver enzymes (ALT, AST, ALP), liver function (bilirubin, INR, albumin), and creatinine |
|||
*Serology to exclude HIV and HBV (HBsAg, anti-HBs, anti-HBc) |
|||
*Transferrin saturation to exclude [[hemochromatosis]] |
|||
*IgG levels, which if elevated can be suggestive of [[cirrhosis]] or possibly [[autoimmune hepatitis]] |
|||
*Baseline liver ultrasound |
|||
*If not clearly cirrhotic, assess liver fibrosis |
|||
**Bloodwork: [[AST:platelet ratio index]] (APRI), [[FIB-4]], FibroTest |
|||
**Imaging: FibroScan |
|||
**Gold standard: biopsy |
|||
===Antivirals=== |
|||
*Include nonstructural 3/4A (NS3/4A) serine protease (-previr), the NS5B RNA dependent RNA polymerase (-buvir) and the NS5A protein (-asvir) |
|||
*Assess drug-drug interactions with [https://www.hepdruginteractions.org/ www.hepdruginteractions.org] |
|||
**PPIs interact with Epclusa and Harvoni |
|||
**Statins require dose reduction; avoid [[atorvastatin]] with Maviret |
|||
**Notable interactions with most anti-epileptics, except leviteracetam |
|||
**[[Sofosbuvir]] increases [[TDF]] levels |
|||
*Choice of treatment regimen depends on genotype, previously-failed treatments, and cirrhosis |
|||
**All protease inhibitors (-previr) are contraindicated in decompensated cirrhosis, which refers to ascites, esophageal variceal hemorrhage, jaundice, or hepatic encephalopathy |
|||
**[[Sofosbuvir]]/[[velpatasvir]]/[[voxilaprevir]] (Vosevi) is indicated for previously-treated patients |
|||
*Durations are typically between 8 and 12 weeks |
|||
**Epclusa 12 weeks for most, now covered by ODB |
|||
**Zepatier 12 weeks for G1 and G4 |
|||
**Maviret 8 weeks for most; 12 weeks for cirrhosis |
|||
**Harvoni 8 weeks if uncomplicated |
|||
====Treatment-Naive Patients Without Cirrhosis==== |
|||
{| class="wikitable" |
|||
! rowspan="2" |Regimen |
|||
! colspan="7" |Duration by Genotype (weeks) |
|||
! rowspan="2" |Notes |
|||
|- |
|- |
||
!1a |
|||
| Ledipasvir/sofosbuvir (Harvoni) |
|||
!1b |
|||
| 12 wk ± ribavirin |
|||
!2 |
|||
| 12 wk |
|||
!3 |
|||
| – |
|||
!4 |
|||
| 12 wk + ribavirin |
|||
!5 |
|||
| 12 wk |
|||
!6 |
|||
| 12 wk |
|||
| 12 wk |
|||
|- |
|- |
||
|[[Ledipasvir]]/[[sofosbuvir]] (Harvoni) |
|||
| Elbasvir/grazoprevir (Zepatier) |
|||
| |
|12 ± RBV |
||
| |
|12 |
||
|— |
|||
| – |
|||
| |
|12 + RBV |
||
| |
|12 |
||
|12 |
|||
| – |
|||
|12 |
|||
| – |
|||
| |
|||
|- |
|- |
||
|[[Elbasvir]]/[[grazoprevir]] (Zepatier) |
|||
| Sofosbuvir/velpatasvir (Epclusa) |
|||
| |
|12-16 ± RBV |
||
| |
|12 |
||
|— |
|||
| 12 wk |
|||
| |
|12 + SOF |
||
| |
|12 |
||
|— |
|||
| 12 wk |
|||
|— |
|||
| 12 wk |
|||
|rule out resistance first in G1a |
|||
|- |
|- |
||
|[[Paritaprevir]]/[[ritonavir]]/[[ombitasvir]] + [[dasabuvir]] (Holkira Pak) |
|||
| Glecaprevir/pibrentasvir (Maviret) |
|||
| |
|12 + RBV |
||
|12 |
|||
| 8 wk |
|||
|— |
|||
| 8 wk |
|||
|— |
|||
| 8 wk |
|||
|— |
|||
| 8 wk |
|||
|— |
|||
| 8 wk |
|||
|— |
|||
| 8 wk |
|||
|add ribavirin for G1a |
|||
|- |
|- |
||
|[[Paritaprevir]]/[[ritonavir]]/[[ombitasvir]] (Technivie) |
|||
| ... |
|||
|— |
|||
|— |
|||
|— |
|||
|— |
|||
|12 + RBV |
|||
|— |
|||
|— |
|||
| |
| |
||
|- |
|||
|[[Sofosbuvir]] + [[daclatasvir]] |
|||
|12 |
|||
|12 |
|||
|12 |
|||
|12 |
|||
|— |
|||
|— |
|||
|— |
|||
| |
| |
||
|- |
|||
|[[Sofosbuvir]]/[[velpatasvir]] (Epclusa) |
|||
|12 |
|||
|12 |
|||
|12 |
|||
|12 |
|||
|12 |
|||
|12 |
|||
|12 |
|||
| |
| |
||
|- |
|||
|[[Glecaprevir]]/[[pibrentasvir]] (Maviret) |
|||
|8 |
|||
|8 |
|||
|8 |
|||
|8 |
|||
|8 |
|||
|8 |
|||
|8 |
|||
| |
| |
||
|- |
|||
|[[Sofosbuvir]]/[[velpatasvir]]/[[voxilaprevir]] (Vosevi) |
|||
|— |
|||
|— |
|||
|— |
|||
|— |
|||
|— |
|||
|— |
|||
|— |
|||
|for treatment failure |
|||
|} |
|||
====Treatment-Naive Patients With Cirrhosis==== |
|||
{| class="wikitable" |
|||
! rowspan="2" |Regimen |
|||
! colspan="7" |Duration by Genotype (weeks) |
|||
! rowspan="2" |Notes |
|||
|- |
|||
!1a |
|||
!1b |
|||
!2 |
|||
!3 |
|||
!4 |
|||
!5 |
|||
!6 |
|||
|- |
|||
|[[Ledipasvir]]/[[sofosbuvir]] (Harvoni) |
|||
|12 ± RBV |
|||
|12 |
|||
|— |
|||
|12 + RBV |
|||
|12 |
|||
|12 |
|||
|12 |
|||
| |
| |
||
|- |
|||
|[[Elbasvir]]/[[grazoprevir]] (Zepatier) |
|||
|12-16 ± RBV |
|||
|12 |
|||
|— |
|||
|12 + SOF |
|||
|12 |
|||
|— |
|||
|— |
|||
|rule out resistance first in G1a |
|||
|- |
|||
|[[Paritaprevir]]/[[ritonavir]]/[[ombitasvir]] + [[dasabuvir]] (Holkira Pak) |
|||
|12 + RBV |
|||
|12 |
|||
|— |
|||
|— |
|||
|— |
|||
|— |
|||
|— |
|||
|add ribavirin for G1a |
|||
|- |
|||
|[[Paritaprevir]]/[[ritonavir]]/[[ombitasvir]] (Technivie) |
|||
|— |
|||
|— |
|||
|— |
|||
|— |
|||
|12 + RBV |
|||
|— |
|||
|— |
|||
| |
| |
||
|- |
|||
|[[Sofosbuvir]] + [[daclatasvir]] |
|||
|24 |
|||
|24 |
|||
|24 |
|||
|24 ± RBV |
|||
|— |
|||
|— |
|||
|— |
|||
| |
| |
||
|- |
|||
|[[Sofosbuvir]]/[[velpatasvir]] (Epclusa) |
|||
|12 |
|||
|12 |
|||
|12 |
|||
|12 ± RBV |
|||
|12 |
|||
|12 |
|||
|12 |
|||
| |
|||
|- |
|||
|[[Glecaprevir]]/[[pibrentasvir]] (Maviret) |
|||
|12 |
|||
|12 |
|||
|12 |
|||
|12 |
|||
|12 |
|||
|12 |
|||
|12 |
|||
| |
|||
|- |
|||
|[[Sofosbuvir]]/[[velpatasvir]]/[[voxilaprevir]] (Vosevi) |
|||
|— |
|||
|— |
|||
|— |
|||
|— |
|||
|— |
|||
|— |
|||
|— |
|||
|for treatment failure |
|||
|} |
|} |
||
====Treatment-Experienced Patients==== |
|||
* Epclusa 12 weeks for most, now OCB covered |
|||
* Zepatier 12 weeks for G1 and G4 |
|||
*Changes the options, mostly longer courses of treatment |
|||
* Maviret 8 weeks for most; 12 weeks for cirrhosis |
|||
* Harvoni 8 weeks if uncomplicated |
|||
===Non-Pharmacologic Management=== |
|||
== Experienced patients == |
|||
*Counsel to avoid sharing products like needles or razors, safe sex, avoid alcohol |
|||
* Changes the options, mostly longer |
|||
*Vaccinate for [[hepatitis A]] and [[Hepatitis B virus|B]] |
|||
===Follow-Up=== |
|||
== Non-pharmacologic management == |
|||
*Need to confirm sustained virologic response (SVR), defined as negative PCR 12 weeks after completing therapy |
|||
* Counsel to avoid sharing products like needles or razors, safe sex, avoid alcohol |
|||
*If they have achieved SVR |
|||
* Vaccinate for Hep A and B |
|||
**In patients without cirrhosis, no specific follow-up is necessary |
|||
**In patients with cirrhosis, they should have biannual HCC screening with ultrasound |
|||
**Annual HCV RNA in patients with ongoing risk factors |
|||
*If they have not achieved, then they should be evaluated for salvage therapy |
|||
== |
==Screening== |
||
*Majority of cases of chronic hepatitis C occur in baby boomers (born 1945 to 1975), though screening for this population appears to be controversial |
|||
* Need to confirm sustained virologic response (SVR) |
|||
===Populations to Screen=== |
|||
= Screening = |
|||
*'''History of injection drug use, ever''' |
|||
* Majority of cases of chronic hepatitis C occur in baby boomers (born 1945 to 1975), though screening for this population appears to be controversial |
|||
*History of incarceration |
|||
*Received healthcare where there is a lack of IPAC |
|||
*Blood products or organ transplantation before 1992 in Canada |
|||
*Born or resided in a country where prevalence of HCV is >3% |
|||
**Central, East and South Asia |
|||
**Australasia and Oceania |
|||
**Eastern Europe |
|||
**Subsaharan Africa |
|||
**North Africa or the Middle East |
|||
*Born to HCV positive mother |
|||
*History of sharing personal care items or sex with an HCV-positive person |
|||
*HIV infection |
|||
*Received hemodialysis |
|||
*Elevated ALT |
|||
*'''Born between 1945 and 1975''' (baby boomers) |
|||
**Recommended in the US and by CASL but not by CTFPHC |
|||
====Opportunistic Screening==== |
|||
== Populations to screen == |
|||
*Emergency rooms |
|||
* '''History of injection drug use, ever''' |
|||
*Hospital inpatients |
|||
* History of incarceration |
|||
*Substance use treatment clinics |
|||
* Received healthcare where there is a lack of IPAC |
|||
* Blood products or organ transplantation before 1992 in Canada |
|||
* Born or resided in a country where prevalence of HCV is >3% |
|||
** Central, East and South Asia |
|||
** Australasia and Oceania |
|||
** Eastern Europe |
|||
** Subsaharan Africa |
|||
** North Africa or the Middle East |
|||
* Born to HCV positive mother |
|||
* History of sharing personal care items or sex with an HCV-positive person |
|||
* HIV infection |
|||
* Received hemodialysis |
|||
* Elevated ALT |
|||
* '''Born between 1945 and 1975''' (baby boomers) |
|||
== |
===Screening Procedure=== |
||
* |
*Anti-HCV antibody |
||
**Serum serology gold standard |
|||
* If positive, proceed to HCV RNA |
|||
**There are some quick point-of-care tests, like from saliva |
|||
* Should be done annually in patients who have ongoing high-risk exposures |
|||
**Also cheap options like dried blood spot testing, which can have RNA testing as well |
|||
*If positive, proceed to HCV RNA |
|||
**May be able to do it as reflex testing |
|||
*Should be done annually in patients who have ongoing high-risk exposures |
|||
= |
==Further Reading== |
||
* |
*Shah H, ''et al''. [https://doi.org/10.1503/cmaj.170453 The management of chronic hepatitis C: 2018 guideline update from the Canadian Association for the Study of the Liver]. ''CMAJ''. 2018;190(22):E677-E687. |
||
* |
*[https://doi.org/10.1093/cid/ciy585 Hepatitis C Guidance 2018 Update: AASLD-IDSA Recommendations for Testing, Managing, and Treating Hepatitis C Virus Infection]. ''Clin Infect Dis''. 2018;67(10):1477-92. |
||
[[Category:Flaviviridae]] |
[[Category:Flaviviridae]] |
||
[[Category:Hepatitis C]] |
Latest revision as of 13:36, 15 September 2022
Background
Microbiology
- Enveloped single-stranded RNA virus in the genus Hepacivirus and family Flaviviridae
- NS5A and NS5B are important non-structural proteins
Life Cycle
- Involves protease, polymerase, and non-structural proteins (NS5A/NS5B)
Epidemiology
- Worldwide about 70 million cases
- Genotype varies by geography
- Genotype 1 most common worldwide
- Genotype 1a and 1b common in Canada
- Disproportionate burden in Indigienous Canadian population in the North
- Very high burden of disease in Canada, causing more years of life lost in Ontario than any other infectious disease
- Genotype 3 more common south-east Asia and in injection drug use
- Genotype 4 common in Egypt (15% prevalence); Egypt has the highest burden in the world
- In Canada, about 245,000 chronic hepatitis C, about half are undiagnosed
- Risk factors: injection drug use (highest risk), prior transfusion, and hemophilia
- Increasing burden of disease as patients age and progress to cirrhosis
- Modes of transmission
- Injection drug use (most important population, highest risk)
- Tattoos
- Blood transfusions before 1992
- Cocaine use from blood on the straws
- Rarely, sexual transmission especially HIV-infected MSM
- Vertical transmission rare (3-5%)
- Iatrogenic or medical transmission, from multi-use vials
Pathophysiology
- In the acute phase, the viral load and liver enzymes fluctuate over months
- Anti-HCV-Ab develops at 12 weeks
- Acute phase lasts 6 months to 2 years
- Spontaneous clearance is rare after 2 years
- Anti-HCV-Ab positive and HCV RNA negative
- Repeat to confirm, but no need to follow it
- No complications, though it is a surrogate for risk behaviours
- Not protected from reinfection
- If it isn't cleared, it becomes chronic
- Lifetime risk of cirrhosis is 50-60%, with 20% having cirrhosis at 20 years
- Liver cancer develops in 1-4%
Clinical Manifestations
- After exposure, incubation period of 5 to 12 weeks
- Not all have symptoms of primary infection, but if they do they are typically non-specific fatigue and myalgias, and occasionally jaundice
- Lasts 2 to 12 weeks
- About 25% have spontaneous viral clearance within 6 to 12 months, with the rest progressing to chronic infection
- Chronic infection progresses slowly and asymptomatically until they develop liver fibrosis, compensated cirrhosis, and finally decompensated cirrhosis
- ~20-25% progress to end-stage liver disease within 20 years
Extrahepatic Manifestations
- Vasculitis
- Hematologic disorders
- Endocrine diseases
- Renal disease
- Dermatologic findings
- Other
- Arthralgias and myalgias are common
- Cardiovascular disease
- Neurologic disorders, including depression, fatigue, and neurocognitive impairment, as well as neuropathy
- Autoantibodies, including rheumatoid factor, ANA, anticardiolipin antibody, anti-thyroid antibodies, and anti-smooth muscle antibody
Diagnosis
- Screening with serology for anti-HCV antibodies followed by RNA PCR to confirm ongoing infection
- The window period for serology is about 5 to 10 weeks before antibodies are detectable
- Viral RNA detectable 2 to 14 days after exposure
- Anti-HCV antibodies appear to be lifelong but not protective against reinfection, so need to check RNA PCR to rule out reinfection
- In Ontario, serology is done with a two-tier algorithm (screening test and confirmatory test)
- Screening test is chemiluminescent microparticle immunoassay (CMIA)
- Confirmatory test is a second chemiluminescence assay
- Interpretation:
- Screening and confirmatory reactive: positive test
- Screening non-reactive: negative test
- Screening reactive (or indeterminate) and confirmatory non-reactive (or indeterminate): inconclusive
- Submit HCV RNA with repeat serology
- If RNA not detected, repeat serology at 6-8 weeks
- If repeatedly inconclusive, discuss with microbiologist
Management
Decision to Treat
- All individuals should be considered for antiretroviral treatment
- Assess readiness for treatment, as good adherence is necessary
- Alcohol, drug use, and mental health disorders are not containdications to treatment
Initial Investigations
- Confirm active infection with HCV RNA then get genotype and subtype
- Two positive HCV RNA tests 6 months apart documents chronic infection, only needed in Ontario
- May need resistance testing
- Genotype only actually matters for cirrhosis (since we can otherwise pick a pan-genotypic regimen)
- Baseline bloodwork, including CBC, liver enzymes (ALT, AST, ALP), liver function (bilirubin, INR, albumin), and creatinine
- Serology to exclude HIV and HBV (HBsAg, anti-HBs, anti-HBc)
- Transferrin saturation to exclude hemochromatosis
- IgG levels, which if elevated can be suggestive of cirrhosis or possibly autoimmune hepatitis
- Baseline liver ultrasound
- If not clearly cirrhotic, assess liver fibrosis
- Bloodwork: AST:platelet ratio index (APRI), FIB-4, FibroTest
- Imaging: FibroScan
- Gold standard: biopsy
Antivirals
- Include nonstructural 3/4A (NS3/4A) serine protease (-previr), the NS5B RNA dependent RNA polymerase (-buvir) and the NS5A protein (-asvir)
- Assess drug-drug interactions with www.hepdruginteractions.org
- PPIs interact with Epclusa and Harvoni
- Statins require dose reduction; avoid atorvastatin with Maviret
- Notable interactions with most anti-epileptics, except leviteracetam
- Sofosbuvir increases TDF levels
- Choice of treatment regimen depends on genotype, previously-failed treatments, and cirrhosis
- All protease inhibitors (-previr) are contraindicated in decompensated cirrhosis, which refers to ascites, esophageal variceal hemorrhage, jaundice, or hepatic encephalopathy
- Sofosbuvir/velpatasvir/voxilaprevir (Vosevi) is indicated for previously-treated patients
- Durations are typically between 8 and 12 weeks
- Epclusa 12 weeks for most, now covered by ODB
- Zepatier 12 weeks for G1 and G4
- Maviret 8 weeks for most; 12 weeks for cirrhosis
- Harvoni 8 weeks if uncomplicated
Treatment-Naive Patients Without Cirrhosis
Regimen | Duration by Genotype (weeks) | Notes | ||||||
---|---|---|---|---|---|---|---|---|
1a | 1b | 2 | 3 | 4 | 5 | 6 | ||
Ledipasvir/sofosbuvir (Harvoni) | 12 ± RBV | 12 | — | 12 + RBV | 12 | 12 | 12 | |
Elbasvir/grazoprevir (Zepatier) | 12-16 ± RBV | 12 | — | 12 + SOF | 12 | — | — | rule out resistance first in G1a |
Paritaprevir/ritonavir/ombitasvir + dasabuvir (Holkira Pak) | 12 + RBV | 12 | — | — | — | — | — | add ribavirin for G1a |
Paritaprevir/ritonavir/ombitasvir (Technivie) | — | — | — | — | 12 + RBV | — | — | |
Sofosbuvir + daclatasvir | 12 | 12 | 12 | 12 | — | — | — | |
Sofosbuvir/velpatasvir (Epclusa) | 12 | 12 | 12 | 12 | 12 | 12 | 12 | |
Glecaprevir/pibrentasvir (Maviret) | 8 | 8 | 8 | 8 | 8 | 8 | 8 | |
Sofosbuvir/velpatasvir/voxilaprevir (Vosevi) | — | — | — | — | — | — | — | for treatment failure |
Treatment-Naive Patients With Cirrhosis
Regimen | Duration by Genotype (weeks) | Notes | ||||||
---|---|---|---|---|---|---|---|---|
1a | 1b | 2 | 3 | 4 | 5 | 6 | ||
Ledipasvir/sofosbuvir (Harvoni) | 12 ± RBV | 12 | — | 12 + RBV | 12 | 12 | 12 | |
Elbasvir/grazoprevir (Zepatier) | 12-16 ± RBV | 12 | — | 12 + SOF | 12 | — | — | rule out resistance first in G1a |
Paritaprevir/ritonavir/ombitasvir + dasabuvir (Holkira Pak) | 12 + RBV | 12 | — | — | — | — | — | add ribavirin for G1a |
Paritaprevir/ritonavir/ombitasvir (Technivie) | — | — | — | — | 12 + RBV | — | — | |
Sofosbuvir + daclatasvir | 24 | 24 | 24 | 24 ± RBV | — | — | — | |
Sofosbuvir/velpatasvir (Epclusa) | 12 | 12 | 12 | 12 ± RBV | 12 | 12 | 12 | |
Glecaprevir/pibrentasvir (Maviret) | 12 | 12 | 12 | 12 | 12 | 12 | 12 | |
Sofosbuvir/velpatasvir/voxilaprevir (Vosevi) | — | — | — | — | — | — | — | for treatment failure |
Treatment-Experienced Patients
- Changes the options, mostly longer courses of treatment
Non-Pharmacologic Management
- Counsel to avoid sharing products like needles or razors, safe sex, avoid alcohol
- Vaccinate for hepatitis A and B
Follow-Up
- Need to confirm sustained virologic response (SVR), defined as negative PCR 12 weeks after completing therapy
- If they have achieved SVR
- In patients without cirrhosis, no specific follow-up is necessary
- In patients with cirrhosis, they should have biannual HCC screening with ultrasound
- Annual HCV RNA in patients with ongoing risk factors
- If they have not achieved, then they should be evaluated for salvage therapy
Screening
- Majority of cases of chronic hepatitis C occur in baby boomers (born 1945 to 1975), though screening for this population appears to be controversial
Populations to Screen
- History of injection drug use, ever
- History of incarceration
- Received healthcare where there is a lack of IPAC
- Blood products or organ transplantation before 1992 in Canada
- Born or resided in a country where prevalence of HCV is >3%
- Central, East and South Asia
- Australasia and Oceania
- Eastern Europe
- Subsaharan Africa
- North Africa or the Middle East
- Born to HCV positive mother
- History of sharing personal care items or sex with an HCV-positive person
- HIV infection
- Received hemodialysis
- Elevated ALT
- Born between 1945 and 1975 (baby boomers)
- Recommended in the US and by CASL but not by CTFPHC
Opportunistic Screening
- Emergency rooms
- Hospital inpatients
- Substance use treatment clinics
Screening Procedure
- Anti-HCV antibody
- Serum serology gold standard
- There are some quick point-of-care tests, like from saliva
- Also cheap options like dried blood spot testing, which can have RNA testing as well
- If positive, proceed to HCV RNA
- May be able to do it as reflex testing
- Should be done annually in patients who have ongoing high-risk exposures
Further Reading
- Shah H, et al. The management of chronic hepatitis C: 2018 guideline update from the Canadian Association for the Study of the Liver. CMAJ. 2018;190(22):E677-E687.
- Hepatitis C Guidance 2018 Update: AASLD-IDSA Recommendations for Testing, Managing, and Treating Hepatitis C Virus Infection. Clin Infect Dis. 2018;67(10):1477-92.