Hepatitis C (HCV)
Hepatitis C is a blood-borne viral infection caused by the Hepatitis C virus (HCV) that primarily affects the liver. It is a major global cause of:
- Chronic hepatitis
- Cirrhosis
- Portal hypertension
- Hepatocellular carcinoma (HCC)
- Liver transplantation
Unlike hepatitis A or B, HCV becomes chronic in 55–85% of infected patients, making it one of the most important causes of chronic liver disease worldwide.
In India
- Prevalence ~0.5–1.5%
- Common in:
- Hemodialysis patients
- Multi-transfused patients (thalassemia)
- IV drug users
Genotypes (Important for therapy)
- Genotype 1 (most common globally)
- Genotype 3 (common in India)
- Genotype 2, 4, 5, 6
👉 With modern pan-genotypic DAAs, genotype testing is often not required.
Transmission
Parenteral transmission is the main route
High-Risk Groups
- IV drug use (most common in developed nations)
- Unsafe injections
- Blood transfusion before 1992
- Hemodialysis
- Healthcare exposure
- Vertical transmission (5–6%)
- Sexual transmission (low but higher in MSM with HIV)
❌ Not spread by casual contact, food, or water.
Natural History
Acute Hepatitis C
- Incubation: 2–12 weeks
- Often asymptomatic
- Mild transaminitis
- Jaundice rare
Outcomes of Acute Infection
|
Outcome |
Percentage |
|
Spontaneous clearance |
15–45% |
|
Chronic infection |
55–85% |
Risk of chronicity higher in:
- Males
- HIV co-infection
- Immunosuppression
Chronic Hepatitis C
Defined as detectable HCV RNA > 6 months.
Pathophysiology
- Persistent viral replication
- Chronic inflammation
- Progressive fibrosis
- Cirrhosis (20–30% over 20 years)
- HCC risk increases after cirrhosis
Extrahepatic Manifestations
HCV is a systemic disease.
|
System |
Manifestation |
|
Renal |
Membranoproliferative GN |
|
Hematologic |
Mixed cryoglobulinemia |
|
Dermatologic |
Lichen planus |
|
Rheumatologic |
Arthralgia |
|
Endocrine |
Thyroiditis |
|
Lymphatic |
B-cell lymphoma |
Classic association:
👉 Mixed cryoglobulinemia
Diagnosis
Step 1: Screening Test
- Anti-HCV antibody (ELISA)
If positive → proceed to RNA testing
Step 2: Confirmatory Test
- HCV RNA by PCR
- Detects active infection
- Quantitative viral load
Step 3: Assess Liver Damage
- LFTs (AST > ALT in advanced disease)
- Platelet count (low = portal hypertension)
- APRI / FIB-4 score
- FibroScan
- Liver biopsy (rare now)
Non-Invasive Fibrosis Assessment in Hepatitis C
APRI | FIB-4 | FibroScan (Transient Elastography)
In modern HCV management (DAA era), liver biopsy is rarely needed. Instead, we use validated non-invasive tools to stage fibrosis and identify cirrhosis.
1️⃣ APRI Score (AST to Platelet Ratio Index)
What it estimates:Degree of liver fibrosis using:AST,Platelet count
Formula
APRI=(ULNASTAST )×100÷Plateletcount(109/L)
Where:
- AST = patient value
- ULN AST = upper limit of normal
Interpretation (WHO & AASLD accepted cutoffs)
|
APRI |
Interpretation |
|
< 0.5 |
No/minimal fibrosis |
|
0.5–1.0 |
Indeterminate |
|
≥ 1.0 |
Significant fibrosis (≥F2) |
|
≥ 2.0 |
Cirrhosis likely |
Why Platelets Matter?
In chronic liver disease:
- Portal hypertension → splenic sequestration → ↓ platelets
- More fibrosis → lower platelets
Limitations
- Affected by acute inflammation
- AST elevation from other causes alters result
- Less accurate in early fibrosis
2️⃣ FIB-4 Score
More accurate than APRI. Widely used in HCV and NAFLD.
FIB4=Plateletcount×ALT Age×AST
Interpretation
|
FIB-4 |
Meaning |
|
< 1.45 |
Advanced fibrosis unlikely |
|
1.45–3.25 |
Indeterminate |
|
> 3.25 |
Advanced fibrosis likely |
|
> 3.25–3.5 |
Strongly suggests cirrhosis |
In primary care:
- <1.3 → rule out advanced fibrosis
- 2.67 → rule in advanced fibrosis
📌 Why It’s Better Than APRI
- Includes age
- Includes ALT
- Higher diagnostic accuracy
3️⃣ FibroScan (Transient Elastography)
It measures liver stiffness in kilopascals (kPa).
Principle
- Low-frequency vibration wave is sent into liver.
- Shear wave velocity measured.
- Stiffer liver → faster wave → higher kPa.
Fibrosis → increased stiffness.
Interpretation in HCV
|
kPa |
Stage |
|
< 7 |
No significant fibrosis |
|
7–9.5 |
Moderate fibrosis |
|
9.5–12.5 |
Advanced fibrosis |
|
> 12.5 |
Cirrhosis likely |
Note: Cutoffs vary slightly by etiology.
Limitations
False elevation in:
- Acute hepatitis
- Congestive hepatopathy
- Cholestasis
- Post-meal state
- Obesity (technical failure)
Not reliable in:
- Ascites (cannot perform)
Current Practice (DAA Era)
In Hepatitis C patients:
Step 1 → Calculate FIB-4
If indeterminate → FibroScan
If cirrhosis suspected → Manage as cirrhosis
Treatment (Game-Changer Era)
Direct-Acting Antivirals (DAAs) have revolutionized therapy.
Cure rate: >95%
Common Regimens (Pan-genotypic)
|
Regimen |
Duration |
|
Sofosbuvir + Velpatasvir |
12 weeks |
|
Glecaprevir + Pibrentasvir |
8–12 weeks |
Mechanism targets:
- NS3/4A protease
- NS5A protein
- NS5B polymerase
Goal of Treatment
- Sustained Virologic Response (SVR)
- Defined as undetectable HCV RNA 12 weeks after therapy
- Equivalent to cure
HCC Surveillance
For:
- Cirrhosis
- Advanced fibrosis
Screening:
- Ultrasound every 6 months
- ± AFP
❌ No vaccine available (due to high mutation rate)