Hepatitis C

HCV Diagnostic testing

Principles of testing

Detection of viral RNA by nucleic acid tests (NAT, usually using reverse transcription polymerase chain reaction; RT PCR) indicates current infection. Detection of antibodies indicates resolved or current infection. The testing algorithm suggested in Figure 1 is based on the following key principles:

• diagnostic assays are most reliable when used on plasma or serum ¹⁹ 2++
• assays for antibody in saliva are very sensitive if optimum salivary collection devices and modified enzyme linked immunosorbent assays (ELISA) are used, but NAT for viral RNA is unreliable ^19-21 2++
• limited testing of dried blood spots for detecting antibody has suggested it may be useful but further evaluation is needed for the detection of viral RNA ¹⁹ 2++
• nucleic acid testing sensitive enough to detect 50-100 IU/ml of virus must be performed to detect current infection ²² 2+
• viral RNA can be detected as early as one to two weeks after infection, whereas antibody can be detected at seven to eight weeks after infection ²³ 4
• antibody to infection may not be generated particularly if the individual is immunosuppressed ²⁴ 4
• following acute infection, HCV RNA may oscillate between positive and negative for several months. Results from samples taken at this time may be misleading. ²³ In an individual positive for HCV antibody, but negative for HCV RNA, a second sample should be tested to confirm the initial diagnosis, especially as the date of infection is unknown in most cases 4
• individuals with a positive HCV antibody test and repeatedly negative RNA do not require further active management of hepatitis C infection ²⁴ 4
• since hepatitis C is a serious communicable disease, after an initial laboratory diagnosis, a second sample should be taken from the patient to confirm correct identification of the original sample ²⁵ 4
• genotyping of individuals with proven HCV infection is required to determine likely response to treatment. Those with genotype 1 infection require longer duration of treatment than those with genotype 2 and 3 (see section 9.1.2) ⁷ 1++
• expert guidance suggests that healthcare workers who have, or might have, sustained an occupational exposure to HCV should be offered RNA testing at 6, 12 and 24 weeks, with anti-HCV testing at 12 and 24 weeks. ²⁶ 4

Diagnostic testing for HCV should be performed on serum or plasma where possible.

Grade B
A body of evidence including studies rated as 2++, directly applicable to the target population, and demonstrating overall consistency of results; or
Extrapolated evidence from studies rated as 1++ or 1+
See all recommendation gradingsGrade B

HCV genotyping should be undertaken if antiviral therapy is being considered.

Grade D
Evidence level 3 or 4; or
Extrapolated evidence from studies rated as 2+
See all recommendation gradingsGrade D

Following an isolated acute percutaneous exposure to blood infected, or strongly suspected of being infected, with HCV, healthcare workers should be offered HCV RNA testing at 6, 12 and 24 weeks and anti-HCV testing at 12 and 24 weeks.

Grade D
Evidence level 3 or 4; or
Extrapolated evidence from studies rated as 2+
See all recommendation gradingsGrade D

Good practice points

• The sign guidelines
  • About the guideline
  • Testing & Diagnosis
    • Quick reference guide
    • Clinical and cost effective testing for HCV
    • HCV diagnostic testing
    • Testing Algorithm
    • HCV testing in children and infants
  • Referral
  • Management
  • Treatment
• Research & resources
• Action Plan
• Patients and carers
• Useful contacts
• Information leaflets