Hepatitis D laboratory findings: Difference between revisions
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* Anti-HDV [[antibodies]] develop late in acute phase and usually decline after infection to subdetectable levels | * Anti-HDV [[antibodies]] develop late in acute phase and usually decline after infection to subdetectable levels | ||
* If HDAg is detectable early during [[infection]], it disappears as anti-HDV appears | * If HDAg is detectable early during [[infection]], it disappears as anti-HDV appears | ||
* All markers of [[viral replication]] disappear in early [[convalescence]], and both [[IgM]] and [[IgG]] anti-HD disappear within months to years after recovery | * All markers of [[viral replication]] disappear in early [[convalescence]], and both [[IgM]] and [[IgG]] anti-HD disappear within months to years after recovery<br> | ||
[[Image:HDV_Coinfection.png|none|thumb|600px|''[http://www.cdc.gov Slide from the Center for Disease Control and Prevention(CDC)]''<ref name="CDC">{{Cite web | title = Center for Disease Control and Prevention (CDC) | url = http://www.cdc.gov}}</ref>]] | |||
===HBV-HDV Superinfection=== | ===HBV-HDV Superinfection=== | ||
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* Progression to chronicity is associated with persisting high levels of [[IgM]] anti-HD and [[IgG]] anti-HD | * Progression to chronicity is associated with persisting high levels of [[IgM]] anti-HD and [[IgG]] anti-HD | ||
* HDAg and HDV RNA remain detectable in [[serum]] and [[liver]] | * HDAg and HDV RNA remain detectable in [[serum]] and [[liver]] | ||
* [[Viremia]] is associated with active [[liver disease]] | * [[Viremia]] is associated with active [[liver disease]]<br> | ||
[[Image:HDV_Superinfection.png|none|thumb|600px|''[http://www.cdc.gov Slide from Center for Disease Control and Prevention(CDC)]''<ref name="CDC">{{Cite web | title = Center for Disease Control and Prevention (CDC) | url = http://www.cdc.gov}}</ref>]] | |||
==Viral Dominance== | ==Viral Dominance== | ||
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==References== | ==References== | ||
{{reflist|2}} | {{reflist|2}} | ||
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{{WS}} | |||
[[Category:Hepatitis|D]] | [[Category:Hepatitis|D]] | ||
[[Category:Viruses]] | [[Category:Viruses]] | ||
[[Category:Disease]] | [[Category:Disease]] | ||
[[Category:Gastroenterology]] | |||
[[Category:Emergency mdicine]] | |||
[[Category:Up-To-Date]] | |||
[[Category:Infectious disease]] | [[Category:Infectious disease]] | ||
[[Category: | [[Category:Hepatology]] | ||
Latest revision as of 22:06, 29 July 2020
Hepatitis D |
Diagnosis |
Treatment |
Hepatitis D laboratory findings On the Web |
American Roentgen Ray Society Images of Hepatitis D laboratory findings |
Risk calculators and risk factors for Hepatitis D laboratory findings |
Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Jolanta Marszalek, M.D. [2] João André Alves Silva, M.D. [3]
Overview
The diagnosis of hepatitis D is made by the detection of HDV RNA in circulation, with RT-PCR. The levels of HBsAg may be used during treatment to evaluate the response, and determine the duration of therapy. After recovery, markers of HDV infection, such as IgM and IgG antibodies disappear within months. Liver biopsy is indicated in HDV RNA positive patients, to assess the stage of liver disease. Findings in liver biopsy are similar to those observed in HBV infection. Coinfection with HIV and HCV should be ruled out in HDV infected patients. Serologic markers such as HDV RNA, HDAg, and IgM and IgG anti-HD antibodies may persist for longer periods in chronic hepatitis D.
Laboratory Findings
Hepatitis D should be considered in any individual who is HBsAg positive or that has evidence of recent HBV infection. The diagnosis of acute hepatitis D is made after evaluation of serologic tests for the virus. Persons infected with HDV develop anti-HDV antibodies. Accordingly, every individual with an HBsAg positive test result, should be studied for the presence of anti-HDV IgG antibodies.[1] Positive HDV antibodies do not necessarily represent active infection, since HDV RNA might have been cleared away (recovery), while the antibodies may remain in circulation for longer periods of time.[2][3] Even in cases of HBsAg seroconversion, or liver transplant, anti-HDV antibodies may be detected during several years.[3][4]
During therapy, the decrease in the levels of HBsAg may be used to determine the duration of treatment. It is also important to determine the levels of HBV DNA, in order to assess the need for an HBV polymerase inhibitor.[5]
The active form of the HDV infection was initially diagnosed by the detection of anti-HDV IgM antibodies. However, today acute active infection is confirmed with real-time PCR, by detecting serum HDV RNA.[6]
Patients presenting with liver disease, following HDV infection, should be tested for anti-HDV IgM antibodies, even when the HDV RNA test is negative. This is due to the fact that the hepatitis D virus shows genome variability, which might lead to false-negative results.[7][8] Although the levels of HDV RNA in the serum do not correlate with the stage of the disease, or liver fibrosis, the HDV RNA quantification may be used to evaluate the response to the antiviral therapy.[9]
According to different studies, it hasn't been noted an association between HDV RNA levels, HBsAg titre, liver test results and the stage of liver disease. Therefore, liver biopsy remains an important tool to assess pathological changes in liver histology.[1]
Each of the markers of HDV infection, including IgM and IgG antibodies, disappears within months after recovery. In chronic hepatitis D, HDV RNA, HDAg, and IgM and IgG anti-HD antibodies persist for longer periods.[10]
Below is a diagram representing the assessment of patients with hepatitis D:
Diagnostic Markers
The table below describes the significance of diagnostic markers in HDV infection. [1]
Diagnostic Markers | Significance |
---|---|
Anti-HDV IgG antibody |
|
Anti-HDV IgM antibody |
|
HDV RNA |
Qualitative
Quantitative
|
HBsAg |
Qualitative
Quantitative
|
HBeAg |
|
HBV DNA |
Quantitative
|
ALT |
|
Liver Biopsy:
- Liver biopsy is not indicated for the routine diagnosis of acute hepatitis D, unless serologic diagnosis is inconclusive. Liver biopsy is indicated when patients are HDV RNA positive, in which case, it will help assess the severity of liver disease.[1]
- Due to the inability of noninvasive markers of fibrosis to predict the correct stage of the disease, liver biopsy should be performed in patients with hepatitis D.[2]
- Findings are similar to those observed in HBV infection. Lymphocytic infiltrates may be observed in hepatocytes.
- Immunohistochemical staining may be positive for HDV antigen with suppression of HBsAg in case of superinfection.
Acute HBV-HDV Coinfection
Acute coinfection of HDV with HBV is characterized by:[11]
- Appearence of HBsAg, HBeAg and HBV DNA in serum during incubation
- Appearence of anti-HBc at onset of clinical disease
- Appearence of IgM anti-HD, HDV RNA, HDAg in serum
- Anti-HDV antibodies develop late in acute phase and usually decline after infection to subdetectable levels
- If HDAg is detectable early during infection, it disappears as anti-HDV appears
- All markers of viral replication disappear in early convalescence, and both IgM and IgG anti-HD disappear within months to years after recovery
HBV-HDV Superinfection
Superinfection of HDV with HBV is characterized by:[11]
- Persistent HDV infection
- HDV viremia appears in serum during preacute phase
- High titres of IgM and IgG anti-HDV are detectable in acute phase, persisting indefinitely
- Titre of HBsAg declines when HDAg appears in serum
- Progression to chronicity is associated with persisting high levels of IgM anti-HD and IgG anti-HD
- HDAg and HDV RNA remain detectable in serum and liver
- Viremia is associated with active liver disease
Viral Dominance
The simultaneous presence of HBV, HDV and sometimes HCV, influences the serologic findings in each patient. Infection by HDV and HBV (either in coinfection or superinfection) suppresses the replication of HBV genome.[1] Patients coinfected with HDV often show:[13][14][15]
Once infection with HDV is cleared, either by host's immune system or with interferon treatment, replication of HBV will then be reactivated.[16]
In prolonged infections, both viruses may become dominant. In which case, serologic levels of HBV DNA and HDV RNA may fluctuate.[17][18]
In patients infected with HCV, along with HDV and HBV, the HDV is the dominant virus. It is able not only to suppress the replication of HBV, but also to inhibit the replication of HCV.[1]
Coinfection with HIV
Patients infected with the HDV should be screened for concomitant infection with HIV.[13][15]
References
- ↑ 1.0 1.1 1.2 1.3 1.4 1.5 Hughes SA, Wedemeyer H, Harrison PM (2011). "Hepatitis delta virus". Lancet. 378 (9785): 73–85. doi:10.1016/S0140-6736(10)61931-9. PMID 21511329.
- ↑ 2.0 2.1 Wedemeyer H, Manns MP (2010). "Epidemiology, pathogenesis and management of hepatitis D: update and challenges ahead". Nat Rev Gastroenterol Hepatol. 7 (1): 31–40. doi:10.1038/nrgastro.2009.205. PMID 20051970.
- ↑ 3.0 3.1 Paraná R, Kay A, Molinet F, Viana S, Silva LK, Salcedo JM; et al. (2006). "HDV genotypes in the Western Brazilian Amazon region: A preliminary report". Am J Trop Med Hyg. 75 (3): 475–9. PMID 16968924.
- ↑ Mederacke I, Filmann N, Yurdaydin C, Bremer B, Puls F, Zacher BJ; et al. (2012). "Rapid early HDV RNA decline in the peripheral blood but prolonged intrahepatic hepatitis delta antigen persistence after liver transplantation". J Hepatol. 56 (1): 115–22. doi:10.1016/j.jhep.2011.06.016. PMID 21762665.
- ↑ 5.0 5.1 Heidrich B, Manns MP, Wedemeyer H (2013). "Treatment options for hepatitis delta virus infection". Curr Infect Dis Rep. 15 (1): 31–8. doi:10.1007/s11908-012-0307-z. PMID 23242761.
- ↑ Mederacke I, Bremer B, Heidrich B, Kirschner J, Deterding K, Bock T; et al. (2010). "Establishment of a novel quantitative hepatitis D virus (HDV) RNA assay using the Cobas TaqMan platform to study HDV RNA kinetics". J Clin Microbiol. 48 (6): 2022–9. doi:10.1128/JCM.00084-10. PMC 2884474. PMID 20351206.
- ↑ Manesis EK, Schina M, Le Gal F, Agelopoulou O, Papaioannou C, Kalligeros C; et al. (2007). "Quantitative analysis of hepatitis D virus RNA and hepatitis B surface antigen serum levels in chronic delta hepatitis improves treatment monitoring". Antivir Ther. 12 (3): 381–8. PMID 17591028.
- ↑ Le Gal F, Gordien E, Affolabi D, Hanslik T, Alloui C, Dény P; et al. (2005). "Quantification of hepatitis delta virus RNA in serum by consensus real-time PCR indicates different patterns of virological response to interferon therapy in chronically infected patients". J Clin Microbiol. 43 (5): 2363–9. doi:10.1128/JCM.43.5.2363-2369.2005. PMC 1153793. PMID 15872267.
- ↑ Zachou K, Yurdaydin C, Drebber U, Dalekos GN, Erhardt A, Cakaloglu Y; et al. (2010). "Quantitative HBsAg and HDV-RNA levels in chronic delta hepatitis". Liver Int. 30 (3): 430–7. doi:10.1111/j.1478-3231.2009.02140.x. PMID 19840253.
- ↑ Webster, Robert (1996). Encyclopedia of virology plus. San Diego: Academic. ISBN 0120001039.
- ↑ 11.0 11.1 "Hepatitis D" (PDF).
- ↑ 12.0 12.1 "Center for Disease Control and Prevention (CDC)".
- ↑ 13.0 13.1 Cross TJ, Rizzi P, Horner M, Jolly A, Hussain MJ, Smith HM; et al. (2008). "The increasing prevalence of hepatitis delta virus (HDV) infection in South London". J Med Virol. 80 (2): 277–82. doi:10.1002/jmv.21078. PMID 18098143.
- ↑ Sagnelli E, Coppola N, Scolastico C, Filippini P, Santantonio T, Stroffolini T; et al. (2000). "Virologic and clinical expressions of reciprocal inhibitory effect of hepatitis B, C, and delta viruses in patients with chronic hepatitis". Hepatology. 32 (5): 1106–10. doi:10.1053/jhep.2000.19288. PMID 11050062.
- ↑ 15.0 15.1 Heidrich B, Deterding K, Tillmann HL, Raupach R, Manns MP, Wedemeyer H (2009). "Virological and clinical characteristics of delta hepatitis in Central Europe". J Viral Hepat. 16 (12): 883–94. doi:10.1111/j.1365-2893.2009.01144.x. PMID 19566789.
- ↑ Castelnau C, Le Gal F, Ripault MP, Gordien E, Martinot-Peignoux M, Boyer N; et al. (2006). "Efficacy of peginterferon alpha-2b in chronic hepatitis delta: relevance of quantitative RT-PCR for follow-up". Hepatology. 44 (3): 728–35. doi:10.1002/hep.21325. PMID 16941695.
- ↑ Schaper M, Rodriguez-Frias F, Jardi R, Tabernero D, Homs M, Ruiz G; et al. (2010). "Quantitative longitudinal evaluations of hepatitis delta virus RNA and hepatitis B virus DNA shows a dynamic, complex replicative profile in chronic hepatitis B and D." J Hepatol. 52 (5): 658–64. doi:10.1016/j.jhep.2009.10.036. PMID 20346531.
- ↑ Wedemeyer H (2010). "Re-emerging interest in hepatitis delta: new insights into the dynamic interplay between HBV and HDV". J Hepatol. 52 (5): 627–9. doi:10.1016/j.jhep.2010.02.001. PMID 20334947.