Limitations of HBsAg testing in the screening of blood donors Wolfram H. Gerlich Institute of Medical Virology University Giessen, Germany SoGAT XVI Langen.

Slides:

Advertisements

Similar presentations

Hemolytic Disease of the Newborn Case #3

Advertisements

Treatment appropriate Normal or minimal hepatitis Chronic hepatitis Normal or inactive hepatitis Progressive fibrosis Cirrhosis HCC HBeAg Anti-HBe HBV.

NPW Microbiology Antenatal Presentation

Use of avidity reagent. Panbio Buffered Avidity Reagent Mild protein-denaturing solution that may be useful in differentiating recent infections from.

Impact of Testing Strategies to Reduce Transmission Risk for HBV Ravi Reddy, M Vermeulen South African National Blood Service (SANBS) 29 July 2013.

Diagnosis of HIV Infection

Hepatitis B: Epidemiology

F. Kourgia, M. Vini, E. Zervou

HEPATITIS B MARKERS AND VACCINE

Screening for HBsAg and Anti-HBc in North American Blood Donors John Saldanha, Roche Molecular Systems SoGAT XXI, May, 2009, Brussels, Belgium.

OnSite HAV IgM Rapid Test Upgraded to Revision H for Better Sensitivity CTK-MK-PPT-R0090 Rev 1.0.

Immunohematology (Blood Bank) CLS 245. What is Immunohematology? It is the study of Antigen-Antibody reaction as they relate to blood disorder.

HEPATITIS A VIRUS Week Response Clinical illness ALT IgM IgG HAV in stool Infection Viremia EVENTS IN HEPATITIS A VIRUS INFECTION.

21 August 2015 Samreen Ijaz Virus Reference Department Health Protection Agency Indigenous HEV infection in the UK: a hazard for blood donation?

Pooled Source Plasma NAT for HIV-1 An Update from the Bayer HIV-1 IND Study Barbara Masecar Bayer Corporation Raleigh, NC Blood Products Advisory Committee.

Faculty of Allied Medical Sciences Clinical Immunology & Serology Practice (MLIS 201)

BioLife Plasma Services Experience with HBV NAT Testing

And the order changeth …. Evolving protocols for TTI testing

Reentry for Donors Deferred Based on Anti-HBc Test Results November 3, 2005 BPAC Meeting FDA/CBER/OBRR/DETTD.

FDA’s Current Considerations of Parvovirus B19 Nucleic Acid Testing (NAT) Mei-ying W. Yu, PhD Division of Hematology CBER/FDA Extraordinary SoGAT Meeting.

HBV-DNA detection by hybridization assay in the serum of anti-HBe positive HBV carriers HBV-DNA + Chronic Hepatitis 11/19 58% 11/14 79% Bonino /13.

Research on HBV in SCDC Xi Zhang, Ye Lu Shanghai Municipal Center for Disease Control and Prevention May, 2008.

Michael Chudy, Paul-Ehrlich-Institut SoGAT XVIII, Bethesda MD

INTRODUCTION High incidence rate High incidence rate Do not grow in the laboratory Do not grow in the laboratory Discovered in 1964 Discovered in 1964.

Hepatitis B Patricia D. Jones, M.D. November 13, 2009.

Blood types are identified by certain antigens in red blood cells Type A RBC’s carry the “A” antigen Type B carry the “B” antigen Type AB both “A” and.

Parvovirus B19 NAT Screening and Infectivity Mei-ying W Yu CBER/FDA SoGAT XVI Paul Ehrlich Institut July 03, 2003.

Establishment of the 1st WHO International Standard for Detection of Antibodies to Hepatitis B Virus Core Antigen (anti-HBc) SoGAT XXI 29 May 2009 Dr.

CHRONIC HEPATITIS B SEROLOGY. Antigens HBsAg -Found on the surface of the intact virus and in serum as unattached particles -Earliest detectable marker.

Standardisation of P. falciparum HBV, HCV and NAT Sally Baylis, NIBSC SoGAT XVIII.

21th VHPB Meeting on “Prevention of viral hepatitis in Italy: lessons learnt and the way forward” Catania, 7-8 november 2002 Impact of HBV S-gene mutants.

1 B19 Testing of Plasma for Fractionation: Current Thinking Mei-ying W Yu, PhD Division of Hematology CBER/FDA SoGAT XVII May 26-27, 2004.

SoGAT, Berne 2006BTS SRC Berne Ltd. Evaluation of the Procleix TIGRIS System at the Blood Transfusion Service Berne Ltd. Dr. Martin Stolz.

Active B19 virions production in hepatoblastoma and hepatocarcinoma cell lines: amplification and genomic stability. Op de beeck A. 1, Draps M.-L. 1, Baurin.

Anti-B19 screening for safe cellular blood products for at–risk patients SoGAT XVIII, USA, May 24-25th, 2005 Harry Bos on behalf of Project Group Parvo.

HBV screening Further improvement of blood safety based on the knowledge deduced from the results on analysis of the donor’s sera positive for HBV DNA.

Blood Products & related Biologicals: SoGAT, 28 May 09 1 |1 | Dr Ana Padilla, Blood Products & related Biologicals Essential Medicines and Pharmaceutical.

Viral load, does it matter? Probably so. Tim Pruett, MD University of Virginia.

GI BLOCK; This practical class is designed and Prepared by: Prof. Samy A. Azer (Medical Education) Dr. Ali Somily (Microbiology) Prof. Abdul Mageed.

Natural history of HBV infection (adapted from Torbenson Lancet 2003) Chronic infection Healthy carriage Recovery occult DNA Anti-HBe Anti-HBc Immune response.

Management of Donors and Units that Test HBV NAT Positive: Current Considerations July 21, 2005 BPAC Meeting Robin Biswas, M.D. FDA/CBER/OBRR/DETTD.

Hepatitis B The Basics David Wong University of Toronto March 2005.

Hepatitis Virus. Primary members HAV HBV HCV HDV HEV.

CURRENT HEALTH PROBLEMS IN STUDENT'S HOME SOUNTRIES HEPATITIS B IN MALAYSIA MOHD ZHARIF ABD HAMID AMINUDDIN BAKI AMRAN.

Ro / BSD Hessen Institut für Transfusionsmedizin SoGAT XVII, Paris, Paris 2004 B19 Overview of Testing for Blood Banks W. Kurt Roth Red Cross Blood Transfusion.

Viral Hepatitis Program Management of Babies Born to HBsAg- Positive Mothers Vickie Weeast Perinatal Hepatitis B Case.

E B—Anti-HBc Chart 1 10/2004 Anti-HBc Testing and Donor Reentry Results of a Pilot Study Susan L. Stramer, Ph.D. American Red Cross Blood Products.

Evaluation of Hepatitis B surveillance system in Armenia, 2014 AUTHORS Karine Gevorgyan Lusine Paronyan Shushan Sargsyan Artavazd Vanyan NCDC, Armenia.

Ro / BSD Hessen Institut für Transfusionsmedizin SoGAT XVI, Langen 3 rd July 2003 Immediate Parvo B19 NAT testing of pooled donor samples: logistics and.

Hepatitis B Fahad Alanazi.

Isolated Hepatitis B Core Antibody

Serologic markers and molecular epidemiology of HBV from an HIV infected cohort from Cameroon Tshifhiwa Magoro 1, Emmaculate Nongpang 2, Lufuno Mavhandu.

Clinicaloptions.com/hepatitis Using Virologic and Serologic Tests in the Management of Hepatitis B Diagnose chronic HBV infection When in slideshow mode,

Abbott Laboratories ConfidentialPage 1 Update on West Nile Virus George J. Dawson, Ph.D. Abbott Laboratories.

MICROBIOLOGY IRS. Gastroenteritis 1) Major cause of infantile death 2) Feacal-oral transmission 3) Gastroenteritis cause dehydration 4) 50 % of all causes.

BARBARA DOMMERT-BRECKLER RN BSN QUALITY IMPROVEMENT DIRECTOR NORTHWEST RENAL NETWORK Hepatitis B: Anti-bodies, Antigens and Immunity 7/9/2016.

Hepatitis B virus infection in renal transplant recipients

Publication stage: In Press Accepted Manuscript

VIRAL DISEASES OF LIVER DR.JEYAKUMAR NELSON UNIT OF MICROBIOLOGY MBBS -BATCH 17.

In The Name of God.

MICROBIOLOGY PRACTICAL

Characterisation of HBV DNA in reference preparations

Update on WHO Projects.

Volume 137, Issue 4, Pages (October 2009)

HBV Infection: Some Sobering Facts

HBV/G Infection of an Apheresis Donor

Figure 2 Distribution of markers of active HBV infection

SoGAT meeting XXI May (2009), Brussels, Belgium

Presentation transcript:

Limitations of HBsAg testing in the screening of blood donors Wolfram H. Gerlich Institute of Medical Virology University Giessen, Germany SoGAT XVI Langen 3rd July 2003

Problems of HBsAg tests Detection limit difficult to define Unclear HBsAg unit –WHO unit not often applied new standard preparation in planning –Paul Ehrlich Inst. (PEI) unit since 1975 Standard and units changed over the years –Nanogram units of test producers too high and discordant –Old PEI unit = 1 ng active HBsAg = 2 WHO unit HBV genotypes react differently Different HBsAg preparations react differently

Anti-a antiserum raised with subsequent injections of genotypes A, D, and C

Problems of HBsAg tests HBV genotypes react differently –WHO provides only standard for genotype A –Worldwide are genotypes B,C und D predominant –Genotype F was not detected for years with some tests Insufficient sensitivity –Best possible ELISA detects 10pg HBsAg/ml –Or 10 6 HBV particles/mL –if excessive HBsAg is not present in very early phase HBsAg is highly variable under immune selection –after post exposure immunisation –during reactivation Consequence: false negative results

Problems of HBsAg tests HBV genotypes react differently –WHO standard only genotype A –Worldwide genotypes B,C und D predominant –Genotype F not detected for years with some tests Insufficient sensitivity even for genotype A –Best possible ELISA detects 10pg HBsAg/ml –This corresponds to 10 6 HBV particles/mL –if excessive HBsAg is not present in early phase HBsAg is highly variable under immune selection –after post exposure immunisation –during reactivation Consequence: false negative results

HBsAg-negative, HBV-infectious blood donation : the donor 16th July 2002 –HBsAg in AxSym negative 17th September 2002 –AxSym (Abbott) positive s/co=2.4 –Enzygnost (Dade Behring) negative s/co=0.8 21st September 2002 –Enzygnost positive s/co=1.9 –HBV-DNA positive 3200 ge/mL –Anti-HBc total antibody and IgM and HBeAg negative Meisel et al, submitted

HBsAg-negative, HBV-infectious blood donation: the recipient 22. July 2002 –receives erythrocyte concentrate from the pre- seroconversion donation –HBsAg and anti-HBc negative 19. November 2002 –HBsAg positive, HBV DNA 1.8x10 10 genomes/mL –No hepatitis, develops persistent viremia –anti-HBc still negative, later positive HBV DNA sequence of donor and recipient –identical, genotype A, in Germany predominant variant –S-gene without mutations

HBsAg-negative, HBV-infectious blood donation : the donor 16th July 2002 –HBsAg in AxSym negative –HBV DNA ca 2000 genomes/mL 17th September 2002 –AxSym (Abbott) positive s/co=2.4 –Enzygnost (Dade Behring) negative s/co=0.8 21st September 2002 –Enzygnost positive s/co=1.9 –HBV-DNA 3200 genomes/mL –Anti-HBc total antibody and IgM and HBeAg negative 12th May 2003, no hepatitis noticed –HBsAg negative, HBV DNA negative –anti-HBc and anti-HBs positive The donor was >60 days infectious without detectable HBsAg Meisel et al, submitted

Superiority of minipool nucleic acid amplification technology for hepatitis B virus over chemiluminescence immunoassay* for hepatitis B surface antigen screening Minegishi et al Japanese Red Cross Vox sang :287 >11 million donations tested in pools of 50 Prescreened with RPHA for HBsAg* and high anti-HBc 181 HBV DNA positive donations found (early phase) copies/mL** N < – > total *Abbotts Prism *ca positive**Taqman

Superiority of minipool nucleic acid amplification technology for hepatitis B virus over chemiluminescence immunoassay* for hepatitis B surface antigen screening Minegishi et al Japanese Red Cross Vox sang :287 >11 million donations tested in pools of 50 Prescreened with RPHA for HBsAg* and high anti-HBc 181 HBV DNA positive donations found (early phase) copies/mL** N HBsAg* neg. < – > total *Abbotts Prism *ca positive**Taqman

Gaps in detection of early phase HBV infection: potential solutions Ignore because of rarity –Only 1.4% of infected donors were missed –In Japan ca 1.6 in donations –much less in Europe and North America 0.05 / in Germany (Roth et al. Transfusion 42:869) Highly sensitive NAT screening –Detection limit? Costs? –Cannot replace HBsAg or anti-HBc testing Vaccination –Costs? Management? Acceptance? Nonresponders? –Could replace NAT and repeat anti-HBc testing –protection against HBV Long lasting in donors (active) Short term in recipient (passive) Escape mutants

Problems of HBsAg tests HBV-Genotypes react differently –WHO standard only genotype A –Worldwide genotypes B,C und D predominant –Genotype F not detected for years with some tests Insufficient sensitivity –Best possible ELISA detects 10pg HBsAg/ml –Or 10 6 HBV particles/mL –if excessive HBsAg is not present in very early phase HBsAg is highly variable under immune selection –after post exposure immunisation –during reactivation Consequence: false negative results

Reactivation of hepatitis B during immunosuppressive lymphoma therapy Patient from Lebanon –15 years ago resolved hepatitis B –Before therapy: anti-HBc +, anti-HBs >1000 IU/L, HBsAg - –Receives in 2002 for four months chemotherapy (CHOP), –Thereafter two months anti-B cell mab Rituximab Develops acute hepatitis B –4x10 9 /mL HBV genomes, anti-HBs 880 Iu/L –Patient dies inspite Lamivudine therapy after 2 weeks HBsAg in AxSym highly positive, in a 2nd test negative –PEI finds 2 further out of 5 tests which fail –sample in one further test weakly +, but not inhibitable HBsAg sequence shows 4 escape mutations –L110R, Y134S, P142L, D144A T.Westhoff et.al, blood, in press

R K S A R Rituximab associated escape mutant

Reactivation of hepatitis B during immunosuppressive lymphoma therapy Patient from Lebanon –15 years ago resolved hepatitis B –Before therapy: anti-HBc +, anti-HBs >1000 IU/L, HBsAg - –Receives in 2002 for four months chemotherapy (CHOP), –Thereafter two months anti-B cell mab Rituximab Develops acute hepatitis B –4x10 9 /mL HBV genomes, anti-HBs 880 IE/L –Patient dies inspite Lamivudine therapy after 2 weeks HBsAg in AxSym +++, in a 2nd test negative –PEI finds 2 further out of 5 tests which fail –sample in one further test weakly +, but not inhibitable HBsAg sequence shows 4 escape mutations –L110R, Y134S, P142L, D144A Serum before therapy: 50 Ge/mL, same mutations T.Westhoff et.al, blood, in press

Summary All questions open Sorry for that Thank you!