Precore and Basal Core Promoter Hepatitis B Virus (HBV) Variants Are Present From a Young Age and Differ Across HBV Genotypes

Background and Aims Hepatitis B virus (HBV) precore (PC) and dual basal core promoter (BCP) mutations halt and down‐regulate hepatitis B e antigen (HBeAg) production respectively. PC mutation is rarely associated with HBV genotype A. We sought to examine the association of these variants with HBV ge...

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Veröffentlicht in:Hepatology (Baltimore, Md.) Md.), 2021-05, Vol.73 (5), p.1637-1651
Hauptverfasser: Ganova‐Raeva, Lilia, Wang, Junyao, Mogul, Douglas, Lisker‐Melman, Mauricio, Chang, Kyong‐Mi, Janssen, Harry L.A., Wahed, Abdus S., Lok, Anna S., Niu, Jianghe, Nasser, Imad, Rusibamayila, Nifasha, Stahler, Alisha C, Stadheim, Linda, Lake, John, Riggs, Shannon M, Rushing, Kathryn, Cerkoski, Jacki, Shaw, Debra DeMarco, Noureldin, Seham, Kaznowski, Diana, Vladutu, Doinita, Cerocchi, Orlando, Bass, Sheila, Rodgers‐Augustyniak, Laurie A, Montanye, Shirley, Peters, Marion, Davis, Rayshawnda, Kuras, Romuald, Ayala, Claudia, Lau, Ivy, Podolskaya, Veronika, von Bakonyi, Anna, DeVole, Nata, Feier, Natasha, Feier, Joel, Oberhelman, Kelly, Kaza, Sravanthi, Huddleston, Leslie, Wong, Richmond, Marsh, Tiffany, Cardona, Danielle, Hofmann, Charlotte, Wolfstone, Alycia, Mooney, Jody, Cooper, Kara L, Imteyaz, Hejab, Oshima, Kiyoko, Kafka, Kim, Islam, Naureen, Fryzek, Nancy, Morris, Nevitt, Hoofnagle, Jay H, Doo, Edward, Torrance, Rebecca J, Valiga, Mary E, Keith, James, Betts, Michael, Montaner, Luis J, Averbach, Frani, Hardison, Regina, Lalama, Christina, Lawlor, Sharon, Lin, Hsing‐Hua S, Lombardero, Manuel, Pelesko, Andrew, Stoliker, Donna, Zhao, Qian, Roberts, Lewis R, Hassan, Mohamed A, Schwarzenberg, Sarah Jane, Di Bisceglie, Adrian M, Wong, David K, Feld, Jordan, Patel, Keyur, Ling, Simon C, Lee, William M, Murakami, Carol S, Perrillo, Robert, Do, Son, Han, Steven‐Huy B, Tran, Tram T, Terrault, Norah A, Khalili, Mandana, Rosenthal, Philip, Fontana, Robert J, Younoszai, Barak, Fried, Michael W, Muir, Andrew, Darling, Jama M, Carithers, Robert C, Shuhart, Margaret, Kowdley, Kris V, Murray, Karen F, Sterling, Richard K, Ghany, Marc G, Jake Liang, T, King, Wendy C, Kleiner, David
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Sprache:eng
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Zusammenfassung:Background and Aims Hepatitis B virus (HBV) precore (PC) and dual basal core promoter (BCP) mutations halt and down‐regulate hepatitis B e antigen (HBeAg) production respectively. PC mutation is rarely associated with HBV genotype A. We sought to examine the association of these variants with HBV genotypes, age, and HBeAg status in a racially diverse population in North America. Prospective study included 1,036 (808 adults, 228 children) participants in the Hepatitis B Research Network. PC and BCP variants were determined by Sanger sequencing, and dominant HBV species (>50%) were reported. Approach and Results Median age was 36.3 years (range, 2‐80), 44.6% HBeAg(+), 74.2% Asians, 13.3% black, and 9.7% white. The dominant PC variant was present in 29.4% participants, including 20 with subgenotype A1 or A2. Seventeen of 20 participants with genotype A and PC had a compensatory C1858T mutation. In the HBeAg(+) cohort, the prevalence of PC and/or BCP variants increased from 14.4% in the first two decades to 51% after 40 years of age. Among those aged 2‐18, 52% and 83% with dominant PC and BCP variants were HBeAg(+) compared to 3.8% and 29% in the >40 years age group. HBeAg clearance rates were significantly higher for those with dominant PC or BCP variants: 24.4 and 15.0 per 100 person‐years compared to 6.0 in wild‐type HBV (P 
ISSN:0270-9139
1527-3350
DOI:10.1002/hep.31506