Background. Rapid and early emergence of clinically significant LAM resistance is thought to be unlikely during the first year of treatment, and as a result LAM is thought to be a reasonable choice as a first line agent for prophylaxis during chemotherapy. Aim. To report fatal HBV reactivation despite appropriate LAM prophylaxis in two previously treatment-naive individuals undergoing R-CHOP chemotherapy. Case Presentation. Case 1 is a 65-year-old man with chronic HBV infection: HBeAg-negative, HBV DNA 6.65E5?IU/mL, ALT 43?IU/L, and Fibroscan 4.4?kPa, consistent with F0, who was diagnosed with lymphoma that was treated with R-CHOP and LAM prophylaxis. HBV DNA fell to 2.18E1?IU/mL within 2 months of starting LAM. Four months after chemotherapy, despite ongoing LAM of 7-month duration with confirmed adherence, severe asymptomatic hepatitis was noted during routine monitoring with ALT 1019?IU/L, HBeAg negative, HBV DNA 1.43E7?IU/mL, and genotyping confirmed L80I and M204I mutations. He died 14 days after flare diagnosis despite a switch to tenofovir (HBV DNA had fallen to 1.94E5?IU/mL 2 weeks after starting tenofovir). Case 2 is a 50-year-old man who was found to have HBeAg-negative hepatitis B, ALT 37?IU/L, and no clinical features of cirrhosis (platelets 283, APRI 0.19) after lymphoma diagnosis. Lymphoma was treated with R-CHOP and LAM prophylaxis. Pretreatment HBV DNA was not done but was 8.90E4?IU/mL 3 weeks after starting LAM and 3.96E3?IU/mL 3 months after starting LAM. Two months after chemotherapy, despite ongoing LAM of 7-month duration with confirmed adherence, severe symptomatic hepatitis presenting with jaundice, abdominal pain, and confusion was noted. ALT 902?IU/L, HBeAg negative, HBV DNA 1.02E8?IU/mL, and genotyping confirmed L80I, M80V, and M204V/S mutations. He died 3 days after flare diagnosis despite the addition of tenofovir. Conclusion. Lamivudine should not be used for prophylaxis of patients with chronic hepatitis B with detectable HBV DNA undergoing chemotherapy with rituximab containing cytotoxic chemotherapy even if they have never had exposure to lamivudine in the past. In this setting, lamivudine failure due to resistance can develop quickly leading to liver failure that cannot be salvaged with tenofovir. Whether LAM is safe for prophylaxis with rituximab-based cytotoxic chemotherapy for patients with undetectable HBV DNA is unknown, but agents with a high barrier to resistance may be preferable. 1. Introduction Reactivation of hepatitis B infection has been reported in 20%–50% of patients during conventional chemotherapy and up
References
[1]
S. Kusumoto, Y. Tanaka, R. Ueda, and M. Mizokami, “Reactivation of hepatitis B virus following rituximab-plus-steroid combination chemotherapy,” Journal of Gastroenterology, vol. 46, no. 1, pp. 9–16, 2011.
[2]
A. M. Evens, B. D. Jovanovic, Y.-C. Su et al., “Rituximab-associated hepatitis B virus (HBV) reactivation in lymphoproliferative diseases: metaanalysis and examination of FDA safety reports,” Annals of Oncology, vol. 22, no. 5, pp. 1170–1180, 2011.
[3]
U. Zurawska, L. Hicks, G. Woo, C. Bell, M. Krahn, et al., “Hepatitis B virus screening before chemotherapy for lymphoma: a cost-effectiveness analysis,” Journal of Clinical Oncology, vol. 30, no. 26, pp. 3167–3173, 2012.
[4]
C. M. Weinbaum, E. E. Mast, and J. W. Ward, “Recommendations for identification and public health management of persons with chronic hepatitis B virus infection,” Hepatology, vol. 49, no. 5, pp. S35–S44, 2009.
[5]
L. H. Katz, A. Fraser, A. Gafter-Gvili, L. Leibovici, and R. Tur-Kaspa, “Lamivudine prevents reactivation of hepatitis B and reduces mortality in immunosuppressed patients: systematic review and meta-analysis,” Journal of Viral Hepatitis, vol. 15, no. 2, pp. 89–102, 2008.
[6]
R. Loomba, A. Rowley, R. Wesley et al., “Systematic review: the effect of preventive lamivudine on hepatitis B reactivation during chemotherapy,” Annals of Internal Medicine, vol. 148, no. 7, pp. 519–528, 2008.
[7]
A. S. F. Lok and B. J. McMahon, “Chronic hepatitis B: update 2009,” Hepatology, vol. 50, no. 3, pp. 661–662, 2009.
[8]
N. Leung, “Clinical experience with lamivudine,” Seminars in Liver Disease, vol. 22, no. 1, pp. 15–21, 2002.
[9]
F. Von Weizs?cker, “Management of chronic hepatitis B,” Praxis, vol. 94, no. 16, pp. 649–652, 2005.
[10]
A. M. Pelizzari, M. Motta, E. Cariani, P. Turconi, E. Borlenghi, and G. Rossi, “Frequency of hepatitis B virus mutant in asymptomatic hepatitis B virus carriers receiving prophylactic lamivudine during chemotherapy for hematologic malignancies,” Hematology Journal, vol. 5, no. 4, pp. 325–328, 2004.
[11]
A.-L. Cheng, C. A. Hsiung, I.-J. Su et al., “Steroid-free chemotherapy decreases risk of hepatitis B virus (HBV) reactivation in HBV-carriers with lymphoma,” Hepatology, vol. 37, no. 6, pp. 1320–1328, 2003.
[12]
W. Yeo, T. C. Chan, N. W. Y. Leung et al., “Hepatitis B virus reactivation in lymphoma patients with prior resolved hepatitis B undergoing anticancer therapy with or without rituximab,” Journal of Clinical Oncology, vol. 27, no. 4, pp. 605–611, 2009.
[13]
M. J. Arin, A. Engert, T. Krieg, and N. Hunzelmann, “Anti-CD20 monoclonal antibody (rituximab) in the treatment of pemphigus,” British Journal of Dermatology, vol. 153, no. 3, pp. 620–625, 2005.
[14]
H.-R. Li, J.-J. Huang, H.-Q. Guo et al., “Comparison of entecavir and lamivudine in preventing hepatitis B reactivation in lymphoma patients during chemotherapy,” Journal of Viral Hepatitis, vol. 18, no. 12, pp. 877–883, 2011.
