Background Studies have shown a positive association between hepatitis B surface antigen (HBsAg)-positive hepatitis B virus (HBV) infection and B-cell non-Hodgkin lymphomas (NHLs), especially for diffuse large B-cell lymphoma (DLBCL) and follicular lymphoma (FL). Nevertheless, the clinical implications of HBV infection in patients with DLBCL and FL are unclear. Moreover, factors that contribute to lymphomagenesis of HBV-associated B-cell NHL remain to be explored. Aims We aimed to examine the prognostic value of HBsAg in DLBCL and in FL. We further explored the factor that might lead to the development of HBV-associated lymphoma, the integration of HBV DNA into the genome of lymphoma cells. Methods We investigated the clinical relevance of HBsAg in immunocompetent patients with DLBCL and in those with FL, respectively. For the DLBCL cohort, patients who had received homogeneous rituximab plus cyclophosphamide, doxorubicin, vincristine, and prednisone as the frontline therapy at National Taiwan University Hospital (NTUH) between 2002 and 2016 were selected. For the FL cohort, patients treated with frontline rituximab-containing chemoimmunotherapy at NTUH between 2006 and 2016 were recruited. Additionally, we selected 45 B-cell NHL cases and used the Hybridization capture-based next generation sequencing (NGS) to characterize the pattern of HBV DNA integration into the genome of lymphoma cells in their tumor samples. Results Among 416 analyzed patients in the DLBCL cohort, 98 (23.6%) were HBsAg-positive. HBsAg positivity was associated with a younger age and more advanced stage at diagnosis, more frequent hepatic impairment during perichemotherapy, and a trend of higher National Comprehensive Cancer Network-International Prognostic Index score. Compared with the HBsAg-negative patients, the HBsAg-positive patients had a poorer 5-year overall survival (OS) rate and shorter 5-year progression-free survival (PFS) rate. Multivariate analyses showed HBsAg was an independent unfavorable prognostic indicator. Regarding the FL cohort including 149 patients, 32 (21.5%) were HBsAg-positive. HBsAg positivity was positively associated with symptomatic splenomegaly, significant serous effusions, and peritreatment hepatic dysfunction. HBsAg-positive patients had significantly poorer OS and shorter PFS than had HBsAg-negative patients. Multivariate analysis still revealed that HBsAg is an independent adverse prognostic factor for OS. Intriguingly, HBsAg-positive patients had a higher incidence of progression of disease within 24 months than had HBsAg-negative patients (cumulative incidence rate, 25.8% vs. 12.4%, P = 0.045). Finally, by conducting high-throughput viral integration detection, a total of 354 HBV integrations were identified from 28.9% (13/45) of HBV-associated NHLs. Nevertheless, there was no clustered genomic hotspot of viral integration. Additionally, only few HBV integrations had clonality in the genome of B-cell NHL. Moreover, the HBV integration did not show persistence and stability by analyzing the paired diagnosis-relapse samples. Furthermore, the presence of HBV integration was not associated with the survival of patients with DLBCL. Conclusions We demonstrated that HBV infection is uniquely relevant to DLBCL and FL. Our research also provides evidences that HBsAg was an independent unfavorable factor significantly associated with survival, highlighting its potential as a novel prognostic predictor of the survival of patients with DLBCL or with FL. Although HBV DNA could indeed integrate into the genome of B-cell NHL, the sample frequency of integration events was far less than that in hepatocellular carcinoma. No significantly enriched viral integration hotspot was discovered. Additionally, only few cases were identified to have clonally expanded lymphoma cells carrying the same integrated viral DNA. Moreover, HBV integration was unstable during disease evolution and not associated with prognosis. Hence, the mechanism of insertional mutagenesis to drive lymphomagenesis might not be applicable to HBV-associated lymphoma. The other factor such as the influence of chronic HBV infection on the tumor immune microenvironment merits further investigation. We look forward to exploring the biological role of HBV infection in B-cell NHL and developing novel therapeutic strategies for this group of patients.