Lymphomas are malignant neoplasms of lymphocyte lineage that present as tumor masses primarily involving the lymphoid organs. According to the WHO classification, they are divided into two main groups, with each group containing a range of families, entities/types and subtypes with heterogeneous clinical outcomes and complex molecular characteristics that change over time. Conventional methods for diagnosing and monitoring lymphomas are invasive and technically demanding, and the heterogeneity of lymphomas further complicates diagnosis and selection of appropriate therapy. The development of liquid biopsy has opened up new possibilities for non-invasive diagnosis, prognosis and monitoring of these complex hematological malignancies. It is a non-invasive method that isolates circulating tumor cells (CTCs), cell-free DNA (cfDNA), exosomes and circulating RNAs (miRNA, lncRNA) from a blood sample or other body fluid. Liquid biopsy provides a comprehensive picture of lymphoma heterogeneity and allows real-time monitoring of tumor dynamics. This review paper explores the current state and future potential of liquid biopsy in lymphomas and highlights its benefits in lymphoma genotyping, early detection of relapse, assessment of treatment response, and monitoring of minimal residual disease and clonal evolution. Advanced PCR-based and NGS-based methods have significantly improved the sensitivity and specificity of liquid biopsy tests. Circulating tumour DNA (ctDNA) has emerged as the most promising and widely applicable liquid biopsy marker in various lymphoma subtypes. MiRNA, exosomes, and lncRNA have the ability to provide additional information about lymphoma biology and disease progression. CTCs have limited utility in most lymphomas due to their small numbers, but can potentially provide information in leukemic phases of the disease. Despite promising results, challenges remain in standardization, clinical validation, and integration with existing diagnostic and prognostic tools. Therefore, these challenges need to be addressed before integrating liquid biopsy into routine clinical practice.