The haemato-oncologist from HCG Cancer Centre, Nashik, discusses how newer therapies are reshaping treatment decisions in aggressive lymphomas.
When Standard Chemotherapy Is No Longer Enough in B-Cell Lymphoma, Says Dr. Priyatesh Dwivedi
The management of B-cell lymphoma has entered a phase where standard chemotherapy alone is no longer sufficient for a growing subset of patients. In routine oncology practice, clinicians are increasingly confronted with cases that either fail to respond adequately to first-line regimens or relapse after an initial response, prompting a reassessment of long-established treatment pathways.
B-cell lymphoma originates from abnormal proliferation of B lymphocytes, a critical component of the immune system. In India, Diffuse Large B-Cell Lymphoma represents the most frequently diagnosed subtype among non-Hodgkin lymphomas. Data from Indian tertiary care centres and academic institutions consistently show that B-cell lymphomas account for the majority of lymphoma diagnoses, with DLBCL forming the largest share. These cases are characterised by rapid progression and require timely intervention, yet their clinical behaviour can vary significantly between patients.
One of the most significant developments in this context has been the clinical introduction of CAR-T cell therapy in India. This form of treatment involves modifying a patient’s own immune cells to recognise and attack malignant B cells. Indigenous CAR-T therapies, including options developed within the country, have made this modality accessible to a broader segment of eligible patients who previously had limited options after chemotherapy failure. In clinical practice, CAR-T therapy is now considered for relapsed or refractory B-cell lymphomas under carefully selected conditions.
Dr. Dwivedi notes that the role of bone marrow transplantation also continues to evolve alongside these therapies. While autologous transplant remains an important option for eligible patients, the availability of advanced immunotherapies has refined patient selection and timing. Decisions are now guided by disease response patterns, molecular risk factors, and overall treatment tolerance rather than by rigid algorithms.
Dr. Dwivedi emphasises that while these therapies represent meaningful progress, they are not universal solutions. Access, eligibility criteria, and long-term outcomes continue to be areas of active evaluation. However, the presence of multiple therapeutic pathways has fundamentally changed how clinicians approach cases where chemotherapy alone is insufficient.
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