Abstract
BackgroundRituximab is a novel chimeric monoclonal antibody that has established itself as a potent therapeutic option for autoimmune medical conditions, including systemic lupus erythematosus, owing to its mechanism of action targeting CD20 cells. Rituximab is also known to cause a spectrum of side effects including hematological abnormalities. Acute isolated thrombocytopenia following rituximab is an uncommon occurrence and, when seen, occurs in the presence of underlying hematological malignancies. Its occurrence in autoimmune diseases is rare. Despite this, acute isolated thrombocytopenia in the backdrop of systemic lupus erythematosus is undocumented.Case presentationA young 36-year-old South Asian female with systemic lupus erythematosus with class IV lupus nephritis poorly responding to standard therapy was initiated on rituximab. Ten days later, she presented with mucocutaneous bleeding and ecchymotic skin lesions. Isolated severe thrombocytopenia was noted with a platelet count of 5 × 109/L (150–450). Anticipating life-threatening bleeding, she was given intravenous immunoglobulin, methyl prednisolone, and platelet transfusion considering a spectrum of initial differential diagnosis. Rituximab was also withheld. Though extensively investigated, most investigations were negative. A platelet destructive process was suspected as bone marrow biopsy showed adequate megakaryocytes. Weighing the risk versus benefit, following recovery, she was reinitiated on rituximab. Within 4 days, she presented again with similar symptoms and severe isolated thrombocytopenia was noted. Rituximab-induced acute thrombocytopenia was considered the working clinical diagnosis.Case discussion and conclusionRituximab can cause a spectrum of hematological abnormalities, including isolated acute thrombocytopenia. Its occurrence in autoimmune conditions is rare, and its manifestation in systemic lupus erythematosus is undocumented. Its exact etiology is still disputed. Usually considered benign, the platelet numbers tend to show improvement with cessation of therapy. However, in the presence of mucocutaneous bleeding in our patient, we took an aggressive approach to management. Though evidence for corrective therapy is anecdotal, it could be justified on the basis of averting potential catastrophic hemorrhagic manifestations. The spectrum of autoimmune disease that potentially predisposes rituximab to cause thrombocytopenia should be extended to include systemic lupus erythematosus.
Highlights
Rituximab is an intravenous chimeric monoclonal antibody [1] developed from deoxyribonucleic acid technology using human and mice genes that act via CD 20 receptors
Case discussion and conclusion: Rituximab can cause a spectrum of hematological abnormalities, including isolated acute thrombocytopenia
In the presence of mucocutaneous bleeding in our patient, we took an aggressive approach to management
Summary
Rituximab is an intravenous chimeric monoclonal antibody [1] developed from deoxyribonucleic acid technology using human and mice genes that act via CD 20 receptors. Her whole blood analysis demonstrated a white cell count of 6.9 × 109/L (4–11 × 109/L), hemoglobin of 11.3 g/dL (11–15 g/dL), and platelet count of 222 × 109/L (150–450 × 109/L) Her remaining blood tests including renal function and inflammatory markers, as well as urinalysis, were normal (Table 1). Rituximab-induced thrombocytopenia was entertained as a differential, the platelet destructive process, lack of previous reported similar cases in SLE patients, and the necessity of treating the class IV nephritis was weighed and a clinical decision was taken to resume rituximab treatment considering it was a less likely etiology Her bloods done before infusion showed a platelet count of 283 × 109/L (150–450 × 109/L). The final working diagnosis was rituximabinduced isolated thrombocytopenia with mucocutaneous hemorrhagic manifestations
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