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Infectious diseases and immunological markers associated with patients with non-Hodgkin lymphoma treated with rituximab
Authors:Kleber Jordão de Souza  Rodrigo Sala Ferro  Paula Andreia Martins Carrilho  Dewton de Moraes Vasconcelos
Institution:1. Internal Medicine Department, Regional Hospital of Presidente Prudente, Presidente Prudente, S?o Paulo, Brazil;2. Infectious Diseases and Immunology Department, Oeste Paulista University, Presidente Prudente, S?o Paulo, Brazil;3. Haematology Service, Santa Casa de Misericórdia of Presidente Prudente, Presidente Prudente, S?o Paulo, Brazil;4. Laboratory of Medical Investigation Unit 56, Hospital das Clínicas da Faculdade de Medicina da Universidade de S?o Paulo, S?o Paulo, Brazil
Abstract:Background: The use of rituximab (RTX) is increasing, even in developing countries. It has become the first-line therapy or adjuvant to chemotherapy (CHOP; cyclophosphamide, hydroxydaunorubicin, oncovin and prednisone) for various diseases, including B cell lymphoma and autoimmune diseases.

Aim: We describe the infectious diseases and immunological markers associated with RTX treatment of patients with non-Hodgkin lymphoma (NHL).

Methods: Serum immunoglobulins were determined before and after intravenous immunoglobulin (IVIg) administration. Pneumo-23IgG-specific anti-pneumococcal antibodies were evaluated before and after vaccination. Immunophenotyping and lymphocyte proliferation were determined in the course of the treatment.

Results: Seven patients were followed and median age was 56.0?±?5.0?years (range, 41.9–71.6?years). At baseline, the mean level of IgG was 333.7?±?40.8?and IgM 40.9?±?11.3?mg/dL, respectively; immunoglobulin A and E (IgA and IgE) were under the limit of detection. Two patients had reduced or absent B cells and T cell subsets were at normal levels in five patients. All patients failed to mount an efficient post-vaccination immune response against hepatitis B virus, tetanus, diphtheria and against the 23-valent pneumococcal polysaccharide vaccine. During RTX/CHOP treatment, human-IgG-immunoglobulin (IVIg) therapy was introduced in six patients after recurrent infections, including community-acquired pneumonia (85.7%), chronic sinusitis (85.7%) and gastroenteritis (42.9%).

Conclusion: Poor response against pneumococcal vaccines increases the susceptibility of respiratory diseases in these patients. In patients with NHL treated with RTX, the benefits achieved with IVIg replacement for the control of recurrent infectious diseases is of paramount importance. Clinicians dealing with monoclonal antibodies against cancer therapy, especially RTX, should be aware of the increasing risks for symptomatic induced hypogammaglobulinemia and respiratory infections.
Keywords:Rituximab  non-Hodgkin lymphoma  infectious diseases  hypogammaglobulinemia  23-valent pneumococcal vaccine
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