Association of serum Rituximab (IDEC–C2B8) concentration and anti-tumor response in the treatment of recurrent low-grade or follicular non-Hodgkin’s lymphoma

Abstract: SummaryBackground; Monoclonal antibodies are being utilized for treatment of patients with low-grade non-Hodgkin's lymphoma as well as other cancers. Results from phase I and II clinical studies has shown that the chimeric monoclonal antibody Rituximab has minimal toxicity and significant therapeutic activity in low grade non-Hodgkin's lymphoma.Patients and methods; We have recently reported on a multicentre pivotal phase III clinical trial involving 166 patients with recurrent low-grade lymphoma who were trea… Show more

“…7 Very few reports exist concerning its administration during pregnancy in humans. 8,9 Given rituximab's pharmacokinetic properties, 3,4,13 and as IgG is known to pass the placental barrier, its administration during pregnancy should consider the potential risk of B-cell depletion in the fetus and newborn. 2 In the two previous reports, both were in the setting of pregnant women with non-Hodgkin's lymphoma.…”

Administration of rituximab during the first trimester of pregnancy without consequences for the newborn

“…7 Very few reports exist concerning its administration during pregnancy in humans. 8,9 Given rituximab's pharmacokinetic properties, 3,4,13 and as IgG is known to pass the placental barrier, its administration during pregnancy should consider the potential risk of B-cell depletion in the fetus and newborn. 2 In the two previous reports, both were in the setting of pregnant women with non-Hodgkin's lymphoma.…”

Administration of rituximab during the first trimester of pregnancy without consequences for the newborn

“…Elevated b2-microglobulin, elevated LDH, bulky disease and age >60 years did not appear to impact response, implying that patients regarded as having a poor prognosis may respond to rituximab. Median rituximab serum levels were significantly higher in responders, compared with the non-responders (Berinstein et al, 1998). Mean serum antibody concentration was inversely correlated with the bulk of the disease and the number of circulating B cells, suggesting that patients with a higher tumor load might need higher doses or prolonged treatment, to achieve the necessary serum levels (Gordan et al, 2005).…”

“…Several arguments are in favor of this approach: the success of re-treatment or the strong correlation between rituximab plasma levels and RR (Berinstein et al, 1998). A recent randomized trial showed that adding maintenance doses of rituximab prolonged response duration (Ghielmini et al, 2004): 202 patients with newly diagnosed or refractory/relapsed FL were treated with standard rituximab (375 mg/m 2 weekly  4).…”

Rituximab therapy in malignant lymphoma

“…M ost of them stopped after only six treatments (6 weeks). This may be too short a treatment period for relevant therapy evaluation, especially when compared with rituximab therapy for malignant lymphomas (29,30). R esponse to rituximab therapy improved from 40% to 60% when the patients were treated during eight compared with four consecutive weeks.…”

“…R esponse to rituximab therapy improved from 40% to 60% when the patients were treated during eight compared with four consecutive weeks. It is possible that a prolonged course is needed, especially for patients with a large tumour bulk (29,30). R esponse evaluation for chemotherapy is normally scheduled after two or three courses given at threeweek intervals.…”

A Population-based Study on the First Forty-Eight Breast Cancer Patients Receiving Trastuzumab (Herceptin®) on a Named Patient Basis in Sweden