The role of sex and weight on rituximab clearance and serum elimination half-life in elderly patients with DLBCL

Müller, Carsten; Murawski, Niels; Wiesen, Martin H. J.; Held, Gerhard; Poeschel, Viola; Zeynalova, Samira; Wenger, Michael; Nickenig, Christina; Peter, Norma; Lengfelder, Eva; Metzner, Bernd; Rixecker, Torben; Zwick, Carsten; Pfreundschuh, Michael; Reiser, Marcel

doi:10.1182/blood-2011-09-380949

Cited by 212 publications

(209 citation statements)

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“…[54][55][56] The nonlinear PK of these types of antibodies may in part be explained by binding of the antibodies to their respective targets, with a large component of target-mediated elimination after the first dose that is chemotherapy) have an elimination half-life in the magnitude of hours and rapidly achieve steady-state following administration (hours-days), while large molecules (e.g., mAbs) have a very long elimination half-life (in the magnitude of weeks) and may take up to 12 weeks to achieve steady-state. 65,66,69,70 …”

Section: -34mentioning

confidence: 99%

“…30,59 The volume of distribution of RTX at steady-state is approximately 9.6 L. Since the plasma volume is only 3-3.5 L, this suggests that the mAb distributes into the extracellular spaces of tissues, except the CNS. 65,66 Indeed, the blood-brain barrier physically impedes entry of macromolecules into the CNS, severely limiting distribution of RTX after i.v. administration.…”

Section: -34mentioning

confidence: 99%

“…This gender difference correlated with a better PFS observed in the total female population (n = 287) of the RICOVER-60 trial compared with males (n = 325). 66 It was suggested that the higher weight of males contributed to their faster RTX clearance, but sex and weight independently affected RTX clearance and elimination half-life.…”

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confidence: 99%

“…66 In the latter study, RTX concentrations were measured 10 min before each infusion, 1 week and 1, 2, 3, 6 and 9 mo after the last infusion. Females were shown to have a longer elimination half-life than males (30.7 vs. 24.7 d, p = 0.003), which resulted in a higher overall exposure to the drug.…”

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confidence: 99%

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Lessons for the clinic from rituximab pharmacokinetics and pharmacodynamics

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Rambaldi

et al. 2013

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Lessons for the clinic from rituximab pharmacokinetics and pharmacodynamics

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Rambaldi

et al. 2013

mAbs

111

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“…This finding strengthens an interpretation that R-CHOEP and R-very intensive chemotherapy are preferable to R-CHOP in aaIPI ≥ 2, but it also suggests that some of the Regional survival differences are due to other factors than first-line chemotherapy regimens. previously been more apparent in older patients (Muller et al, 2012;Pfreundschuh et al, 2014). We emphasize that our findings were independent in multivariate analysis adjusted for all prognostic clinical factors (gender, age, aaIPI and bulky disease).…”

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confidence: 49%

Chemotherapeutic intensity and survival differences in young patients with diffuse large B‐cell lymphoma: a Swedish Lymphoma Registry study

et al. 2016

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Summary Young patients with diffuse large B‐cell lymphoma (DLBCL) are variably treated with rituximab combined with cyclophosphamide‐doxorubicin‐vincristine‐prednisone (R‐CHOP), CHOP‐etoposide (R‐CHOEP), and anthracycline‐based regimens with the addition of high‐dose cytarabine/methotrexate (R‐HDA/M). Using the nationwide, population‐based Swedish Lymphoma Registry, we evaluated outcome, by treatment and Healthcare Region, in all 751 DLBCL patients aged ≤60 years without central nervous involvement, diagnosed in Sweden between 2007 and 2012. Overall survival was estimated using multivariate Cox analysis. In patients with age‐adjusted international prognostic index (aaIPI) ≥ 2, the 5‐year overall survival (OS) was 70%, 76% and 85% after R‐CHOP, R‐CHOEP and R‐HDA/M, respectively (P = 0·002); the corresponding estimates were 40%, 55%, and 92% in aaIPI = 3 (P = 0·014). There were large therapeutic differences between Sweden's six Healthcare Regions for aaIPI ≥ 2: three were “Moderate” (more R‐CHOP) and three “Intensive” (more R‐CHOEP and R‐HDA/M). Patients with aaIPI ≥ 2 who were treated in the Intensive Regions, showed better OS (P < 0·00005), particularly those with aaIPI = 3 (5‐year OS, 62% vs. 30%; P < 0·00005). There were no regional differences in therapy or survival in patients with aaIPI < 2. We conclude that in younger high‐risk patients, survival appears superior after more intensive therapy than R‐CHOP.

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