Literature DB >> 24190981

Complement activation and intraventricular rituximab distribution in recurrent central nervous system lymphoma.

Cigall Kadoch1, Jing Li, Valerie S Wong, Lingjing Chen, Soonmee Cha, Pamela Munster, Clifford A Lowell, Marc A Shuman, James L Rubenstein.   

Abstract

PURPOSE: To elucidate the mechanistic basis for efficacy of intrathecal rituximab. We evaluated complement activation as well as the pharmacokinetics of intraventricular rituximab in patients who participated in two phase 1 multicenter studies. EXPERIMENTAL
DESIGN: We evaluated complement activation as a candidate mediator of rituximab within the central nervous system (CNS). Complement C3 and C5b-9 were quantified by ELISA in serial cerebrospinal fluid (CSF) specimens after intraventricular rituximab administration. We determined rituximab concentration profiles in CSF and serum. A population three- compartment pharmacokinetic model was built to describe the disposition of rituximab following intraventricular administration. The model was derived from results of the first trial and validated with results of the second trial.
RESULTS: Complement C3 and C5b-9 were reproducibly activated in CSF after intraventricular rituximab. Ectopic expression of C3 mRNA and protein within CNS lymphoma lesions was localized to myeloid cells. Constitutive high C3 activation at baseline was associated with adverse prognosis. A pharmacokinetic model was built, which contains three distinct compartments, to describe the distribution of rituximab within the neuroaxis after intraventricular administration.
CONCLUSIONS: We provide the first evidence of C3 activation within the neuroaxis with intraventricular immunotherapy and suggest that complement may contribute to immunotherapeutic responses of rituximab in CNS lymphoma. Penetration of rituximab into neural tissue is supported by this pharmacokinetic model and may contribute to efficacy. These findings have general implications for intraventricular immunotherapy. Our data highlight potential innovations to improve efficacy of intraventricular immunotherapy both via modulation of the innate immune response as well as innovations in drug delivery. ©2013 AACR

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Year:  2013        PMID: 24190981      PMCID: PMC3944388          DOI: 10.1158/1078-0432.CCR-13-0474

Source DB:  PubMed          Journal:  Clin Cancer Res        ISSN: 1078-0432            Impact factor:   12.531


  53 in total

1.  Intraventricular treatment of relapsed central nervous system lymphoma with the anti-CD20 antibody rituximab.

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Authors:  Marek Honczarenko; Mariusz Z Ratajczak; Anne Nicholson-Weller; Leslie E Silberstein
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Review 4.  Neuroprotection from complement-mediated inflammatory damage.

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Review 5.  Role of intrathecal rituximab and trastuzumab in the management of leptomeningeal carcinomatosis.

Authors:  Anthony J Perissinotti; David J Reeves
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Authors:  P Feugier; J M Virion; H Tilly; C Haioun; G Marit; M Macro; D Bordessoule; C Recher; M Blanc; T Molina; P Lederlin; B Coiffier
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10.  Intraventricular administration of BDNF increases the number of newly generated neurons in the adult olfactory bulb.

Authors:  T Zigova; V Pencea; S J Wiegand; M B Luskin
Journal:  Mol Cell Neurosci       Date:  1998-07       Impact factor: 4.314

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6.  Phase 1 investigation of lenalidomide/rituximab plus outcomes of lenalidomide maintenance in relapsed CNS lymphoma.

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7.  Phosphodiesterase type 5 inhibitor Tadalafil increases Rituximab treatment efficacy in a mouse brain lymphoma model.

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Review 8.  Molecular profiling of primary central nervous system lymphomas - predictive and prognostic value?

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Review 10.  On point in primary CNS lymphoma.

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