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Dive into the research topics where Peter Robert Baum is active.

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Featured researches published by Peter Robert Baum.


Rheumatology | 2011

Distinct in vitro binding properties of the anti-CD20 small modular immunopharmaceutical 2LM20-4 result in profound and sustained in vivo potency in cynomolgus monkeys

Cheryl Nickerson-Nutter; Lioudmila Tchistiakova; Nilufer Seth; Marion Kasaian; Barbara Sibley; Stephane Olland; Richard Zollner; William A. Brady; Kendall M. Mohler; Peter Robert Baum; Alan Wahl; Deborah Herber; Yulia Vugmeyster; David Wensel; Neil M. Wolfman; Davinder Gill; Mary Collins; Kyri Dunussi-Joannopoulos

Objectives. To characterize the in vitro binding and effector function properties of CD20-directed small modular immunopharmaceutical (SMIP) 2LM20-4, and to compare its in vivo B-cell depletion activity with the mutated 2LM20-4 P331S [no in vitro complement-dependent cytotoxicity (CDC)] and rituximab in cynomolgus monkeys. Methods. Direct binding is examined in flow cytometry, confocal microscopy, scatchard and lipid raft assays. Effector function assays include CDC and Fc-mediated cellular toxicity. In the 6-month-long in vivo B-cell depletion study, single i.v. dosages of 1 or 10 mg/kg of anti-CD20 proteins were administered to monkeys and B-cell counts were monitored in peripheral blood, bone marrow and lymph nodes. Results. 2LM20-4 has lower saturation binding to human primary B cells and recruits fewer CD20 molecules into lipid rafts compared with rituximab; however, it induces higher in vitro CDC. In competitive binding, 2LM20-4 only partially displaces rituximab, suggesting that it binds to a fraction of CD20 molecules within certain locations of the plasma membrane as compared with rituximab. In monkeys, 2LM20-4 had more sustained B-cell depletion activity than rituximab in peripheral blood and had significantly more profound and sustained activity than 2LM20-4 P331S and rituximab in the lymph nodes. Conclusions. SMIP 2LM20-4, which binds to a fraction of CD20 molecules as compared with rituximab, has more potent in vitro CDC, and more potent and sustained B-cell depletion activity in cynomolgus monkeys. Our work has considerable clinical relevance since it provides novel insights related to the emerging B-cell depletion therapies in autoimmune diseases.


European Journal of Immunology | 1994

Induction of B cell costimulatory function by recombinant murine CD40 ligand.

Mary K. Kennedy; Kendall M. Mohler; Kurt Shanebeck; Peter Robert Baum; Kathleen S. Picha; Carol Otten-Evans; Charles A. Janeway; Kenneth H. Grabstein


Archive | 2009

Cd86 antagonist multi-target binding proteins

Peter Armstrong Thompson; Peter Robert Baum; Philip Tan; John W. Blankenship; Sateesh Kumar Natarajan


Archive | 2009

TCR Complex Immunotherapeutics

Valerie Odegard; Catherine J. McMahan; Peter Robert Baum; Peter Armstrong Thompson; Philip Tan; John W. Blankenship; Sateesh Kumar Natarajan


Archive | 2009

Multi-Specific Binding Proteins Targeting B Cell Disorders

Philip Tan; Laura S. Grosmaire; Peter Robert Baum; Peter Armstrong Thompson


Archive | 2008

Erbb2 binding proteins and use thereof

Davinder Gill; Fionnuala Mcaleese; Laird Bloom; Peter Armstrong Thompson; Peter Robert Baum; Paul A. Algate


Archive | 2009

Antagonists of IL-6

Lynda Misher; Alan Keith Lofquist; Peter Robert Baum; Peter Armstrong Thompson


Archive | 2009

Agents immunothérapeutiques il6

Lynda Misher; Alan Keith Lofquist; Peter Robert Baum; Peter Armstrong Thompson


Archive | 2009

Protéines de liaison multicibles antagonistes de cd86

Peter Armstrong Thompson; Peter Robert Baum; Philip Tan; John W. Blankenship; Sateesh Kumar Natarajan


Archive | 2009

Immunothérapie impliquant le complexe tcr

Valerie Odegard; Catherine J. McMahan; Peter Robert Baum; Peter Armstrong Thompson; Philip Tan; John W. Blankenship; Sateesh Kumar Natarajan

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Paul A. Algate

Fred Hutchinson Cancer Research Center

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