Your search keyword '"Fenn, Sebastian"' showing total 3 results

1. Crystal Structure of an Anti-Ang2 CrossFab Demonstrates Complete Structural and Functional Integrity of the Variable Domain.

Author

Fenn, Sebastian, Schiller, Christian B., Griese, Julia J., Duerr, Harald, Imhof-Jung, Sabine, Gassner, Christian, Moelleken, Joerg, Regula, Joerg Thomas, Schaefer, Wolfgang, Thomas, Markus, Klein, Christian, Hopfner, Karl-Peter, and Kettenberger, Hubert

Subjects

*CRYSTAL structure, *ANTIGENS, *BIOCHEMISTRY, *PROTEIN structure, *DRUG development, *IMMUNOCHEMISTRY, *COMPUTATIONAL biology, *BIOMEDICAL engineering

Abstract

Bispecific antibodies are considered as a promising class of future biotherapeutic molecules. They comprise binding specificities for two different antigens, which may provide additive or synergistic modes of action. There is a wide variety of design alternatives for such bispecific antibodies, including the “CrossMab” format. CrossMabs contain a domain crossover in one of the antigen-binding (Fab) parts, together with the “knobs-and-holes” approach, to enforce the correct assembly of four different polypeptide chains into an IgG-like bispecific antibody. We determined the crystal structure of a hAng-2-binding Fab in its crossed and uncrossed form and show that CH1-CL-domain crossover does not induce significant perturbations of the structure and has no detectable influence on target binding. [ABSTRACT FROM AUTHOR]

Published

2013

2. Structural biochemistry of nuclear actin-related proteins 4 and 8 reveals their interaction with actin.

Author

Fenn, Sebastian, Breitsprecher, Dennis, Gerhold, Christian B, Witte, Gregor, Faix, Jan, and Hopfner, Karl-Peter

Subjects

*BIOCHEMISTRY, *ACTIN, *CHROMATIN, *SACCHAROMYCES cerevisiae, *POLYMERIZATION, *CRYSTALS, *MONOMERS

Abstract

Nuclear actin and actin-related proteins (Arps) are integral components of various chromatin-remodelling complexes. Actin in such nuclear assemblies does not form filaments but associates in defined complexes, for instance with Arp4 and Arp8 in the INO80 remodeller. To understand the relationship between nuclear actin and its associated Arps and to test the possibility that Arp4 and Arp8 help maintain actin in defined states, we structurally analysed Arp4 and Arp8 from Saccharomyces cerevisiae and tested their biochemical effects on actin assembly and disassembly. The solution structures of isolated Arp4 and Arp8 indicate them to be monomeric and the crystal structure of ATP-Arp4 reveals several differences to actin that explain why Arp4 does not form filaments itself. Remarkably, Arp4, assisted by Arp8, influences actin polymerization in vitro and is able to depolymerize actin filaments. Arp4 likely forms a complex with monomeric actin via the barbed end. Our data thus help explaining how nuclear actin is held in a discrete complex within the INO80 chromatin remodeller. [ABSTRACT FROM AUTHOR]

Published

2011

3. Structure of a Construct of a Human Poly(C)-binding Protein Containing the First and Second KH Domains Reveals Insights into Its Regulatory Mechanisms.

Author

Zhihua Du, Fenn, Sebastian, Tjhen, Richard, and James, Thomas L.

Subjects

*CARRIER proteins, *PROTEINS, *PROTEIN binding, *NUCLEOTIDE sequence, *RNA-protein interactions, *NUCLEAR magnetic resonance, *BIOCHEMISTRY

Abstract

Poly(C)-binding proteins (PCBPs) are important regulatory proteins that contain three KH (hnRNP K homology) domains. Binding poly(C) D/RNA sequences via KH domains is essential for multiple PCBP functions. To reveal the basis for PCBP-D/RNA interactions and function, we determined the structure of a construct containing the first two domains (KH1-KH2) of human PCBP2 by NMR. KH1 and KH2 form an intramolecular pseudodimer. The large hydrophobic dimerization surface of each KH domain is on the side opposite the D/RNA binding interface. Chemical shift mapping indicates both domains bind poly(C) DNA motifs without disrupting the KH1-KH2 interaction. Spectral comparison of KH1-KH2, KH3, and full-length PCBP2 constructs suggests that the KH1-KH2 pseudodimer forms, but KH3 does not interact with other parts of the protein. From NMR studies and modeling, we propose possible modes of cooperative binding tandem poly(C) motifs by the KH domains. D/RNA binding may induce pseudodimer dissociation or stabilize dissociated KH1 and KH2, making protein interaction surfaces available to PCBP-binding partners. This conformational change may represent a regulatory mechanism linking D/RNA binding to PCBP functions. [ABSTRACT FROM AUTHOR]

Published

2008