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Dive into the research topics where Jan Terje Andersen is active.

Publication


Featured researches published by Jan Terje Andersen.


FEBS Journal | 2008

Ligand binding and antigenic properties of a human neonatal Fc receptor with mutation of two unpaired cysteine residues

Jan Terje Andersen; Sune Justesen; Burkhard Fleckenstein; Terje E. Michaelsen; Gøril Berntzen; Muluneh Bekele Daba; Vigdis Lauvrak; Søren Buus; Inger Sandlie

The neonatal Fc receptor (FcRn) is a major histocompatibility complex class I‐related molecule that regulates the half‐life of IgG and albumin. In addition, FcRn directs the transport of IgG across both mucosal epithelium and placenta and also enhances phagocytosis in neutrophils. This new knowledge gives incentives for the design of IgG and albumin‐based diagnostics and therapeutics. To study FcRn in vitro and to select and characterize FcRn binders, large quantities of soluble human FcRn are needed. In this report, we explored the impact of two free cysteine residues (C48 and C251) of the FcRn heavy chain on the overall structure and function of soluble human FcRn and described an improved bacterial production strategy based on removal of these residues, yielding ∼ 70 mg·L−1 of fermentation of refolded soluble human FcRn. The structural and functional integrity was proved by CD, surface plasmon resonance and MALDI‐TOF peptide mapping analyses. The strategy may generally be translated to the large‐scale production of other major histocompatibility complex class I‐related molecules with nonfunctional unpaired cysteine residues. Furthermore, the anti‐FcRn response in goats immunized with the FcRn heavy chain alone was analyzed following affinity purification on heavy chain‐coupled Sepharose. Importantly, purified antibodies blocked the binding of both ligands to soluble human FcRn and were thus directed to both binding sites. This implies that the FcRn heavy chain, without prior assembly with human β2‐microglobulin, contains the relevant epitopes found in soluble human FcRn, and is therefore sufficient to obtain binders to either ligand‐binding site. This finding will greatly facilitate the selection and characterization of such binders.


Archive | 2010

Engineering of the Fc Region for Improved PK (FcRn Interaction)

Tove Olafsen; Jan Terje Andersen; Inger Sandlie; Anna M. Wu


Archive | 2012

Enhanced albumins and albumin fusion technology: tuning circulatory half-life with Novozymes Albufuse ® Flex to meet medical needs

Karen A. Bunting; Filipa Antunes; Jason Cameron; Lizzie Allan; Jens Erik Nielsen; Anne Cox; Les Evans; Darrell Sleep; Dorthe Viuff; Jan Terje Andersen; Inger Sandlie


Archive | 2017

variantes de albumina

Andrew Plumridge; Darrell Sleep; Esben Peter Friis; Inger Sandlie; Jan Terje Andersen; Jason Cameron


Archive | 2017

Anti-viral engineered immunoglobulins

Maria Bottermann; Inger Sandlie; Leo C. James; Stian Foss; Jan Terje Andersen


Gastroenterology | 2017

Neonatal FC Receptor Cooperates with Classical FC Gamma Receptors to Control Inflammatory Bowel Disease through Regulating Immune Complex Processing

Jonathan J Hubbard; Timo Rath; Michal Pyzik; Jan Terje Andersen; Walter Kim; Niklas Krupka; Edda Fiebiger; Jerrold R. Turner; Jonathan N. Glickman; Wayne I. Lencer; Inger Sandlie; Derry C. Roopenian; Kristi Baker; Richard S. Blumberg


Archive | 2014

Modelo animal farmacocinético

Jason Cameron; Darrell Sleep; Inger Sandlie; Jan Terje Andersen


Archive | 2014

Pharmacokinetic animal model

Jason Cameron; Darrell Sleep; Inger Sandlie; Jan Terje Andersen


Archive | 2011

Dérivés et variants d'albumine

Andrew Plumridge; Darrell Sleep; Inger Sandlie; Jan Terje Andersen; Jason Cameron; Leslie Evans; Steven Athwal; Elizabeth Allan; Esben Peter Friis


Archive | 2010

Variants d'albumine

Andrew Plumridge; Darrell Sleep; Jason Cameron; Inger Sandlie; Jan Terje Andersen; Esben Peter Friis

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Darrell Sleep

University of Nottingham

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Jason Cameron

University of Nottingham

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Dorthe Viuff

University of Nottingham

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Filipa Antunes

University of Nottingham

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