Flores-Flores_2002_J.Neural.Transm.Suppl_62_165

Reference

Title : Development of human antibody fragments directed towards synaptic acetylcholinesterase using a semi-synthetic phage display library - Flores-Flores_2002_J.Neural.Transm.Suppl_62_165
Author(s) : Flores-Flores C , Nissim A , Shochat S , Soreq H
Ref : J Neural Transm Suppl , 62 :165 , 2002
Abstract :

Current Alzheimer's disease therapies suppress acetylcholine hydrolysis by inhibiting acetylcholinesterase (AChE) at cholinergic synapses. However, anticholinesterases promote alternative splicing changing the composition of brain AChE variants. To study this phenomenon we developed monoclonal antibodies to acetylcholinesterase synaptic peptide (ASP), a synthetic peptide with the C-terminal sequence unique to the human synaptic variant AChE-S. Screening of a phage display human antibody library allowed the isolation of single-chain Fv (scFv) antibodies that were highly specific for ASP, and displayed closely related third complementarity determining regions of the variable heavy chain domain (V(H)-CDR3). BIAcore analysis demonstrated dissociation constants at the micromolar range: 1.6 x 10(-6) and 2.0 x 10(-6) M for ASP and the complete AChE-S protein, respectively. The anti-ASP antibodies provide a novel tool for studying the synaptic AChE-S variant, the expression of which is altered in ageing and dementia.

PubMedSearch : Flores-Flores_2002_J.Neural.Transm.Suppl_62_165
PubMedID: 12456061

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Citations formats

Flores-Flores C, Nissim A, Shochat S, Soreq H (2002)
Development of human antibody fragments directed towards synaptic acetylcholinesterase using a semi-synthetic phage display library
J Neural Transm Suppl 62 :165

Flores-Flores C, Nissim A, Shochat S, Soreq H (2002)
J Neural Transm Suppl 62 :165