Automated Screening Procedure for High-Throughput Generation of Antibody Fragments | Zendy

Johan Hallborn | Zendy; Roland Carlsson | Zendy

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Automated Screening Procedure for High-Throughput Generation of Antibody Fragments

Author(s) -

Johan Hallborn,

Roland Carlsson

Publication year - 2002

Publication title -

biotechniques

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 0.617

H-Index - 131

eISSN - 1940-9818

pISSN - 0736-6205

DOI - 10.2144/dec02-hallborn

Subject(s) - proteome , proteomics , phage display , computational biology , computer science , high throughput screening , peptide library , antibody , biology , microbiology and biotechnology , bioinformatics , genetics , peptide sequence , gene

In the emerging field of proteomics, there is an urgent need for catcher molecules such as antibodies for detecting the proteome or parts of the proteome in a microarray format. A suitable source for providing a large diversity of binders is obtained by combinatorial libraries, such as phage display libraries of single chain antibody fragments (scFv) or Fab fragments. To find novel binders from the n-CoDeR libraries with a high throughput, we have automated the screening process with robotics. The automated system is configured to screen tens of thousands of clones per day to target antigens in various formats, including peptides and soluble proteins, as well as cell-bound targets; thus, it is well designed to meet demands from the proteomics area.

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