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Journal article

Antibody informatics for drug discovery

From

Astellas Pharma Inc.1

Sanofi Aventis Deutschland GmbH2

La Jolla Institute for Allergy & Immunology3

Department of Systems Biology, Technical University of Denmark4

Center for Biological Sequence Analysis, Department of Systems Biology, Technical University of Denmark5

MedImmune Ltd.6

European Bioinformatics Institute7

Université de Montpellier8

More and more antibody therapeutics are being approved every year, mainly due to their high efficacy and antigen selectivity. However, it is still difficult to identify the antigen, and thereby the function, of an antibody if no other information is available. There are obstacles inherent to the antibody science in every project in antibody drug discovery.

Recent experimental technologies allow for the rapid generation of large-scale data on antibody sequences, affinity, potency, structures, and biological functions; this should accelerate drug discovery research. Therefore, a robust bioinformatic infrastructure for these large data sets has become necessary.

In this article, we first identify and discuss the typical obstacles faced during the antibody drug discovery process. We then summarize the current status of three sub-fields of antibody informatics as follows: (i) recent progress in technologies for antibody rational design using computational approaches to affinity and stability improvement, as well as ab-initio and homology-based antibody modeling; (ii) resources for antibody sequences, structures, and immune epitopes and open drug discovery resources for development of antibody drugs; and (iii) antibody numbering and IMGT.

Here, we review “antibody informatics,” which may integrate the above three fields so that bridging the gaps between industrial needs and academic solutions can be accelerated. This article is part of a Special Issue entitled: Recent advances in molecular engineering of antibody.

Language: English
Year: 2014
Pages: 2002-2015
ISSN: 18781454 , 15709639 , 18782434 and 00063002
Types: Journal article
DOI: 10.1016/j.bbapap.2014.07.006
ORCIDs: Marcatili, Paolo , 0000-0002-0756-5149 , 0000-0002-5859-1064 , 0000-0003-0116-9353 and 0000-0003-2820-1608

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