1. Academic Validation
  2. David vs. Goliath: The Structure, Function, and Clinical Prospects of Antibody Fragments

David vs. Goliath: The Structure, Function, and Clinical Prospects of Antibody Fragments

  • Antibodies (Basel). 2019 Apr 9;8(2):28. doi: 10.3390/antib8020028.
Adam Bates 1 Christine A Power 2
Affiliations

Affiliations

  • 1 Biopharm Molecular Discovery, GlaxoSmithKline, Hertfordshire SG1 2NY, UK. adam.x.bates@gsk.com.
  • 2 Biopharm Molecular Discovery, GlaxoSmithKline, Hertfordshire SG1 2NY, UK. christine.a.power@gsk.com.
Abstract

Since the licensing of the first monoclonal antibody therapy in 1986, monoclonal Antibodies have become the largest class of biopharmaceuticals with over 80 Antibodies currently approved for a variety of disease indications. The development of smaller, antigen binding antibody fragments, derived from conventional Antibodies or produced recombinantly, has been growing at a fast pace. Antibody fragments can be used on their own or linked to Other molecules to generate numerous possibilities for bispecific, multi-specific, multimeric, or multifunctional molecules, and to achieve a variety of biological effects. They offer several advantages over full-length monoclonal Antibodies, particularly a lower cost of goods, and because of their small size they can penetrate tissues, access challenging epitopes, and have potentially reduced immunogenicity. In this review, we will discuss the structure, production, and mechanism of action of EMA/FDA-approved fragments and of those in clinical and pre-clinical development. We will also discuss current topics of interest surrounding the potential use of antibody fragments for intracellular targeting and blood-brain barrier (BBB) penetration.

Keywords

ADC; BiTE®; ImmTAC®; Nanobody®; TandAb; V-NAR; antibody fragments; diabodies; domain antibodies; fab; scFv.

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