Progress on Phage Display Technology: Tailoring Antibodies for Cancer Immunotherapy

Author:

França Renato Kaylan Alves12ORCID,Studart Igor Cabral34,Bezerra Marcus Rafael Lobo34,Pontes Larissa Queiroz34,Barbosa Antonio Marcos Aires35ORCID,Brigido Marcelo Macedo1ORCID,Furtado Gilvan Pessoa34ORCID,Maranhão Andréa Queiroz1ORCID

Affiliation:

1. Molecular Immunology Laboratory, Department of Cellular Biology, Institute of Biological Sciences, University of Brasilia, Brasilia 70910-900, Brazil

2. Graduate Program in Molecular Pathology, University of Brasilia, Brasilia 70910-900, Brazil

3. Oswaldo Cruz Foundation, Fiocruz Ceará, Eusébio 61773-270, Brazil

4. Graduate Program in Biotechnology of Natural Resources, Federal University of Ceará, Fortaleza 60440-970, Brazil

5. Graduate Program in Applied Informatics, University of Fortaleza, Fortaleza 60811-905, Brazil

Abstract

The search for innovative anti-cancer drugs remains a challenge. Over the past three decades, antibodies have emerged as an essential asset in successful cancer therapy. The major obstacle in developing anti-cancer antibodies is the need for non-immunogenic antibodies against human antigens. This unique requirement highlights a disadvantage to using traditional hybridoma technology and thus demands alternative approaches, such as humanizing murine monoclonal antibodies. To overcome these hurdles, human monoclonal antibodies can be obtained directly from Phage Display libraries, a groundbreaking tool for antibody selection. These libraries consist of genetically engineered viruses, or phages, which can exhibit antibody fragments, such as scFv or Fab on their capsid. This innovation allows the in vitro selection of novel molecules directed towards cancer antigens. As foreseen when Phage Display was first described, nowadays, several Phage Display-derived antibodies have entered clinical settings or are undergoing clinical evaluation. This comprehensive review unveils the remarkable progress in this field and the possibilities of using clever strategies for phage selection and tailoring the refinement of antibodies aimed at increasingly specific targets. Moreover, the use of selected antibodies in cutting-edge formats is discussed, such as CAR (chimeric antigen receptor) in CAR T-cell therapy or ADC (antibody drug conjugate), amplifying the spectrum of potential therapeutic avenues.

Funder

FAP-DF

CAPES

CNPq-DCIT

Publisher

MDPI AG

Subject

Virology,Infectious Diseases

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