Tumor-targeting domains for chimeric antigen receptor T cells Journal Articles

abstract

• Immunotherapy with chimeric antigen receptor (CAR) T cells has been advancing steadily in clinical trials. Since the ability of engineered T cells to recognize intended tumor-associated targets is crucial for the therapeutic success, antigen-binding domains play an important role in shaping T-cell responses. Single-chain antibody and T-cell receptor fragments, natural ligands, repeat proteins, combinations of the above and universal tag-specific domains have all been used in the antigen-binding moiety of chimeric receptors. Here we outline the advantages and disadvantages of different domains, discuss the concepts of affinity and specificity, and highlight the recent progress of each targeting strategy.

authors

• Bezverbnaya, Ksenia
• Mathews, Ashish
• Sidhu, Jesse
• Helsen, Christopher W
• Bramson, Jonathan

status

• published 

publication date

• January 2017

has subject area

• 1103 Clinical Sciences (FoR)
• 1107 Immunology (FoR)
• 1115 Pharmacology and Pharmaceutical Sciences (FoR)
• Animals (MeSH)
• Genetic Therapy (MeSH)
• Humans (MeSH)
• Immunotherapy, Adoptive (MeSH)
• Molecular Targeted Therapy (MeSH)
• Neoplasms (MeSH)
• Receptors, Antigen, T-Cell (MeSH)
• Recombinant Fusion Proteins (MeSH)
• T-Cell Antigen Receptor Specificity (MeSH)
• T-Lymphocytes (MeSH)

published in

• Immunotherapy  Journal

keywords

• Animals
• CAR
• Genetic Therapy
• Humans
• Immunotherapy, Adoptive
• Molecular Targeted Therapy
• Neoplasms
• Receptors, Antigen, T-Cell
• Recombinant Fusion Proteins
• T-Cell Antigen Receptor Specificity
• T-Lymphocytes
• adoptive cell therapy
• antigen recognition
• engineered T cells
• immunotherapy

Digital Object Identifier (DOI)

• 10.2217/imt-2016-0103

PubMed ID

• 28000526

start page

• 33

end page

• 46

volume

• 9

issue

• 1