RIPPA: Identification of MHC‐II Binding Peptides from Antigen Using a Yeast Display‐Based Approach

Liu, Rongzeng; Jiang, Wei; Li, Ying; Mellins, Elizabeth

doi:10.1002/cpz1.350

Cited by 2 publications

(1 citation statement)

References 16 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Combining phage display with yeast display is particularly useful for developing high affinity TCRL mAbs ( 71 ). Since first developed ( 42 ), yeast display technology has evolved, allowing surface display of monomeric or dimeric protein scaffolds ( 72 , 73 ). Thus, either scFv or Fab identified from a phage-Ab library can be affinity matured using the yeast platform.…”

Section: Generation Of Tcrl Mabs Targeting P/mhc-ii Complexesmentioning

confidence: 99%

TCR-like antibodies targeting autoantigen-mhc complexes: a mini-review

2022

Self Cite

View full text Add to dashboard Cite

T cell receptors (TCRs) recognize peptide antigens bound to major histocompatibility complex (MHC) molecules (p/MHC) that are expressed on cell surfaces; while B cell-derived antibodies (Abs) recognize soluble or cell surface native antigens of various types (proteins, carbohydrates, etc.). Immune surveillance by T and B cells thus inspects almost all formats of antigens to mount adaptive immune responses against cancer cells, infectious organisms and other foreign insults, while maintaining tolerance to self-tissues. With contributions from environmental triggers, the development of autoimmune disease is thought to be due to the expression of MHC risk alleles by antigen-presenting cells (APCs) presenting self-antigen (autoantigen), breaking through self-tolerance and activating autoreactive T cells, which orchestrate downstream pathologic events. Investigating and treating autoimmune diseases have been challenging, both because of the intrinsic complexity of these diseases and the need for tools targeting T cell epitopes (autoantigen-MHC). Naturally occurring TCRs with relatively low (micromolar) affinities to p/MHC are suboptimal for autoantigen-MHC targeting, whereas the use of engineered TCRs and their derivatives (e.g., TCR multimers and TCR-engineered T cells) are limited by unpredictable cross-reactivity. As Abs generally have nanomolar affinity, recent advances in engineering TCR-like (TCRL) Abs promise advantages over their TCR counterparts for autoantigen-MHC targeting. Here, we compare the p/MHC binding by TCRs and TCRL Abs, review the strategies for generation of TCRL Abs, highlight their application for identification of autoantigen-presenting APCs, and discuss future directions and limitations of TCRL Abs as immunotherapy for autoimmune diseases.

show abstract