2016
DOI: 10.1039/c6mb00219f
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Library-based display technologies: where do we stand?

Abstract: Over the past two decades, library-based display technologies have been staggeringly optimized since their appearance in order to mimic the process of natural molecular evolution. Display technologies are essential for the isolation of specific high-affinity binding molecules (proteins, polypeptides, nucleic acids and others) for diagnostic and therapeutic applications in cancer, infectious diseases, autoimmune, neurodegenerative, inflammatory pathologies etc. Applications extend to other fields such as antibo… Show more

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Cited by 98 publications
(77 citation statements)
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“…Unnatural amino acid-containing peptidomimetics can be developed by single-residue scanning of a parent sequence or scaffold [14], computational and rational design, or phenotype and/or genotype-linked display from phage [23] or yeast [24]. N -Alkyl amino acids (e.g.…”
Section: Unnatural Amino Acidsmentioning
confidence: 99%
See 1 more Smart Citation
“…Unnatural amino acid-containing peptidomimetics can be developed by single-residue scanning of a parent sequence or scaffold [14], computational and rational design, or phenotype and/or genotype-linked display from phage [23] or yeast [24]. N -Alkyl amino acids (e.g.…”
Section: Unnatural Amino Acidsmentioning
confidence: 99%
“…Using advances in molecular evolution and display, investigators rapidly selected high-affinity candidates from their library of 147 noncanonical and unnatural amino acids. Phage display is well established, and there are also other techniques, such as yeast display, based on combinatorial molecular display or in vitro compartmentalization, which are amenable to the display of unnatural amino acids [23]. …”
Section: Unnatural Amino Acidsmentioning
confidence: 99%
“…In this context, microbial biotechnology already provides important solutions at various levels, such as increasing production yields in bioreactors using microorganisms (i.e. yeasts, bacteria), reducing the time and cost associated with the slow growth of mammalian cells, and assisting on the optimization and engineering of biologics thanks to the high cloning capacity of microorganisms and the efficient screening methods of microbial libraries (Hoogenboom, 2005; Galan et al ., 2016). In addition to these conventional technologies, microbial engineering is developing innovative approaches to produce and deliver complex biologics in situ , within the body, ideally in a controlled and programmable way.…”
Section: Biologics and Microbial Engineeringmentioning
confidence: 99%
“…Puromycin functions to mimic the role of amino-acyl tRNA by attaching itself to a DNA primer affixed to the mRNA template. This allows puromycin to attach itself covalently to the nascent antibody protein based on the peptidyl transferase activity of the ribosome [12,22].…”
Section: Antibody Engineering 18mentioning
confidence: 99%
“…The covalent display technology (CDT) exploits the properties of the replication initiator protein from E. coli bacteriophage P2 [31]. A pool of DNA encoding antibody molecules is generated as a fusion to the P2A coding sequence [12]. The DNA pool is then transcribed and translated using cell free expression systems.…”
Section: Antibody Engineering 18mentioning
confidence: 99%