| Literature DB >> 22328160 |
Sang-Chul Lee1, Keunwan Park, Jieun Han, Joong-jae Lee, Hyun Jung Kim, Seungpyo Hong, Woosung Heu, Yu Jung Kim, Jae-Seok Ha, Seung-Goo Lee, Hae-Kap Cheong, Young Ho Jeon, Dongsup Kim, Hak-Sung Kim.
Abstract
Repeat proteins have recently been of great interest as potential alternatives to immunoglobulin antibodies due to their unique structural and biophysical features. We here present the development of a binding scaffold based on variable lymphocyte receptors, which are nonimmunoglobulin antibodies composed of Leucine-rich repeat modules in jawless vertebrates, by module engineering. A template scaffold was first constructed by joining consensus repeat modules between the N- and C-capping motifs of variable lymphocyte receptors. The N-terminal domain of the template scaffold was redesigned based on the internalin-B cap by analyzing the modular similarity between the respective repeat units using a computational approach. The newly designed scaffold, termed "Repebody," showed a high level of soluble expression in bacteria, displaying high thermodynamic and pH stabilities. Ease of molecular engineering was shown by designing repebodies specific for myeloid differentiation protein-2 and hen egg lysozyme, respectively, by a rational approach. The crystal structures of designed repebodies were determined to elucidate the structural features and interaction interfaces. We demonstrate general applicability of the scaffold by selecting repebodies with different binding affinities for interleukin-6 using phage display.Entities:
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Year: 2012 PMID: 22328160 PMCID: PMC3295290 DOI: 10.1073/pnas.1113193109
Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN: 0027-8424 Impact factor: 11.205