Potent and Specific Inhibition of Glycosidases by Small Artificial Binding Proteins (Affitins)

Correa, Agustín; Pacheco, Sabino; Mechaly, A.E.; Obal, Gonzalo; Béhar, Ghislaine; Mouratou, Barbara; Oppezzo, Pablo; Alzari, Pedro M.; Pecorari, Frédéric

doi:10.1371/journal.pone.0097438

Cited by 44 publications

(57 citation statements)

References 51 publications

(83 reference statements)

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“…The deletion of three residues from the ␣-helix end of D1Sac7d could also explain the decrease in activity observed for D1Sso7d. In fact, we observed in the three-dimensional structure of a lysozyme/anti-lysozyme Affitin complex that this part of the Affitin was in contact with lysozyme (Correa et al, 2014). This work illustrates the difficulty to anticipate possible effects on binding activity of a mutational/grafting approach, even when applied to a rigid region (Kahsai et al, 2005) of the protein.…”

Section: Figmentioning

confidence: 80%

“…The method of improving a scaffold for binding is often driven by structure/function relationships with other proteins. For instance, the binding mode of antibodies involving CDR loops has inspired the engineering of new generations of Monobodies, DARPins, and Affitins with artificially extended loop(s) (Correa et al, 2014;Koide et al, 2012;Schilling et al, 2014).…”

Section: Introductionmentioning

confidence: 99%

“…Binders with high pH and thermal stabilities have been obtained by coupling the generation of combinatorial libraries of Sac7d variants corresponding to the randomization of 10-14 residues of the ␤-sheet surface originally involved in the binding of DNA and selections against different targets. We recently reported that natural (Béhar et al, 2013) or artificially extended loops (Correa et al, 2014) of Sac7d can be advantageously recruited to generate Affitins, some of them showing potent inhibition properties by penetrating deep into a glycosidase active site.…”

Section: Introductionmentioning

confidence: 99%

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Switching an anti-IgG binding site between archaeal extremophilic proteins results in Affitins with enhanced pH stability

Béhar

Pacheco

Maillasson

et al. 2014

Journal of Biotechnology

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As a useful reagent for biotechnological applications, a scaffold protein needs to be as stable as possible to ensure longer lifetimes. We have developed archaeal extremophilic proteins from the “7 kDa DNA-binding” family as scaffolds to derive affinity proteins (Affitins). In this study, we evaluated a rational structure/sequence-guided approach to stabilize an Affitin derived from Sac7d by transferring its human IgG binding site onto the framework of the more thermally stable Sso7d homolog. The chimera obtained was functional, well expressed in Escherichia coli, but less thermally stable than the original Affitin (T(m) = 74.2 °C vs. T(m) = 80.4 °C). Two single mutations described as thermally stabilizing wild type Sso7d were introduced into chimeras. Only the double mutation nearly restored thermal stability (T(m) = 76.9 °C). Interestingly, the chimera and its double mutant were stable from pH 0 up to at least pH 13. Our results show that it is possible to increase further the stability of Affitins toward alkaline conditions (+2 pH units) while conserving their advantageous properties. As Affitins are based on a growing family of homologs from archaeal extremophiles, we conclude that this approach offers new potential for their improvement, which will be useful in demanding biotechnological applications.

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Section: Figmentioning

confidence: 80%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Switching an anti-IgG binding site between archaeal extremophilic proteins results in Affitins with enhanced pH stability

Béhar

Pacheco

Maillasson

et al. 2014

Journal of Biotechnology

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“…DSC experiments were carried out in PBS as described previously49 using a VP-DSC instrument (Microcal, Northampton, MA) and data was analyzed with the software supplied with the equipment.…”

Section: Methodsmentioning

confidence: 99%

The archaeal “7 kDa DNA-binding” proteins: extended characterization of an old gifted family

Kalichuk

Béhar

Renodon-Cornière

et al. 2016

Sci Rep

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The “7 kDa DNA-binding” family, also known as the Sul7d family, is composed of chromatin proteins from the Sulfolobales archaeal order. Among them, Sac7d and Sso7d have been the focus of several studies with some characterization of their properties. Here, we studied eleven other proteins alongside Sac7d and Sso7d under the same conditions. The dissociation constants of the purified proteins for binding to double-stranded DNA (dsDNA) were determined in phosphate-buffered saline at 25 °C and were in the range from 11 μM to 22 μM with a preference for G/C rich sequences. In accordance with the extremophilic origin of their hosts, the proteins were found highly stable from pH 0 to pH 12 and at temperatures from 85.5 °C to 100 °C. Thus, these results validate eight putative “7 kDa DNA-binding” family proteins and show that they behave similarly regarding both their function and their stability among various genera and species. As Sac7d and Sso7d have found numerous uses as molecular biology reagents and artificial affinity proteins, this study also sheds light on even more attractive proteins that will facilitate engineering of novel highly robust reagents.

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“…These two mini‐proteins are ideal candidates to study in atomic detail the interplay between native interactions and interactions at the protein surface. Affitin H4 is an artificial protein able to selectively bind antigens that can be easily engineered to recognize various protein or DNA targets.…”

Section: Introductionmentioning

confidence: 99%

Artificial proteins as allosteric modulators of PDZ3 and SH3 in two‐domain constructs: A computational characterization of novel chimeric proteins

et al. 2016

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Artificial multidomain proteins with enhanced structural and functional properties can be utilized in a broad spectrum of applications. The design of chimeric fusion proteins utilizing protein domains or one-domain miniproteins as building blocks is an important advancement for the creation of new biomolecules for biotechnology and medical applications. However, computational studies to describe in detail the dynamics and geometry properties of two-domain constructs made from structurally and functionally different proteins are lacking. Here, we tested an in silico design strategy using all-atom explicit solvent molecular dynamics simulations. The well-characterized PDZ3 and SH3 domains of human zonula occludens (ZO-1) (3TSZ), along with 5 artificial domains and 2 types of molecular linkers, were selected to construct chimeric two-domain molecules. The influence of the artificial domains on the structure and dynamics of the PDZ3 and SH3 domains was determined using a range of analyses. We conclude that the artificial domains can function as allosteric modulators of the PDZ3 and SH3 domains. Proteins 2016; 84:1358-1374. © 2016 Wiley Periodicals, Inc.

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Potent and Specific Inhibition of Glycosidases by Small Artificial Binding Proteins (Affitins)

Cited by 44 publications

References 51 publications

Switching an anti-IgG binding site between archaeal extremophilic proteins results in Affitins with enhanced pH stability

Switching an anti-IgG binding site between archaeal extremophilic proteins results in Affitins with enhanced pH stability

The archaeal “7 kDa DNA-binding” proteins: extended characterization of an old gifted family

Artificial proteins as allosteric modulators of PDZ3 and SH3 in two‐domain constructs: A computational characterization of novel chimeric proteins

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