Long-range PEG stapling: macrocyclization for increased protein conformational stability and resistance to proteolysis

Xiao, Qiang; Ashton, Dallin S; Jones, Zachary; Thompson, Katherine P.; Price, Joshua L.

doi:10.1039/d0cb00075b

Cited by 10 publications

(12 citation statements)

References 93 publications

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“…[27][28][29][30][31][32][33] We recently showed that stapling via olefin metathesis vs. the copper-catalyzed azide-alkyne cycloaddition (CuAAC) provide similar increases in the conformational stability of WW, a βsheet miniprotein derived from the WW domain of the human protein Pin1. 34,35 We observed similar levels of stabilization for staples comprised of discrete polyethylene glycol oligomers (i.e., PEG staples) vs. conventional hydrocarbon staples. The most important determinant of PEG-staple-based stabilization in WW is that the two crosslinked groups be far apart in primary sequence but close together in the folded tertiary structure.…”

Section: Introductionmentioning

confidence: 64%

“…27–33 We recently showed that stapling via olefin metathesis vs. the copper-catalyzed azide–alkyne cycloaddition (CuAAC) provide similar increases in the conformational stability of WW, a β-sheet miniprotein derived from the WW domain of the human protein Pin1. 34,35 We observed similar levels of stabilization for staples comprised of discrete polyethylene glycol oligomers ( i.e. , PEG staples) vs. conventional hydrocarbon staples.…”

Section: Introductionmentioning

confidence: 67%

“…We then prepared PEG-stapled variant sd27e/29g'-z4x from d27e/29g'-z4x via CuAAC, which connects the azide of z4 to the alkyne of x via a triazole linkage (Figure 2C,D). 35 Our approach differs from that of Arora and coworkers 48,49 in the structure of the z4x staple and its placement between eand g'-positions that are not involved in a salt bridge with each other: in the structure of parent compound dA/B, Glu27 is involved in a salt bridge with Lys22', whereas Lys29' is involved in a salt bridge with Glu34.…”

Section: Resultsmentioning

confidence: 93%

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Structural guidelines for stabilization of α-helical coiled coils via PEG stapling

et al. 2022

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Section: Introductionmentioning

confidence: 64%

Section: Introductionmentioning

confidence: 67%

Section: Resultsmentioning

confidence: 93%

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Structural guidelines for stabilization of α-helical coiled coils via PEG stapling

et al. 2022

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“…In particular, INCYPRO provides straight‐forward access to diverse linker structures. [81] In general, it can be expected that more cyclization strategies will be developed which allow the simultaneous introduction of an additional functionality (e. g. PEG chains [84] or photo‐switchable moieties[ 85 , 86 ]).…”

Section: Discussionmentioning

confidence: 99%

Protein Macrocyclization for Tertiary Structure Stabilization

2021

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Proteins possess unique molecular recognition capabilities and enzymatic activities, features that are usually tied to a particular tertiary structure. To make use of proteins for biotechnological and biomedical purposes, it is often required to enforce their tertiary structure in order to ensure sufficient stability under the conditions inherent to the application of interest. The introduc-tion of intramolecular crosslinks has proven efficient in stabilizing native protein folds. Herein, we give an overview of methods that allow the macrocyclization of expressed proteins, discussing involved reaction mechanisms and structural implications.

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“…Interestingly, steric hindrance by these size-increasing moieties also protects against proteolytic degradation. [13][14][15] ; Class 2: increase in size via controlled oligomerization; 16 Class 3: covalent linking to long-living serum protein (e.g., FDA-approved drugs albiglutide and dulaglutide, exanatide that conjugated to albumin and the IfG4 Fc domain) [17][18][19] and Class 4: incorporation of moieties that bind non-covalently to serum proteins such as albumin, [20][21][22][23] immunoglobulin, 24,25 FcRn, 26 transthyretin, 27 and transferrin. 28,29 An important example in the last class is lipidation of peptides to allow interaction with serum albumin.…”

Section: Introductionmentioning

confidence: 99%

Genetically-Encoded Discovery of Perfluoroaryl-Macrocycles that Bind to Albumin and Exhibit Extended Circulationin-vivo

Wong

Kirberger

Qiu

et al. 2022

Preprint

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In this paper, we report selection of albumin-binding macrocyclic peptides from genetically encoded libraries of peptides modified by perfluoroaryl-cysteine SNAr chemistry. Modification of phage-displayed libraries SXCXnC-phage, n=3-5, where X is any amino acid except for cysteine by decafluoro-diphenylsulfone (DFS), yields genetically-encoded library of octafluoro-diphenylsulfone-crosslinked macrocycles (OFS-SXCXnC-phage). Selection from these libraries using albumin as a bait identified a family of significantly enriched perfluoroaryl-macrocycles. Synthesis of perfluoroaryl-macrocycles predicted by phage display and testing their binding properties by 19F NMR and fluorescent polarization identified OFS-macrocycle with SICRFFC sequence as the most potent albumin binder. We observed that OFS-macrocycles slowly react with biological nucleophiles such as glutathione. Replacing decafluoro-diphenylsulfone by nearly isosteric pentafluorophenyl sulfide yielded perfluorophenylsulfide (PFS)-crosslinked macrocycles devoid of undesired reactivity. The augmented lead PFS-macrocycle with SICRFFC sequence exhibited KD = 4-6 μM towards human serum albumin and similar affinities towards rat and mouse albumins. When injected in mouse, the PFS-SICRFFCGGG compound was significantly retained in circulation in vivo when compared to control PFS-macrocyclic peptide. The perfluoroaryl-macrocycles with SICRFFC motif are the smallest known peptide macrocycle with significant affinity for human albumin and they are a productive starting point for future development of compact macrocycles with predictable circulation half-life in vivo.

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Long-range PEG stapling: macrocyclization for increased protein conformational stability and resistance to proteolysis

Abstract: Long-range stapling of two Asn-linked PEG oligomers via olefin metathesis substantially increases the conformational stability of the WW and SH3 domain tertiary structures and the GCN4 coiled-coil quaternary structure.

Cited by 10 publications

References 93 publications

Structural guidelines for stabilization of α-helical coiled coils via PEG stapling

Structural guidelines for stabilization of α-helical coiled coils via PEG stapling

Protein Macrocyclization for Tertiary Structure Stabilization

Genetically-Encoded Discovery of Perfluoroaryl-Macrocycles that Bind to Albumin and Exhibit Extended Circulationin-vivo

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