Induced Folding of Protein‐Sized Foldameric β‐Sandwich Models with Core β‐Amino Acid Residues

Olajos, Gábor; Hetényi, Anasztázia; Wéber, Edit; Németh, Lukács; Szakonyi, Zsolt; Fülöp, Ferenc; Martinek, Tamás A.

doi:10.1002/chem.201405581

Cited by 15 publications

(11 citation statements)

References 68 publications

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“…b-Sheet forming a/b-peptides were designed too [123][124][125][126][127][128]. Importantly, these structures might be useful in PPI modification where water-accessible flat surfaces play a crucial role.…”

Section: B-peptidesmentioning

confidence: 99%

An overview of peptide and peptoid foldamers in medicinal chemistry

Mándity¹,

Fülöp²

2015

Expert Opinion on Drug Discovery

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Various new foldamers have been created with a range of structures and biological applications. Membrane-acting antibacterial foldamers have been introduced. A general property of these structures is their amphiphilic nature. The amphiphilicity can be stationary or induced by the membrane binding. Cell-penetrating foldamers have been described which serve as cargo molecules, and foldamers have been used as autophagy inducers. Anti-Alzheimer compounds too have been created and the greatest breakthrough was attained via the modification of protein-protein interactions. This can serve as the chemical and pharmaceutical basis for the relevance of foldamers in the future.

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Section: B-peptidesmentioning

confidence: 99%

An overview of peptide and peptoid foldamers in medicinal chemistry

Mándity¹,

Fülöp²

2015

Expert Opinion on Drug Discovery

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“…In protein prosthesis, 6,7 backbone engineering 8 allows individual residues or sequences within proteins to be replaced with non-natural residues. [9][10][11][12][13] Notable examples include the incorporation of b-amino acid residues in the B1 domain of Streptococcal protein G (GB1) 14 and Betabellin-14, 15 the re-engineering of a heterodimeric chorismate mutase enzyme 16 using sequence based design, the replacement of loop regions in GB1 using PEG 17 and the incorporation of an entire b-amino acid topological mimic of an a-helix into IL8. 18 a-Helix mimetics [19][20][21][22][23] employ a suitably functionalised generic scaffold to reproduce the spatial projection and composition of key side chains found at a helical interface between two proteins.…”

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confidence: 99%

Towards “bionic” proteins: replacement of continuous sequences from HIF-1α with proteomimetics to create functional p300 binding HIF-1α mimics

et al. 2016

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“…Replacing  residues with a hydrophobic surface area similar to (1R,2S)-ACHC (1c and 1d) resulted in a high original -sheet content and a low inducibility, which highlighted the importance of the compatibility of the sidechain with the hydrophobic core. 16 The cyclic side-chain fitted into the peripheral regions of the inner core, but substitution in the centre of the tightly packed core was unfavourable (1a, 1b, 2a and 2b). It has previously been shown that appropriate orientation of the side-chains facilitates the hydrophobic interactions that play crucial roles in -sheet folding, and they are scaled up by increasing temperature.…”

Section: Please Do Not Adjust Marginsmentioning

confidence: 99%