Semisynthetic prion protein (PrP) variants carrying glycan mimics at position 181 and 197 do not form fibrils

Araman, Can; Thompson, Robert E.; Wang, Siyao; Hackl, Stefanie; Payne, Richard J.; Becker, Christian F. W.

doi:10.1039/c7sc02719b

Cited by 23 publications

(27 citation statements)

References 53 publications

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“…Thus, lipopeptides can be used as mimics of the GPI anchor's ability to attach PrP to the cell membrane. A similar strategy with regard to using a lipidated peptide as a GPI‐mimicking membrane anchor was pursued by Becker et al, when starting to develop semisynthetic strategies, based on EPL and protein trans ‐splicing (PTS) (Figure ), to access to different posttranslationally modified PrP variants (Figure ) …”

Section: Semisynthesis Strategies For Prpmentioning

confidence: 99%

“…This strategy was aimed at introduction sugars into PrP but did not fully succeed. Shortly after that, Araman et al demonstrated a semisynthetic approach to generate PrP variants modified with monodisperse PEG chains as mimics of N ‐glycans that are similar in size and molar mass (Figure C). A new EPL strategy was established to achieve this, in which expressed PrP (aa 23‐177) with a C ‐terminal thioester is used in EPL reactions with PEGylated, synthetic peptides (aa 179‐231).…”

Section: Semisynthesis Strategies For Prpmentioning

confidence: 99%

“…Different strategies were utilized by Baskakov, 252 Baldwin, 253 Figure 4), to access to different posttranslationally modified PrP variants ( Figure 5). 228,241,[255][256][257][258][259][260][261] In the EPL 245,246 reaction, a protein thioester, obtained by cleaving a fusion protein consisting of the protein of interest (POI) and an intein, is linked to a chemically synthesized peptide 243 containing an N-terminal cysteine in a reaction similar to NCL. 244 An initial transesterifaction leads to formation of a thioester linking the recombinant and synthetic PrP segments, and a subsequent irreversible S → N acyl shift establishes the amide bond at the ligation site ( Figure 4A).…”

Section: Semisynthesis Strategies For Prpmentioning

confidence: 99%

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Prion protein—Semisynthetic prion protein (PrP) variants with posttranslational modifications

Hackl

Becker

2019

Journal of Peptide Science

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Deciphering the pathophysiologic events in prion diseases is challenging, and the role of posttranslational modifications (PTMs) such as glypidation and glycosylation remains elusive due to the lack of homogeneous protein preparations. So far, experimental studies have been limited in directly analyzing the earliest events of the conformational change of cellular prion protein (PrPC) into scrapie prion protein (PrPSc) that further propagates PrPC misfolding and aggregation at the cellular membrane, the initial site of prion infection, and PrP misfolding, by a lack of suitably modified PrP variants. PTMs of PrP, especially attachment of the glycosylphosphatidylinositol (GPI) anchor, have been shown to be crucially involved in the PrPSc formation. To this end, semisynthesis offers a unique possibility to understand PrP behavior in vitro and in vivo as it provides access to defined site‐selectively modified PrP variants. This approach relies on the production and chemoselective linkage of peptide segments, amenable to chemical modifications, with recombinantly produced protein segments. In this article, advances in understanding PrP conversion using semisynthesis as a tool to obtain homogeneous posttranslationally modified PrP will be discussed.

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Section: Semisynthesis Strategies For Prpmentioning

confidence: 99%

Section: Semisynthesis Strategies For Prpmentioning

confidence: 99%

Section: Semisynthesis Strategies For Prpmentioning

confidence: 99%

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Prion protein—Semisynthetic prion protein (PrP) variants with posttranslational modifications

Hackl

Becker

2019

Journal of Peptide Science

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“…Christian Becker (University of Vienna, Austria) discussed a semisynthetic approach to generate prion protein (PrP) variants modified with monodisperse poly(ethylene glycol) (PEG) units as mimics of N‐glycans. The incorporation of PEG at different glycosylation sites in PrP only induced small changes in the secondary structure, but effectively inhibited the aggregation of PrP in vitro …”

Section: Post‐translational Modifications and Artificial Peptides To mentioning

confidence: 99%

“…The incorporation of PEG at different glycosylation sites in PrP only induceds mall changesi n the secondary structure,b ut effectivelyi nhibited the aggregation of PrP in vitro. [26] Apart from glycoproteins, recent efforts in understanding PTMs such as SUMOylation, ubiquitylation, phosphorylation, and lipidation of proteins were also discussed. Champak Chatterjee (University of Washington, USA) presented his laboratory's efforts towards understanding the mechanistic basis of gene regulation by chromatin SUMOylation.…”

Section: Protein Synthesis Beyond the Ribosome: Advances In Chemical mentioning

confidence: 99%

Building Peptide Bonds in Haifa: The Seventh Chemical Protein Synthesis (CPS) Meeting

Lang

2017

ChemBioChem

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Synthesis of Asparagine Derivatives Harboring a Lewis X Type DC‐SIGN Ligand and Evaluation of their Impact on Immunomodulation in Multiple Sclerosis

Doelman

Marqvorsen

Chiodo

et al. 2020

Chemistry A European J

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The protein myelin oligodendrocyte glycoprotein (MOG) is a key component of myelin and an autoantigen in the disease multiple sclerosis (MS). Post‐translational N‐glycosylation of Asn31 of MOG seems to play a key role in modulating the immune response towards myelin. This is mediated by the interaction of Lewis‐type glycan structures in the N‐glycan of MOG with the DC‐SIGN receptor on dendritic cells (DCs). Here, we report the synthesis of an unnatural Lewis X (LeX)‐containing Fmoc‐SPPS‐compatible asparagine building block (SPPS=solid‐phase peptide synthesis), as well as asparagine building blocks containing two LeX‐derived oligosaccharides: LacNAc and Fucα1‐3GlcNAc. These building blocks were used for the glycosylation of the immunodominant portion of MOG (MOG31‐55) and analyzed with respect to their ability to bind to DC‐SIGN in different biological setups, as well as their ability to inhibit the citrullination‐induced aggregation of MOG31‐55. Finally, a cytokine secretion assay was carried out on human monocyte‐derived DCs, which showed the ability of the neoglycopeptide decorated with a single LeX to alter the balance of pro‐ and anti‐inflammatory cytokines, inducing a tolerogenic response.

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Semisynthetic prion protein (PrP) variants carrying glycan mimics at position 181 and 197 do not form fibrils

Abstract: Semisynthesis and characterization of homogeneously mono- and di-PEGylated full length PrP variants to study the impact of PEGylation (as N-glycan mimics) on protein folding and aggregation.

Cited by 23 publications

References 53 publications

Prion protein—Semisynthetic prion protein (PrP) variants with posttranslational modifications

Prion protein—Semisynthetic prion protein (PrP) variants with posttranslational modifications

Building Peptide Bonds in Haifa: The Seventh Chemical Protein Synthesis (CPS) Meeting

Synthesis of Asparagine Derivatives Harboring a Lewis X Type DC‐SIGN Ligand and Evaluation of their Impact on Immunomodulation in Multiple Sclerosis

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