Sortase-mediated backbone cyclization of proteins and peptides

Hof, Wim van ’t; Maňásková, Silvie Hansenová; Veerman, E.C.I.; Bolscher, Jan G. M.

doi:10.1515/hsz-2014-0260

Cited by 39 publications

(30 citation statements)

References 46 publications

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“…Recent examples include the synthesis of camelid-derived antibody fragment conjugates for the treatment of B-cell lymphoma, the installation of non-isotopically labeled protein domains to facilitate NMR analysis of proteins with limited solubility, the construction of immuno-PET reagents for non-invasive cancer imaging, and the preparation of multifunctional protein nanoparticles [2–5]. This is by no means an exhaustive list, and we refer the reader to other excellent reviews for more comprehensive discussions of sortagging applications [6–10]. Rather than focus on applications, our goal for this review is to provide an overview of advances in sortagging methodology itself.…”

Section: Introductionmentioning

confidence: 99%

Recent advances in sortase-catalyzed ligation methodology

Antos

Truttmann

Ploegh

2016

Current Opinion in Structural Biology

144

139

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The transpeptidation reaction catalyzed by bacterial sortases continues to see increasing use in the construction of novel protein derivatives. In addition to growth in the number of applications that rely on sortase, this field has also seen methodology improvements that enhance reaction performance and scope. In this opinion, we present an overview of key developments in the practice and implementation of sortase-based strategies, including applications relevant to structural biology. Topics include the use of engineered sortases to increase reaction rates, the use of redesigned acyl donors and acceptors to mitigate reaction reversibility, and strategies for expanding the range of substrates that are compatible with a sortase-based approach.

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Section: Introductionmentioning

confidence: 99%

Recent advances in sortase-catalyzed ligation methodology

Antos

Truttmann

Ploegh

2016

Current Opinion in Structural Biology

144

139

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“…The use of enzymes as biocatalysts in peptide cyclization increasingly attracted attention due to their nontoxic nature, cost‐effectiveness, and high chemoselectivity. With the development of protein engineering biotechnology, a variety of enzymes have been exploited for peptide cyclization, such as butelase, trypsin, protease OaAEP1b, prenyl transferase, PatG, sortase, subtiligase, peptiligase, thioesterase, glutathione S‐transferase, transglutaminase, etc. In 2002, Kohli et al discovered an isolated thioesterase, which displayed the capability of catalyzing the cyclization of linear peptides tethered to a carrier protein via a phosphopantetheine linker.…”

Section: Strategies To Develop Cyclic Peptides Into Therapeutic Agentsmentioning

confidence: 99%

A gold mine for drug discovery: Strategies to develop cyclic peptides into therapies

Jing

Jin

2019

Medicinal Research Reviews

121

130

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As a versatile therapeutic modality, peptides attract much attention because of their great binding affinity, low toxicity, and the capability of targeting traditionally “undruggable” protein surfaces. However, the deficiency of cell permeability and metabolic stability always limits the success of in vitro bioactive peptides as drug candidates. Peptide macrocyclization is one of the most established strategies to overcome these limitations. Over the past decades, more than 40 cyclic peptide drugs have been clinically approved, the vast majority of which are derived from natural products. The de novo discovered cyclic peptides on the basis of rational design and in vitro evolution, have also enabled the binding with targets for which nature provides no solutions. The current review summarizes different classes of cyclic peptides with diverse biological activities, and presents an overview of various approaches to develop cyclic peptide‐based drug candidates, drawing upon series of examples to illustrate each strategy.

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“…If the end goal is selective modification of a specific protein terminus, then such dual-functionalized derivatives should be avoided, as they may be susceptible to intramolecular transpeptidation, giving rise to circular protein products (Antos et al, 2009b; Jia et al, 2014; van ’t Hof, Maňásková, Veerman, & Bolscher, 2015). In certain cases, proteins containing a C-terminal LPXTG site and an N-terminal glycine may be amenable to site-specific modification at both sites.…”

Section: Strategic Planningmentioning

confidence: 99%

“…Notable examples include the ligation of proteins or peptides to fluorophores (Popp et al, 2007; Yamamoto & Nagamune, 2009), carbohydrates (Samantaray, Marathe, Dasgupta, Nandicoori, & Roy, 2008; Wu, Guo, Wang, Swarts, & Guo, 2010), polymers (Parthasarathy et al, 2007; Qi, Amiram, Gao, McCafferty, & Chilkoti, 2013), solid supports (Chan et al, 2007; Le, Raeeszadeh-Sarmazdeh, Boder, & Frymier, 2015; Sinisi et al, 2012), therapeutics (Beerli, Hell, Merkel, & Grawunder, 2015; Fang et al, 2016), lipids (Antos et al, 2008; Wu et al, 2010), nucleic acids (Koussa, Sotomayor, & Wong, 2014; Pritz et al, 2007), metal chelators (Paterson et al, 2014; Westerlund, Honarvar, Tolmachev, & Eriksson Karlström, 2015), viral particles (Hess et al, 2013; Schoonen et al, 2015), live cells (Popp et al, 2007; Shi et al, 2014; Yamamoto & Nagamune, 2009), or even intramolecular ligations for generating cyclic proteins and peptides (Antos et al, 2009b; Jia et al, 2014; van ’t Hof et al, 2015). A full discussion of all relevant applications is beyond the scope of this unit, and we refer to the reader to reviews on this topic (Haridas, Sadanandan, & Dheepthi, 2014; Popp & Ploegh, 2011; Ritzefeld, 2014; Schmohl & Schwarzer, 2014).…”

Section: Commentarymentioning

confidence: 99%

Site‐Specific Protein Labeling via Sortase‐Mediated Transpeptidation

et al. 2017

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Strategies for site-specific protein modification are highly desirable for the construction of conjugates containing non-genetically-encoded functional groups. Ideally, these strategies should proceed under mild conditions, and be compatible with a wide range of protein targets and non-natural moieties. The transpeptidation reaction catalyzed by bacterial sortases is a prominent strategy for protein derivatization that possesses these features. Naturally occurring or engineered variants of sortase A from Staphylococcus aureus catalyze a ligation reaction between a five-amino-acid substrate motif (LPXTG) and oligoglycine nucleophiles. By pairing proteins and synthetic peptides that possess these ligation handles, it is possible to install modifications onto the protein N- or C-terminus in site-specific fashion. As described in this unit, the successful implementation of sortase-mediated labeling involves straightforward solid-phase synthesis and molecular biology techniques, and this method is compatible with proteins in solution or on the surface of live cells.

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Sortase-mediated backbone cyclization of proteins and peptides

Cited by 39 publications

References 46 publications

Recent advances in sortase-catalyzed ligation methodology

Recent advances in sortase-catalyzed ligation methodology

A gold mine for drug discovery: Strategies to develop cyclic peptides into therapies

Site‐Specific Protein Labeling via Sortase‐Mediated Transpeptidation

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