Nitrogen Arylation for Macrocyclization of Unprotected Peptides

Lautrette, Guillaume; Touti, Faycal; Lee, Hong Geun; Dai, Peng; Pentelute, Bradley L.

doi:10.1021/jacs.6b03757

Cited by 109 publications

(126 citation statements)

References 42 publications

Supporting

Mentioning

121

Contrasting

Unclassified

Order By: Relevance

“…Considering natural residues, cysteine (Cys) has been the residue of choice for stapling through alkylation,3 arylation,4 cycloaddition,4b and disulfide forming reactions both at native5 or engineered6 Cys residues. More recently, nitrogen arylation has also been shown to be a useful strategy for macrocyclization of lysine residues on peptides 7. Otherwise, efficient macrocyclization of linear peptides through the formation of an oxadiazole has also been reported 8.…”

mentioning

confidence: 99%

Oxetane Grafts Installed Site‐Selectively on Native Disulfides to Enhance Protein Stability and Activity In Vivo

et al. 2017

View full text Add to dashboard Cite

A four‐membered oxygen ring (oxetane) can be readily grafted into native peptides and proteins through site‐selective bis‐alkylation of cysteine residues present as disulfides under mild and biocompatible conditions. The selective installation of the oxetane graft enhances stability and activity, as demonstrated for a range of biologically relevant cyclic peptides, including somatostatin, proteins, and antibodies, such as a Fab arm of the antibody Herceptin and a designed antibody DesAb‐Aβ against the human Amyloid‐β peptide. Oxetane grafting of the genetically detoxified diphtheria toxin CRM197 improves significantly the immunogenicity of this protein in mice, which illustrates the general utility of this strategy to modulate the stability and biological activity of therapeutic proteins containing disulfides in their structures.

show abstract

mentioning

confidence: 99%

Oxetane Grafts Installed Site‐Selectively on Native Disulfides to Enhance Protein Stability and Activity In Vivo

et al. 2017

View full text Add to dashboard Cite

show abstract

mentioning

confidence: 99%

Palladium‐Mediated Arylation of Lysine in Unprotected Peptides

et al. 2017

Self Cite

View full text Add to dashboard Cite

A mild method for the arylation of lysine in an unprotected peptide is presented. In the presence of a preformed biarylphosphine-supported Pd(II)-aryl complex and weak base, lysine amino groups underwent C–N bond formation at room temperature. The process generally exhibited high selectivity for lysine over other amino acids containing nucleophilic side chains and was applicable to the conjugation of a variety of organic compounds, including complex drug molecules, with an array of peptides. Lastly, this method was also successfully applied to the formation of cyclic peptides via macrocyclization.

show abstract

“…Recently, we have reported a lysine stapling strategy with highly electron deficient arenes that proceeds via S N Ar to form chemically and biologically stable constructs that addresses the aforementioned concerns. 27 In the presence of a stapling reagent derived from 1,2-bis(4-bromophenoxy)ethane, p53 peptide with an additional lysine residue underwent facile macrocyclization (Scheme 2). The protocol provided access to both [i, i+4] and [i, i+7] stapled products with comparable efficiencies.…”

mentioning

confidence: 99%

“…The reaction allows for the formation of N-aryl conjugates, which are more stable than the corresponding S-aryl conjugates. 27 Furthermore, this protocol operates under mild conditions and is selective over most other nucleophilic amino acid residues. The success of this method stems from the use of the biarylphosphine ligands BrettPhos and t-BuBrettPhos in conjunction with the mildly basic sodium phenoxide.…”

mentioning

confidence: 99%

Palladium‐Mediated Arylation of Lysine in Unprotected Peptides

et al. 2017

Self Cite

View full text Add to dashboard Cite

A mild method for the arylation of lysine in an unprotected peptide is presented. In the presence of a preformed biarylphosphine‐supported palladium(II)–aryl complex and a weak base, lysine amino groups underwent C−N bond formation at room temperature. The process generally exhibited high selectivity for lysine over other amino acids containing nucleophilic side chains and was applicable to the conjugation of a variety of organic compounds, including complex drug molecules, with an array of peptides. Finally, this method was also successfully applied to the formation of cyclic peptides by macrocyclization.

show abstract

Nitrogen Arylation for Macrocyclization of Unprotected Peptides

Cited by 109 publications

References 42 publications

Oxetane Grafts Installed Site‐Selectively on Native Disulfides to Enhance Protein Stability and Activity In Vivo

Oxetane Grafts Installed Site‐Selectively on Native Disulfides to Enhance Protein Stability and Activity In Vivo

Palladium‐Mediated Arylation of Lysine in Unprotected Peptides

Palladium‐Mediated Arylation of Lysine in Unprotected Peptides

Contact Info

Product

Resources

About