The Staudinger Ligation

Bednarek, Christin; Wehl, Ilona; Jung, Nicole; Schepers, Ute; Bräse, Stefan

doi:10.1021/acs.chemrev.9b00665

Cited by 207 publications

(162 citation statements)

References 365 publications

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“…In this synthesis, a modified traceless Staudinger ligation was developed and applied to the stereoselective construction of the sterically cumbersome ( E )/( Z )‐ΔIle residues in solution (Figure 1 b). [21–25] We found that introducing two CF 3 groups and one methoxy group of 9 to the original phosphinophenol structure drastically improved the efficiency of the enamide formation from alkenyl azide 10 . When 9 and 10 were coupled in an aqueous solvent at room temperature, N 2 expulsion, intramolecular amidation from 11 , and release of phosphine oxide 12 proceeded to generate 13 with retention of the original E / Z stereochemistry of 10 .…”

Section: Resultsmentioning

confidence: 94%

“…In this synthesis, am odifiedt raceless Staudinger ligationw as developed and applied to the stereoselectivec onstruction of the sterically cumbersome( E)/(Z)-DIle residues in solution (Figure1b). [21][22][23][24][25] We found that intro-ducing two CF 3 groups ando ne methoxy group of 9 to the originalphosphinophenol structure drastically improved the efficiency of the enamide formation from alkenyla zide 10.W hen 9 and 10 werecoupled in an aqueous solvent at room temperature, N 2 expulsion, intramolecular amidation from 11,a nd release of phosphine oxide 12 proceeded to generate 13 with retention of the original E/Z stereochemistryo f10.A dduct 13 was in turn converted to the requisite Fmoc-protected dipeptide 15 by at wo-stepp rotective group manipulation. The three dipeptides with the (E)/(Z)-DIle residues were thus prepared and employed for peptide elongation on resin to attain the solid-phase total synthesis of 1.…”

Section: Resultsmentioning

confidence: 99%

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Divergent Solid‐Phase Synthesis and Biological Evaluation of Yaku'amide B and Its Seven E/Z Isomers

Kamiya

Miura

Itoh

et al. 2020

Chemistry A European J

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Yaku′amide B (1) inhibits cancer cell growth through a unique mechanism of action. Compound 1 binds to mitochondrial FoF1‐ATP synthase, inhibits ATP production, and enhances ATP hydrolysis. The presence of one (E)‐ and two (Z)‐α,β‐dehydroisoleucines (ΔIle) in the linear 13‐mer sequence is the most unusual structural feature of 1. To uncover the biological importance of these residues, we synthesized 1 and its seven E/Z isomers 2–8 by devising a new divergent solid‐phase strategy. Both the (E)‐ and (Z)‐ΔIle residues were stereoselectively constructed by traceless Staudinger ligation on resin to ultimately deliver 1–8. All isomers 2–8 displayed effects on the inhibition of cell growth and ATP production, and enhanced ATP hydrolysis, thus indicating that 2–8 share the same mode of action as 1. The least potent isomer, 8, was isomeric at three ΔIle residues of the most potent 1. These findings together indicate that the E/Z stereochemistry of the three ΔIle residues controls the magnitude of the biological functions of 1.

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Section: Resultsmentioning

confidence: 94%

Section: Resultsmentioning

confidence: 99%

Divergent Solid‐Phase Synthesis and Biological Evaluation of Yaku'amide B and Its Seven E/Z Isomers

Kamiya

Miura

Itoh

et al. 2020

Chemistry A European J

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“…While the structure of the aryl azide dictates its reactivity, [33][34][35] functionalised aryl azides have relatively high biological stability, with selective reactivity for strained alkenes and alkynes ([3+2]-cycloadditions), [35][36][37] triphenylphosphines (Staudinger reaction), 38 or H 2 S. [39][40][41] We have developed the alkene-azide [3+2]-cycloaddition as a bioorthogonal click-to-release reaction for prodrugs 28,29,32 and hydrogels, 30,31 while others have investigated H 2 S; a gaseous transmitter in the body, as an activation mechanism for aryl azide-containing probes, prodrugs, and materials. [39][40][41] Alkyl azides can also be reduced by H 2 S 42 or glutathione, 43 however, aryl azides are considered more responsive to, and selective toward, alkenes and H 2 S, 44 even in the presence of other endogenous thiol/thiolate species (e.g., glutathione).…”

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confidence: 99%

Synthesis and formulation of self‐immolative PEG‐aryl azide block copolymers and click‐to‐release reactivity with trans‐cyclooctene

Dadhwal

Lee

Goswami

et al. 2021

Journal of Polymer Science

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Self-immolative aryl azides can react with trans-cyclooctenes (TCO), triphenylphosphines or hydrogen sulfide (H 2 S) to activate prodrugs, imaging probes and drug delivery systems. To date, the synthesis of polymers containing these aryl azide self-immolative linkers and their reactivity with a strained alkene (i.e., in a bioorthogonal reaction) has not been explored. Also, due to the instability of aryl azides towards light and high temperatures, the polymerization methods compatible with aryl azides are limited. Through systematic investigation of the reversible addition-fragmentation chain transfer (RAFT) and atom transfer radical polymerization (ATRP) methods, a self-immolative PEG-aryl azide block copolymer (PEG 45-b-ABOC 28 2) and a non-responsive 4-fluoroaryl block copolymer (PEG 45-b-FBOC 24 3) was prepared. ATRP provided the desired polymers in a highly controlled manner, whereas the RAFT conditions led to higher levels of aryl azide polymer degradation. The ATRP derived polymers 2 and 3 were formulated into nanoparticles of approximately 200 nm diameter, and particle triggering was demonstrated by the [3+2]cycloaddition reaction of TCO with PEG 45-b-ABOC 28 2 in solution (pure polymer) and as a formulated nanoparticle. Preliminary in vitro cell viability studies suggested that the stimuli-responsive aryl azide polymers/nanoparticles are not cytotoxic up to 200 μg/ml concentrations.

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“…[16] The most well-established routes for the formation of amides involve the reactiono fa mines with activated carboxylic acids or their corresponding derivatives, [17] the Schmidt reaction, [18] the Beckmann rearrangement reaction, [19] and modified Staudinger reaction. [20] From the perspective of green chemistry,t hesep rocesses generate al arge amount of byproducts andc hemical waste, so they need to be improved or replaced. Thus, much effort is being devoted to making the formation of amide bonds more "green."…”

Section: Introductionmentioning

confidence: 99%

Visible‐Light‐Mediated Oxidative Amidation of Aldehydes by Using Magnetic CdS Quantum Dots as a Photocatalyst

Zhang

et al. 2021

Chemistry A European J

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Am agnetic CdS quantum dot(Fe 3 O 4 /polydopamine (PDA)/CdS) was synthesized through af acile and convenient method from inexpensives tarting materials. Characterization of the prepared catalyst was performedb ym eans of FTIR spectroscopy,X RD, SEM, TEM, energy-dispersive Xray spectroscopy, and vibrating-samplem agnetometert ech-niques. Fe 3 O 4 /PDA/CdS was found to be ah ighly active photocatalyst for the amidation of aromatic aldehydes by using air as ac lean oxidantu nder mild conditions. The photocatalyst can be recovered by magnetic separation and successfully reused for five cycles without considerable loss of its catalytic activity.

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The Staudinger Ligation

Cited by 207 publications

References 365 publications

Divergent Solid‐Phase Synthesis and Biological Evaluation of Yaku'amide B and Its Seven E/Z Isomers

Divergent Solid‐Phase Synthesis and Biological Evaluation of Yaku'amide B and Its Seven E/Z Isomers

Synthesis and formulation of self‐immolative PEG‐aryl azide block copolymers and click‐to‐release reactivity with trans‐cyclooctene

Visible‐Light‐Mediated Oxidative Amidation of Aldehydes by Using Magnetic CdS Quantum Dots as a Photocatalyst

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