Pd‐Catalyzed Asymmetric N‐Allylation of Amino Acid Esters with Exceptional Levels of Catalyst Control: Stereo‐Divergent Synthesis of ProM‐15 and Related Bicyclic Dipeptide Mimetics

Dohmen, Stephan; Reiher, Martin; Albat, Dominik; Akyol, Sema; Barone, M.; Neudörfl, Jörg‐Martin; Kühne, Ronald; Schmalz, Hans‐Günther

doi:10.1002/chem.202000307

Cited by 9 publications

(14 citation statements)

References 54 publications

(21 reference statements)

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“…The compounds employed in this study were synthesized by modular assembly of the building blocks using established coupling protocols ( 40 ). The required ProM scaffolds ProM-1 ( 41 , 43 ), ProM-2 ( 45 ), ProM-9 ( 46 ), ProM-13 ( 46 ), ProM-15 ( 47 ), and ProM-17 ( 47 ) ( Fig. 1 B ) were synthesized as separately published.…”

Section: Resultsmentioning

confidence: 99%

“…Such a modification opened the possibility to probe the underlying hydrophobic binding groove with different moieties (ProM-15 and ProM-17; Fig. 1 B ) ( 47 ). The resulting less rigid inhibitors 4a and 5a showed a greatly improved affinity toward ENAH EVH1 by –5.5 kJ/mol compared to 1a , thereby nearly restoring the binding energy of the TEDEL-containing chimera 2

N ( Table 1 ).…”

Section: Resultsmentioning

confidence: 99%

“…In the course of our research into small molecules as potential inhibitors of protein–protein interactions ( 39 ) we recently in silico designed and stereo-selectively synthesized scaffolds, coined ProMs, which mimic pairs of prolines in PPII conformation ( 40 ). The modular combination of different ProMs thereby allowed us to generate nonpeptidic secondary-structure mimetics that fulfill the steric requirements of the addressed proline-rich motif-recognizing domain ( 41 – 47 ). For the EVH1 domain, our proof-of-concept study yielded a canonically binding, nontoxic, cell-membrane-permeable, 706-Da inhibitor 1 ( Fig.…”

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confidence: 99%

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Designed nanomolar small-molecule inhibitors of Ena/VASP EVH1 interaction impair invasion and extravasation of breast cancer cells

Barone

Müller

Chiha

et al. 2020

Proc. Natl. Acad. Sci. U.S.A.

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Battling metastasis through inhibition of cell motility is considered a promising approach to support cancer therapies. In this context, Ena/VASP-depending signaling pathways, in particular interactions with their EVH1 domains, are promising targets for pharmaceutical intervention. However, protein–protein interactions involving proline-rich segments are notoriously difficult to address by small molecules. Hence, structure-based design efforts in combination with the chemical synthesis of additional molecular entities are required. Building on a previously developed nonpeptidic micromolar inhibitor, we determined 22 crystal structures of ENAH EVH1 in complex with inhibitors and rationally extended our library of conformationally defined proline-derived modules (ProMs) to succeed in developing a nanomolar inhibitor (Kd=120 nM,MW=734Da). In contrast to the previous inhibitor, the optimized compounds reduced extravasation of invasive breast cancer cells in a zebrafish model. This study represents an example of successful, structure-guided development of low molecular weight inhibitors specifically and selectively addressing a proline-rich sequence-recognizing domain that is characterized by a shallow epitope lacking defined binding pockets. The evolved high-affinity inhibitor may now serve as a tool in validating the basic therapeutic concept, i.e., the suppression of cancer metastasis by inhibiting a crucial protein–protein interaction involved in actin filament processing and cell migration.

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Section: Resultsmentioning

confidence: 99%

N ( Table 1 ).…”

Section: Resultsmentioning

confidence: 99%

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confidence: 99%

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Designed nanomolar small-molecule inhibitors of Ena/VASP EVH1 interaction impair invasion and extravasation of breast cancer cells

Barone

Müller

Chiha

et al. 2020

Proc. Natl. Acad. Sci. U.S.A.

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“…Unfortunately, all our attempts to obtain MediPhos‐Pd complexes as crystalline compounds remained unsuccessful so far. Therefore, it remains uncertain whether the coordination modes and geometries are similar to those of Trost‐type ligands and whether the higher activity of our ligands [8a] relates to the lack of NH units in the chiral bridge, which promote the formation of catalytically inactive tetra‐coordinate Pd(II) complexes [13]…”

Section: Resultsmentioning

confidence: 99%

“…Nevertheless, we recently reported a protocol which allows the Pd‐catalyzed asymmetric N ‐allylation of various amino acid esters with exceptional levels of catalyst control using i Pr‐MediPhos ( L3* ) as a chiral ligand (Scheme 2). [8] As an example, the N‐allylation of methyl glycinate ( 4 a ) with carbonates rac‐ 5 was achieved with high enantioselectivity and the products of type 6 were used in the synthesis of the ProM‐15 derivative 7 and related compounds [8a] …”

Section: Introductionmentioning

confidence: 99%

Improved Synthesis of MediPhos Ligands and Their Use in the Pd‐Catalyzed Enantioselective N‐Allylation of Glycine Esters

et al. 2021

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A new class of chiral C2‐symmetric diphosphines (MediPhos) was recently shown to give superior results in the Pd‐catalyzed asymmetric N‐allylation of amino acid esters. We here describe a new, improved protocol for the preparation of such ligands through bidirectional SN2‐coupling of a tartrate‐derived ditosylate with 6‐alkyl‐2‐bromophenols followed by double lithiation/phosphanylation. This method gave access to a series of nine ligands with branched alkyl substituents, which were benchmarked in the enantioselective Pd‐catalyzed N‐allylation of tert‐butyl glycinate with racemic (E)‐2,8‐dimethylnona‐5‐en‐4‐yl methyl carbonate (up to 95 % ee). In addition, the analogous transformation of tert‐butyl glycinate with methyl (E)‐nona‐5‐en‐4‐yl carbonate was optimized. The obtained allylic amines were then used in the stereoselective synthesis of the conformationally restricted proline‐derived dipeptide analogs ProM‐17 and ProM‐21.

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A General Stereocontrolled Synthesis of Opines through Asymmetric Pd‐Catalyzed N‐Allylation of Amino Acid Esters

2021

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A stereo-divergent synthesis of natural and unnatural opines in stereochemically pure form is based on the direct palladiumcatalyzed N-allylation of α-amino acid esters (up to 97 % ee or 99 : 1 d.r.) using methyl (E)-2-penten-4-yl carbonate in the presence of only 1 mol% of a catalyst, prepared in-situ from the C 2 -symmetric diphosphine iPr-MediPhos and [Pd(allyl)Cl] 2 . Selected target compounds (incl. a derivative of the drug enalapril) were efficiently obtained from the N-allylated intermediates by oxidative cleavage (ozonolysis) of the allylic C=C bond under temporary N-Boc-protection.

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Pd‐Catalyzed Asymmetric N‐Allylation of Amino Acid Esters with Exceptional Levels of Catalyst Control: Stereo‐Divergent Synthesis of ProM‐15 and Related Bicyclic Dipeptide Mimetics

Cited by 9 publications

References 54 publications

Designed nanomolar small-molecule inhibitors of Ena/VASP EVH1 interaction impair invasion and extravasation of breast cancer cells

Designed nanomolar small-molecule inhibitors of Ena/VASP EVH1 interaction impair invasion and extravasation of breast cancer cells

Improved Synthesis of MediPhos Ligands and Their Use in the Pd‐Catalyzed Enantioselective N‐Allylation of Glycine Esters

A General Stereocontrolled Synthesis of Opines through Asymmetric Pd‐Catalyzed N‐Allylation of Amino Acid Esters

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