Synthesis and biological activity of hydroxamic acid-derived vasopeptidase inhibitor analogues

[structure: see text] Syntheses of novel hydroxamic acid-derived azepinones containing pendant mercaptoacyl groups or formyl hydroxamates are described. These new analogues of therapeutically important ACE and NEP inhibitors include unprecedented changes at the previously assumed essential acid component.     

Synthesis of oxa-bridged analogues of farnesyltransferase inhibitor RPR 115135

Two synthetic routes to new oxygen-bridged analogues of farnesyltransferase inhibitors are described that follow either a [3 + 2]/[4 + 2] or a [4 + 2]/[3 + 2] sequence of reactions. The first approach has been achieved by reacting the in situ generated phenylisobenzofuran (PIBF) 4 with pyrroline 5a and has led stereoselectively to racemic 18, which was transformed in a few steps into the target molecule 2. The second pathway relies on a key intermediate 6, obtained either by condensation of PIBF with methyl acrylate, followed by a deprotonation/selenation and an oxidation/elimination sequence, or by cycloaddition between PIBF and alpha-phenylselenoacrylate 11, followed by the same oxidation/elimination sequence. The reaction of 6 with amino dipole 7 gives diastereoselective access to pyrrolidine 25, a precursor of the second target 3, an epimer of 2.     

Synthesis of photoactive analogues of a cystine knot trypsin inhibitor protein

We describe the preparation of a recently described photoactive amino acid analogue (photoMethionine) by two novel synthetic routes, one of which is flexible and enantiospecific, and the site-specific chemical incorporation of photoMethionine into a defined and functionally active protein using a combination of solid-phase peptide synthesis and modern chemical ligation methodology. Site-specific labeling of proteins with this amino acid analogue through chemical synthesis provides valuable probes for photoaffinity cross-linking studies.     

Synthesis of macrocyclic peptide analogues of proteasome inhibitor TMC-95A

The synthesis of three constrained macrocyclic peptide analogues 1 of TMC-95A as potential proteasome inhibitors is described. The key step involves a Ni(0)-mediated macrocyclization of tripeptides 2 bearing halogenated aromatic side chains for the formation of the biaryl junction. In addition, an enantioselective preparation of l-7-bromotryptophan methyl ester 3 using a Corey-O'Donnell alkylation of the glycine benzophenone imine was achieved in good overall yield with very high ee (>85%) on a multigram scale.     

Synthesis of dihydrolysergol analogues

As a part of a search for novel biological active ergoline derivatives, the indole ring present in the ergoline skeleton (indole[4,3‐f,g]quinoline) was converted into different heterocyclic ring systems such as quinazoline 2 , benzofurane 3 and benzoxazole 4 . Due to the paramount importance of chirality to attain biological activity, natural dihydrolysergic acid 1 was chosen as starting material and a synthetic pathway conservative in term of chirality was followed.     

Synthesis of cyclosporin analogues

Analogues of Cyclosporin modified at positions 1 and/or 2 have been synthesised; synthesis of linear peptides was investigated by fragment condensation and stepwise synthesis and a number of cyclisation methods were evaluated.Synthesis of [(Me)(Thr¹)]-, (Hyp¹)-, (Hyp¹, Nle²)-, [(Me)Ser¹]-, (Me)Ser¹, Nle²]-, [(Me)Ser¹, Nva]- [(Me)Thr¹, Nle²]-, [(Me)Thr¹, Nva]-, [(Me)Ser¹, Thr²]- and [Dab¹]- Cyclosporins and constituent fragments are described.     

Synthesis of indazole C-nueleosides and analogues

1-Deoxy-1-diazo-3,6-anhydro-4,5,7-tri-O-benzoyl-D-allo-heptulosc (III) has been prepared from 2,5-anhydro-3,4,6-tri-O-benzoyl-D-allonic acid. 1,3-Dipolar cycloaddition of III to benzyne afforded the indazole C-nucleoside analog V. Cycloaddition of methyl 6-deoxy-6-diazo-2,3-O-isopropylidene-β-D-ribohexofuranosid-5-ulose (IV) to the benzyne generated from 5-methyl-anthranilic acid gave a mixture of the β-isomeric C-glycosylindazoles VI and VII along with traces of the corresponding α-anomers VIa and VIIa. Finally, a multistep transformation of the acyclic carbohydrate moiety of 2,3,4,5-tetra-O-acetyl-1-(indazol-3-yl)-keto-D-ribopentulose (I, R = H, n = 3 , D-ribo) led to the C-nucleoside indazole, 3-(2,3-O-isopropylidene-β-D-ribofuranosyl)-indazol (X), as the major product.     

胞壁酰二肽(MDP)及其类似物的合成

本文报道胞壁酰二肽(MDP)及其类似物MDP[γ-Abu]^1、MDP-Oxalys的合成。应用一些新的合成方法和一种新型高效缩合剂, 简化了合成步骤, 提高了收率。     

Synthesis of asperopterin-B and some analogues

Homolytic 1-hydroxyalkylation on 8-methylisoxanthopterin by a primary or secondary alcohol and ammonium peroxydisulfate in a pH 5-6 phosphate buffer gave two naturally occuring pteridines, Asperopterin-B and 6-(1-hydroxypropyl)-8-methylisoxanthopterin, and several analogues.     

Synthesis of selenium analogues of the naturally occurring glycosidase inhibitor salacinol and their evaluation as glycosidase inhibitors

The syntheses of two selenium analogues (10 and 11) of the naturally occurring sulfonium ion, salacinol (3), are described. Salacinol is one of the active principles in the aqueous extracts of Salacia reticulata that are traditionally used in Sri Lanka and India for the treatment of diabetes. The synthetic strategy relies on the nucleophilic attack of a 2,3,5-tri-O-benzyl-1,4-anhydro-4-seleno-D-arabinitol at the least hindered carbon of benzyl- or benzylidene-protected D- or L-erythritol-1,3-cyclic sulfate. The use of 1,1,1,3,3,3-hexafluoro-2-propanol as a solvent in the coupling reaction proves to be beneficial. Enzyme inhibition assays indicate that 10 is a better inhibitor (K(i) = 0.72 mM) of glucoamylase than 3, which has a K(i) value of 1.7 mM. In contrast, 11 showed no significant inhibition of glucoamylase. Compounds 10 and 11 showed no significant inhibition of barley-alpha-amylase or porcine pancreatic-alpha-amylase.     

Synthesis of psoralens and analogues.

This review presents briefly the various classical syntheses of psoralens and angelicins which generally start from preformed suitably substituted coumarin or benzofuran derivatives. However, the discovery of the photocyclo-C-4 addition of psoralens to pyrimidine bases prompted new developments in this area. In particular, improved synthesis of psoralens and substituted angelicins, and synthesis of new analogues such as furochromenes, pyridopsoralens, pyrano benzopyrandiones, dioxinocoumarins and aza-psoralens were described recently. This review focuses on the chemical syntheses of these various compounds.     

Synthesis of thioglycoside-based UDP-sugar analogues

Arbuzov reaction of O-acetyl-protected glycosylthiomethyl chlorides with triethyl phosphite and then phosphonate ethyl ester cleavage with trimethylsilyl bromide afforded glycosylthiomethyl phosphonates 13, 18, 22, and 26. These intermediates could be readily transformed into the O-deprotected phosphonates 7-10 and into title compounds 1-4. Similarly, sulfonomethyl phosphonate moieties containing UDP-sugar analogues 5 and 6 were obtained.     

Synthesis of bridged aza-rebeccamycin analogues

The syntheses of rebeccamycin analogues possessing a 7-azaindole moiety instead of an indole unit, and with both indole and azaindole moieties linked to the carbohydrate are described. In these bridged aza compounds, the oxygen of the pyranose heterocycle is oriented towards either the indole, or the azaindole unit. In these series, compounds bearing a free imide nitrogen were synthesized by coupling the corresponding aglycones with a sugar pre-tosylated in 2-position via a Mitsunobu reaction. To obtain a precursor for bridged aza-rebeccamycin analogues substituted in 6-position on the sugar moiety, a 2,6-ditosylated sugar was used.     

Synthesis of chiral cyclam analogues

Chiral non-racemic analogues of cyclam were prepared via reaction of (1R, 2R)-cyclohexane-1,2-diamine with appropriately substituted malonyl dichlorides. Larger macrocycles are formed as by-products in some cases. All new macrocycles were characterised by X-ray crystallography.     

Synthesis of cyclobutane serine analogues

In this paper, we describe a thermal [2 + 2] cycloaddition involving 2-acylaminoacrylates as electron-poor acceptor alkenes, a reaction that involves a Michael-Dieckmann-type process. The reaction gives rise to a new substituted cyclobutane skeleton that can be transformed into amino acid derivatives. For example, a number of transformations were carried out to give the two pairs of stereoisomers of the 2-hydroxycyclobutane-alpha-amino acid serine analogue (c(4)Ser); compounds 22 and 23. This synthesis covers a gap in knowledge in the broad field of restricted amino acids.     

Synthesis of granulatimide bis-imide analogues

The synthesis of dipyrrolo[3,4-a:3,4-c]carbazole-1,3,4,6-tetraones, structurally related to granulatimide is reported. These compounds can be considered as granulatimide analogues in which a maleimide heterocycle replaces the imidazole moiety. The synthesis of pyridino[2,3-b]dipyrrolo[3,4-e:3,4-g]indole-1,3,4,6-tetraones is also reported. In these compounds, a 7-azaindole unit replaces the indole moiety present in the granulatimide and isogranulatimide structures.     

Synthesis of carbamate-containing cyclodextrin analogues

[formula: see text] The one-pot cyclooligomerization of a saccharide-derived p-nitrophenyl carbamate monomer was developed to generate a series of novel carbamate-containing cyclodextrin analogues. The "transcarbamoylation" occurs by initial base-induced activation to the isocyanate, followed by polycondensation/cyclization of the isocyanato alcohol. In the presence of NaH, only cyclized oligomers were observed, suggesting the importance of Na+ in promoting the efficiency of the cyclization process. The facile deprotection of the oligomers was achieved.     

Synthesis of C-nor-heterocyclic steroid analogues

2-Substituted-amino-10H-thiazolo[5,4-b]benz[e]indene derivatives 5 representing a novel ring system were synthesized. Their acylation led to exo-acylated derivatives 9 that could be converted to the corresponding glycine analogues 12 .