Stepwise and one-pot cross-coupling-heteroannulation approaches toward 2-substituted C5-, C6-, and C7-nitroindoles

A general and efficient synthesis of 2-substituted C5-, C6-, and C7-nitroindoles has been established. Starting from commercially available 2-amino nitrophenols, C5-, C6-, and C7-nitroindoles were synthesized via the stepwise Pd-catalyzed cross-coupling of nitro 2-trifloxyanilides with 1-alkynes followed by the t-BuOK-mediated heteroannulation. A Pd-catalyzed one-pot coupling-heteroannulation procedure was carried out by using nitro 2-trifluoroacetamidoaryl triflates.     

C,C- and C,N-Chelated Organocopper Compounds

Copper-catalyzed and organocopper-involved reactions are of great significance in organic synthesis. To have a deep understanding of the reaction mechanisms, the structural characterizations of organocopper intermediates become indispensable. Meanwhile, the structure-function relationship of organocopper compounds could advance the rational design and development of new Cu-based reactions and organocopper reagents. Compared to the mono-carbonic ligand, the C,N- and C,C-bidentate ligands better stabilize unstable organocopper compounds. Bidentate ligands can chelate to the same copper atom via η²-mode, forming a mono-cupra-cyclic compounds with at least one acute C-Cu-C angle. When the bidentate ligands bind to two copper atoms via η¹-mode at each coordinating site, the bimetallic macrocyclic compounds will form nearly linear C-Cu-C angles. The anionic coordinating sites of the bidentate ligand can also bridge two metals via μ₂-mode, forming organocopper aggregates with Cu-Cu interactions and organocuprates with contact ion pair structures. The reaction chemistry of some selected organocopper compounds is highlighted, showing their unique structure–reactivity relationships.     

Tumescenamide C,an antimicrobial cyclic lipodepsipeptide from Streptomyces sp.

Tumescenamide C, a new cyclic lipodepsipeptide, was isolated from a culture broth of an actinomycete Streptomyces sp. KUSC_F05. Tumescenamide C was a congener of tumescenamides A and B, representing a sixteen-membered ring system, consisting of two proteinogenic and three non-proteinogenic amino acids, to which a methyl-branched fatty acid was attached. The planar structure was determined by spectroscopic analysis, while its absolute stereochemistry was determined by chemical degradation and asymmetric synthesis. Tumescenamide C exhibited antimicrobial activity with high selectivity against Streptomyces species.     

Synthesis, biology, and modeling of a C-4 carbonyl C,D-seco-taxoid

A C,D-seco-paclitaxel derivative 26 was prepared from taxine and tested for biological activity. Chemical reactivity of the seco-compounds proved to be substantially modified, with respects to taxoids. The corresponding C,D-seco-taxoid does not show tubulin stabilizing activity or cytotoxicity. Explanation of these observations based on molecular modeling is provided.     

epi-Aszonalenins A, B, and C from Aspergillus novofumigatus

Three new benzodiazepines have been isolated from an unusual chemotype of Aspergillus novofumigatus: epi-aszonalenins A, B, and C. The structures were elucidated by use of one- and two-dimensional NMR spectroscopic techniques and HR ESI MS. The relative configuration was established on the basis of a single crystal X-ray diffraction study of epi-aszonalenin A and the absolute configuration was determined by optical rotation comparison with the literature data. The absolute configurations of epi-aszonalenins B and C were determined by circular dichroism comparison to epi-aszonalenin A.     

Preparation of C5-substituted O,5′-cyclouridine

The synthesis of hitherto unknown C5-substituted O⁶,5′-cyclouridines is described. The 2′,3′-isopropylidene-uridine was treated with N-halogenosuccinimides forming appropriate bridged 5-halogeno derivatives. Using lithiation method, bromine substituent at C5 position was exchanged into various alkyl and alkenyl derivatives.     

Total synthesis of maremycins A,B, C1/C2, D1, and D2

The total synthesis of maremycins A, B, C₁/C₂, D₁, and D₂ is achieved starting from the natural amino acids l-isoleucine and S-methyl-l-cysteine, in which the total synthesis of maremycins B, C₁/C₂, and D₂ is accomplished for the first time. The synthesis features a position-selective intramolecular bromination process for the synthesis of key chiral building block, a Pd-catalyzed indole synthesis for the preparation of (2S,3S)-β-methyltryptophan and hydroxylation of oxindoles by molecular oxygen. In addition, the protocol for conversion of maremycins A and B to maremycins C and D was improved.     

C(C6F4PPh2-o)NMe a C,P-chelate and C,N-bridging ligand. Crystal structure of

Addition of PPh₂H and base to cis-[{Pd₂(μ-Cl)₂[μ-C((C₆F₅)=N(Me)]₂}_n] results in formation of a CP bond at the expense of a CF bond to give the title complex, the crystal structure of which has been determined.     

Studies towards the total synthesis of cruentaren A and B: Stereoselective synthesis of fragments C1-C11, C12-C22 and C23-C28

A convergent and stereoselective approach for the synthesis of C1-C11, C12-C22, and C23-C28 fragments of cytotoxic natural products cruentaren A and B are accomplished. Highlights of the strategy include a Sharpless epoxidation followed by a regioselective opening of epoxide to generate anti and syn-stereochemistry at C9-C10 and C15-C16, an Alder-Rickert reaction between a 1,5-dimethoxy-1,4-cyclohexadiene and dienophile to construct the aromatic ring, and a lithium-mediated aldol reaction to install the C17-C18 anti-stereochemistry. The synthesis of C1-C11 and C12-C22 fragments proceed with a longest linear sequence of 10 and 17 steps from commercially available 2-butyne-1,4-diol and cis-2-butene-1,4-diol respectively.     

Synthesis, modification, and optical properties of C3-ethynylated chlorophyll derivatives

3-Ethynyl-chlorin was prepared from methyl pyropheophorbide-d using Bestmann-Ohira reagent. The mono-substituted acetylene was subjected to copper-free, Pd-mediated coupling to form chlorin derivatives possessing a series of substituted ethynyl groups at the C3-position. Its 1,3-dipolar cycloadditions with azido compounds were also demonstrated.     

Polycavernoside C and C2, the new analogs of the human lethal toxin polycavernoside A, from the red alga, Gracilaria edulis

Two new analogs of the human lethal toxin polycavernoside A, polycavernoside C and C2 (0.1-0.2 mg for each), were isolated from the red alga, Gracilaria edulis. The relative stereostructure of polycavernoside C and the absolute structure of polycavernoside C2 were determined by spectroscopic analysis and synthesis of the model of their aglycon.     

Relationship between the CaF2 (C 1) and CdCl2 (C 19) structure types,with assorted remarks on C 19, anti-C 19, and related compounds

It is shown how the 6:(3 + 3)-coordinated AB₂ layer structure of the C 19 type can be derived by continuous rhombohedral distortion from the cubic 8:8-coordinated C 1-type structure. The magnitude of the distortion actually observed (as manifested in the $\text{c}\text{a}$ ratio per AB₂ layer, R₁) is considered in relation to geometric factors, with particular attention to the competing CdI₂ (C 6) structure type. Reasons are suggested for the nonoccurrence of the C 19 structure type among M(OH)₂ and of the anti-C 19 type among the simple hexahalometallates(IV), A₂MX₆. Finally, the structures of alkylammonium hexahalometallates(IV), (R_nNH_4?n)₂MX₆, are surveyed to demonstrate how the charge arrangements of the composite cations and anions in these compounds are able to mimic the structure types encountered with simple AB₂ compounds.     

Total synthesis of diastereomeric marine butenolides possessing a syn-aldol subunit at C10 and C11 and the related C11-ketone

Two diastereomeric marine butenolides, (4S,10R,11R)- and (4S,10S,11S)-4,11-dihydroxy-10-methyldodec-2-en-1,4-olide, possessing a syn-aldol subunit at C10 and C11 have been efficiently synthesized by using a three-module coupling strategy. The enantiomeric syn-aldol modules prepared by the syn-selective aldol reaction of the norephedrine-derived chiral propionates were coupled with the chiral C3-C7 module via 1,3-dithiane bisalkylation. The butenolide ring was then installed via a high-yielding ring-closing metathesis (RCM) reaction. Oxidation of the diastereomeric C11-alcohols furnished the corresponding C11-ketones, which are produced by the same marine microorganism.     

The stereoselective total syntheses of pectinolides A,B, and C

The stereoselective total synthesis of pectinolide B has been accomplished for the first time along with total syntheses of pectinolides A and C. MacMillan α-hydroxylation and Sharpless asymmetric dihydroxylation reactions are involved in generating the three stereogenic centers. Other important transformations in the synthesis are Z-selective Still–Gennari olefination, selective benzylation of the homoallylic alcohol, and a one-pot MOM deprotection followed by lactonization leading to all three pectinolides A–C being synthesized from a common intermediate. Pectinolides A, B, and C were synthesized from n-hexanal in 19, 20, and 18 steps with overall yields of 8.8%, 6.72%, and 9.2%, respectively.     

Agariblazeispirol C from the cultured mycelia of the fungus, Agaricus blazei, and the chemical conversion of blazeispirol A

Agariblazeispirol C, which has a unique steroidal skeleton, has been isolated from the cultured mycelia of Agaricus blazei (Agaricaceae). The structure of agariblazeispirol C was established to be (23S,24S)-13,23-cyclo-25-hydroxy-14β-methyl-18-nor-des-A-ergosta-5,7,9,11,17(20)-pentaen-22-one by comparison of extensive 1D and 2D NMR spectral data with those of agariblazeispirols A and B. At the same time, agariblazeispirol C was synthesized by the reaction of blazeispirol A with BF₃·OEt₂ along with some interesting compounds.     

Stemona-amines C–E,new alkaloids from Stemona tuberosa

Three new alkaloids, stemona-amines C–E, were isolated from the roots of Stemona tuberosa Lour. (Stemonaceae). The structures of stemona-amines C and D were determined by X-ray crystallography and that of stemona-amine E was determined by interpretation of spectroscopic data. The absolute structures of stemona-amines C and D were established by VCD spectroscopy.     

Salarin C, a new cytotoxic sponge-derived nitrogenous macrolide

A novel nitrogenous macrolide, designated salarin C (3), was isolated from the Madagascan sponge Fascaplysinopsis sp. The structure of the compound was elucidated by interpretation of MS and 1D and 2D NMR spectra. Salarin C is closely related to salarin A and is considered to be the precursor of salarins A and B (1,2). Air oxidation was found to transform 3 to 1. Salarin C was found to inhibit cell proliferation of human leukeamic cell lines UT-7 and K562 and the murine pro-B cell line Ba/F3 at concentrations of 0.0005-0.5 mg/ml. A possible biogenesis is discussed.     

Synthesis of the C8-C20 and C21-C30 segments of pectenotoxin 2

In this study, we synthesized the C8-C20 and C21-C30 segments of the diarrhetic shellfish toxin pectenotoxin 2. The C8-C20 segment was assembled from a phosphonate corresponding to the C8-C15 segment (prepared from l-malic acid in 19 steps) and an aldehyde corresponding to the C16-C20 segment (synthesized from 3-methyl-3-butenol in nine steps) by a twelve-step process including the Horner-Wadsworth-Emmons reaction, regio- and stereoselective reduction of the resulting enone, diastereoselective epoxidation, and 5-exo epoxide cleavage forming the C-ring. The C21-C30 segment was constructed in 13 steps from (S)-glycidol via a route involving E-ring formation by 5-exo epoxide cleavage and stereoselective methylation at C27 by the Evans method.     

First synthesis of decaturin C,an antiinsectant diterpenoid isolated from Penicillium thiersii

The first synthesis of (+)-decaturin C, an antiinsectant diterpenoid isolated from Penicillium thiersii, was accomplished by starting from (R)-(?)-Wieland–Miescher ketone, in which our original spiro-cyclization reaction was featured as a key step.