Total synthesis and biological evaluation of pacidamycin D and its 3'-hydroxy analogue

Full details of the total synthesis of pacidamycin D (4) and its 3'-hydroxy analogue 32 are described. The chemically labile Z-oxyacyl enamide moiety is the most challenging chemical structure found in uridylpeptide natural products. Key elements of our approach to the synthesis of 4 include the efficient and stereocontrolled construction of the Z-oxyvinyl halides 6 and 7 and their copper-catalyzed cross-coupling with the tetrapeptide carboxamide 5, a thermally unstable compound containing a number of potentially reactive functional groups. This synthetic route also allowed us to easily prepare 3'-hydroxy analogue 32. The assemblage by cross-coupling of the Z-oxyvinyl halide 6 and the carboxamide 5 at a late stage of the synthesis provided ready access to a range of uridylpeptide antibiotics and their analogues, despite their inherent labile nature with potential epimerization, simply by altering the tetrapeptide moiety.     

Single Crystal of a Prussian Blue Analogue Based on Rubidium Manganese Hexacyanoferrate.

ChemInform is a weekly Abstracting Service, delivering concise information at a glance that was extracted from about 200 leading journals. To access a ChemInform Abstract, please click on HTML or PDF.     

Synthesis of some antipyrinylazo and thiazolylazo compounds with pentan-2,4-dione and their reactions with metal ions

The reagents were synthesized by using pentan-2,4-dione as the coupling component with diazotized 4-aminoantipyrine or 2-aminothiazole. Two kinds of azo compounds were obtained under different conditions: 1-(4-antipyrinylazo)-1-(4-antipyrinylhydrazino)propan-2-one (Azonol A-1) and 3-(4-antipyrinylazo)pentan-2,4-dione (Azonol A-2) from 4-aminoantipyrine, and 1-(2-thiazolylazo)-1-(2-thiazolylhydrazino)propan-2-one (TAA-1) and 3-(2-thiazolylazo)pentan-2,4-dione (TAA-2) from 2-aminothiazole. The structure of Azonol A-1 was determined by single-crystal x-ray crystallography. The reactions of these reagents with various metal ions were examined. Azonol A-1 and TAA-1 form metal chelates at low pH values. Azonol A-1 is useful as a metallochromic indicator in titrations of bismuth with EDTA at pH 0.5–2, and as a spectrophotometric reagent for copper (II) (0.2–1.5 mg l^?1) at pH 0.3–1.2.     

UVB DNA Dosimeters Analyzed by Polymerase Chain Reactions

Abstract— Purified bacteriophage Λ DNA was dried on a UV-tran-sparent polymer film and served as a UVB dosimeter for personal and ecological applications. Bacteriophage Λ. DNA was chosen because it is commercially available and inexpensive, and its entire sequence is known. Each dosimeter contained two sets of DNA sandwiched between UV-transparent polymer films, one exposed to solar radiation (experimental) and another protected from UV radiation by black paper (control). The DNA dosimeter was then analyzed by a polymerase chain reaction (PCR) that amplifies a 500 base pair specific region of Λ DNA. Photoinduced damage in DNA blocks polymerase from synthesizing a new strand; therefore, the amount of amplified product in UV-exposed DNA was reduced from that found in control DNA. The average lesion frequency per 500 base pair per strand at 16 PCR cycles was –1.22, 1.00, 0.70 and 0.50 for 30 ng, 50 ng, 100 ng and 150 ng of dried DNA, respectively, after a total dose of 60 kj m 2 delivered with a solar UVB simulator. Although the average lesion frequency increases linearly with increasing doses for four different amounts of template DNA, the lesion frequency seems to be averaged by the amplified products from the protected Λ DNA molecules below the top few layers. The average daily dose, equivalent to the UV dose applied with the solar UVB simulator, was 10.2±0.4 kj m2 with the 50 ng containing DNA dosimeter in September 1995 in Melbourne, FL. Both 50 ng and 150 ng containing DNA dosimeters produced the same average daily dose within experimental error in January 1996, which was 5.2±0.3 kj m 2 at the same location. The dried Λ DNA dosimeter is compact, robust, safe and transportable, stable over long storage times and provides the total UVB dose integrated over the exposure time.     

Synthesis of diversely functionalized hexahydropyrrolo[2,3-b]indoles using domino reactions, olefination, isomerization and Claisen rearrangement followed by reductive cyclization

Hexahydropyrrolo[2,3-b]indoles 6 were synthesized in five steps from indolin-3-one 8 by a general and efficient method, in which elements of molecular diversity were readily added onto the 3a-position of the pyrrolo[2,3-b]indole ring system. Horner-Wadsworth-Emmons reaction of 2-allyloxyindolin-3-ones 7, derived from indolin-3-one 8 and a variety of allylic alcohols, smoothly proceeded with successive Claisen rearrangement to give the corresponding 3-allyl-3-cyanomethylindolin-2-ones 15. Indolin-2-ones 15 were converted into pyrrolo[2,3-b]indoles 6 using partial hydrolysis followed by reductive cyclization with LiAlH(4). Synthesis of N-methylated pyrrolo[2,3-b]indole derivatives 23 and 26 is also described.     

Flavonol glycosides in leaves of two Diospyros species

Fourteen flavonol glycosides including two new compounds were isolated from the leaves of two Diospyros plants (D. cathayensis and D. rhombifolia). The structures of isolated compounds were determined by spectroscopic analysis. The scavenging activity of 1,1-diphenyl-2-picrylhydrazyl (DPPH) radical of the isolated compounds was also investigated.     

Acid-catalyzed reactions of 3-(hydroxymethyl)- and 3-(1-hydroxyethyl)pyrazolo[1,5-a]pyridines

Treatment of 3-(hydroxymethyl)pyrazolo[1,5-a]pyridines with trifluoroacetic acid in refluxing dichloro-methane led to the formation of bis(pyrazolo[1,5-a]pyrid-3-yl)methanes or bis[(pyrazolo[1,5-a]pyrid-3-yl)]-methyl ethers depending upon the concentration of trifluoroacetic acid. In contrast, similar treatment of 3-(1-hydroxyethyl)pyrazolo[1,5-a]pyridines gave a mixture of 3-vinylpyrazolo[1,5-a]pyridines and 1,3-bis(pyrazolo-[1,5-a]pyrid-3-yl)-1-butenes.     

Enantioselective total synthesis of ustiloxin D

Ustiloxin D and phomopsin A are potent antimitotic agents that bind to tubulin and interfere with cellular microtubule function. A synthetic strategy has been developed to allow access to both of the natural products as well as a variety of variants of the ustiloxin and phomopsin family members in order to provide sufficient quantities for biological studies. Herein we report the enantioselective total synthesis of ustiloxin D using a longest linear sequence of 20 steps. Four of the five stereocenters were set using catalytic asymmetric methodologies. In particular, Evans's new Al-catalyzed asymmetric aldol reaction facilitated access to both syn and anti products corresponding to the different benzylic stereochemistries found in ustiloxins and phomopsins. In addition, due to its high functional group tolerance, Trost's Pd-mediated etherification was used to construct the chiral tertiary alkyl-aryl ether. Taken together, these synthetic strategies allow us to use densely functionalized intermediates to realize an efficient synthesis of ustiloxin D.     

Absolute configuration and conformation of 1,1′-spirob[benz[g]indan]

Two diastereomers of 3,3′-di-t-butyl-1,1′-spirobi[benz[g]indan] have been prepared; c.d. spectral evidence is presented for the difference between their conformations.