Synthesis and transformation of novel cyclic β-amino acid derivatives from (+)-3-carene

The regio- and stereoselective addition of chlorosulfonyl isocyanate to (+)-3-carene 1 resulted in β-lactam 2, which was converted to N-Boc-β-amino acid 4, β-amino ester 7, and carboxamide derivatives 18 and 20 via N-Boc activation and mild ring opening. The corresponding β-amino ester 7 was transformed to 2-thioxopyrimidin-4-one 11 and 2,4-pyrimidinedione 13. LAH reduction of 5 and 7 resulted in amino alcohols 6 and 8. The reaction of 8 with phenyl isothiocyanate, followed by cyclisation, furnished 1,3-oxazine 15.     

Inokosterone, an insect metamorphosing substance from Achyranthes fauriei : Absolute configuration and synthesis

Inokosterone, a phytoecdysone isolated from Achyranthes fauriei (Amaranthaceae), has been partially acetylated to give the 2,26-diacetate (4) which has been converted into methyl 5 - acetoxy - 4 - methylpentanoate (7), showing no apparent []_D, and 2β - acetoxy - 3β,14 - dihydroxy - 5β - pregn - 7 - ene - 6,20 - dione (8). Chemical and physiochemical studies have shown the configurations at C-20 and C-22 to be R. Inokosterone has thus been concluded to be a mixture of C-25 epimers of (20R,22R) - 2β,3β,14,20,22,26 - hexahydroxy - 5β - cholest - 7 - en - 6 - one (1). After the synthesis of the model compound, a C-25 epimeric mixture of (20R,22R) - 3β,20,22,26 - tetrahydroxy - 5 - cholestane (23), inokosterone has been synthesized via (20R) - 2β,3β,14,20 - tetrahydroxy - 20 - formyl - 5β - pregn - 7 - en - 6 - one (25) by Grignard reaction with 4 - (tetrahydrofuran - 2 - yloxy) - 3 - methylbutynylmagnesium bromide (15) followed by hydrogenation and hydrolysis. The use of an NMR shift reagent with the inokosterone acetates (9, 29) and the optical activity measurement of - methylglutaric acid (3) derived from inokosterone have established that inokosterone is a 1:2 mixture of the C-25 R and S epimers.     

Design,Synthesis, and Antimicrobial Evaluation of some Novel Pyridine,Coumarin, and Thiazole Derivatives

Treatment of 2‐cyano‐N′‐(1‐(pyridin‐2‐yl)ethylidene)acetohydrazide 1 with aromatic/heterocyclic aldehydes 2a–f gave arylidene derivatives 3a–f . Polysubstituted pyridine derivatives 4a,b were prepared either from reaction of arylidene 3a,b with malononitrile or from reaction of acetohydrazide 1 with arylidenemalononitrile 5a,b . Cyclocondensation of acetohydrazide 1 with salicylaldehyde derivatives and acetylacetone furnished pyrido‐coumarins 6,7 and 2‐pyridone‐3‐carbonitrile 8, respectively. In addition, pyrido‐thiazoles 13 and 15 were obtained through reaction of 2‐(1‐(pyridin‐2‐yl)ethylidene)hydrazinecarbothioamide 11 with hydrazonyl chlorides and α‐haloketones, respectively. The structures of synthesized compounds were elucidated with spectral and elemental data. The antimicrobial activity of the synthesized compounds was studied.     

Total asymmetric syntheses of 3- and 4-deoxy-hexoses and derivatives

(1S,4S)-7-Oxabicyclo[2.2.1]hept-5-en-2-one ((−)-5, a “naked sugar”) has been converted to (−)-(1R,4S,6S)-6-endo-benzyloxy-2-bromo-7-oxabicyclo[2.2.1]hept-2-ene ((−)-12) in a highly stereoselective fashion. Double hydroxylation of the C=C double bond of (−)-12, followed by acetylation and Baeyer-Villiger oxidation of the resulting -acetoxyketone (−)-14 afforded (−)-5-O-acetyl-2-O-benzyl-3-deoxy-β-D-arabino-hexofuranurono-6,1-lactone ((−)-15). This compound was converted readily into (+)-methyl 3-deoxy--D-arabino-hexofuranoside ((+)-6 and (+)-methyl 3-deoxy-β-L-xylo-hexofuranoside ((+)-7) and partially protected derivatives. (−)-15 was also converted into 4-deoxy-D-lyxo-hexopyranose (34) and several partially protected derivatives such as (+)-methyl 4-deoxy-2,3-O-isopropylidene--D-lyxo-hexopyranoside ((+)-8).     

New preparation of benzylic aluminum and zinc organometallics by direct insertion of aluminum powder

The reaction of commercial Al-powder (3 equiv) and InCl(3) (1-5 mol %) with benzylic chlorides provides various functionalized benzylic aluminum sesquichlorides under mild conditions (THF, 20 °C, 3-24 h) without homocoupling (<5%). These new benzylic organometallics reacted smoothly with various electrophiles (Pd-catalyzed cross-couplings, or Cu-mediated acylations, allylations, or 1,4-addition reactions). Electron-poor benzylic chlorides or substrates prone to Wurtz coupling can be converted to benzylic zinc compounds by the reaction of Al-powder in the presence of ZnCl(2).     

Transformations of kurchi alkaloids—I The action of nitrous acid on holarrhimine

Holarrhimine (I), 18-hydroxy-3β,20-diamino-5-pregnene, was treated with nitrous acid under different conditions. From the reaction mixtures several crystalline products were isolated and characterized as 3β-hydroxy-18-20β-oxido-5-pregnene (II), the nitrate ester of II (III), 3β-nitro-18-20β-oxido-5-pregnene (IV), 6-methoxy-18-20β-oxido-3,5-cyclopregnane (V) and 3β,18-dihydroxy-20-amino-5-pregnene (VII). On treatment with boron trifluoride and acetic anhydride compounds II, IV, V and an unidentified compound (VI) gave the same triacetate 3β,18,20-triacetoxy-5-pregnene (VIII).     

The reaction of (μ-H)2Os3(CO)9(PPh3) with ethylene affords the ethylidene complex (μ-H)2Os3(CO)9(PPh3)(μ-CHCH3)

The product isolated from the reaction of (μ-H)₂Os₃(CO)₉(PPh₃) with ethylene is shown to be the ethylidene complex (μ-H)₂Os₃(CO)₉(PPh₃)(μ-CHCH₃) (1) rather than the ethylene complex (μ-H)(H)Os₃(CO)₉(PPh₃)(C₂H₄), as previously claimed. The characterization of 1 is based on a combination of ¹H and ¹³C NMR results. The ¹H NMR data (δ 6.84 (1 H_D), 2.53 (3 H_C), J(CD) = 7.4 Hz) establish the presence of the ethylidene moiety, whereas detailed analysis of the 1-D and 2-D ¹³C NMR spectra of ¹³CO-enriched 1 indicates the relative positions of the ethylidene, hydride, and phosphine ligands on the triosmium framework.     

脱卤亚磺化研究——连二亚硫酸钠作为新的脱卤亚磺化试剂

全氟碘代烷与亚硫酸盐发生单电子转移反应生成全氟亚磺酸盐;连二亚硫酸钠水溶液热分解时,ESR表明生成SO_2~-主阴离子自由基,这两者促使我们尝试用连二亚硫酸钠代替亚硫酸盐与全氟卤代烷反应.实验表明对于全氟碘代烷及溴代烷它是一种有效的     

Syntheses of (5E)-PGE2 and New 6-Functionalized Derivatives by the Use of Palladium-Catalyzed Decarboxylative Allylic Alkylation

(5 )-Prostaglandin E₂ (7) was synthesized fron ( )-4- -butyldimethylsilyloxy-2-cyclopentenone (1) by 2-alkenyloxycarbonylatlon of the organocopper conjugate-addition adduct (3) followed by intramolecular palladium-catalyzed decarboxylative allylic alkylation. The (5 )-prostaglandin E₂ skeleton was also obtained from the β-keto allylic ester (11) by a similar decarboxylative allylic alkylation. The decarboxylative allylic alkylation of another type of the three-component coupling product (12) gave new 6-methyleneprostaglandin E1 skeleton (15a), which was converted into new 6-methylprosta-glandin I methyl ester (20) 6-methyleneprostaglandin F₁ derivative (16) by two different ways. The stereochemistry of this intramolecular decarboxylative allylic alkylation was discussed in the reaction of 2-[( )- or ( )-2-butenyloxy-carbonyl] cyclopentanone systems.     

Asymmetric 1,3-dipolar cycloaddition of chiral sulphinylethenes with 1-methyl-3-oxido-pyridinium and some nitrones

1,3-Dipolar cycloaddition of (R)-(+)-p-tolyl vinyl sulphoxide 1 with 1-methyl-3-oxidopyridinium 6 proceeded in a diastereoselective manner to afford the exo and endo cycloadducts 11a,b and 12a in 36%, 7% and 29% yield, respectively. The absolute configuration of 11a was determined by its transformation to (1S)-(−)-2-tropanol (−)-15. Attempts to the cycloaddition of the sulphinylethenes 17–19 with the pyridinium 6 were nsuccessful under several conditions. The reaction of the sulphoxide 20 with pyrroline 1-oxide 21 gave an inseparable mixture of products. The cycloaddition of 20 with 3,4,5,6-tetrahydropyridine 1-oxide22 afforded a mixture of four adducts in ca. 90% yield. High level of diastereoselectivity was achieved for the endo cycloaddition affording the adduct 23 in 33% isolated yield. The absolute configuration of 23 was confirmed by a single-crystal X-ray diffraction study. The stereochemical course of the reaction was discussed based on the absolute configuration of the products.     

Unusual Knoevenagel condensations of 16a-substituted-16-methylene-17-keto-steroids

A Knoevenagel condensation between 3β-acetoxy-16-pyrrolidinylmethylenandrost-5-en-17-one (8c) and an excess of malononitrile led unexpectedly to 3β-acetoxyandrost-5-eno-[17,16-c]-1′,6′-dicyanoaniline (12a) as the major product and 3β-acetoxy-16-pyrrolidinylmethylen-17-dicyanomethylenandrost-5-ene (11a) as the minor product. Knoevenagel reactions of other 16a-substituted-16-methylen-17-keto steroids were studied to evaluate the scope and mechanism of the reaction.     

Synthesis of tetramethyldisilane-bridged bis(1-indenyl) tetracarbonyl di-iron: A novel thermal rearrangement reaction between the Si-Si and Fe-Fe bonds

The title complex (Me₂SiSiMe₂)(η⁵-l-indenyl)Fe(CO)]₂(μ-CO)₂ (1) was prepared by the reaction of 1,2-bis(1-indenyl)tetramethyl-disilane and Fe(CO)₅ in refluxing heptane. Its thermal rearrangement product [Me₂Si(η⁵-1-indenyl)Fe(CO)₂]₂ (2) was also obtained from the reaction. 1 in refluxing xylene can be readily converted into 2. The crystal structures of the cis isomer 1c and the trans isomer 2t were determined by X-ray diffraction.     

Unusual sulfated marine steroids from the ophiuroid ophioderma longicaudum

Polar extracts of the ophiuroid Ophioderma longicaudun contain unusual sterol sulfates together with a mixture of common 3β-hydroxysterol sulfates. The more polar compound has been shown to be 5β-cholestane-3, 4,11β,12β,21-pentol 3,21-disulfate 1. A second group of unusual compounds are disulfated 3,21-dihydroxysteroids. After solvolysis to remove the sulfate groups they have been identified as : (20R)-5-cholestane-3, 21-diol 4a, (20R)-cholest-5-ene-3,21-diol 5a, (20R22E)-cholest-5,22-diene-3,21-diol 6a and (20R)-24-methylcholest-5,24(28)-diene-3,21-diol 7a. Analysis of the “non-sulfated” sterol fractions has shown the presence of common 3β-hydroxy sterols.     

Research on steroids. 41. Conversion products of 17-alpha-strophanthidins

Pseudostrophanthidin ( 2 ) can be easily prepared by treating strophanthidin ( 1 ) with concentrated hydrochloric acid in the cold [1]. 2 has served as the initial product for the preparation of a number of analogues and homologues of steroid hormones [2] [3]. 17α-Pseudostrophanthidin ( 4 ) is considered a suitable starting material for an extension of these investigations. It was logical to attempt the preparation of 4 from 17α-strophanthidin ( 3 ) under conditions identical with those used in the conversion of 1 into 2. However, these experiments did not lead to 4 but, instead, by way of the unstable 14ξ-chloro-14-deoxy-17α-strophanthidin ( 5 ) to 14-anhydro-17α-strophanthidin ( 6 ). This result is essentially in agreement with findings reported in the literature [5]. To support the structure assigned to 6 , this compound was also prepared by a different, unambiguous, route. Treatment of 3 with thionyl chloride in pyridine gave mainly 3β, 5β-O, Osulfinyl-14-anhydro-17α-strophanthidin ( 8 ), which was converted into 6 by mild hydrolysis. In turn 6 , as obtained via the unstable chloro compound 5 , gave on treatment with thionyl chloride in pyridine a product identical with 8. – 6 was characterized as the 3-acetate 7 . As extension of these experiments, 17α-strophanthidol ( 10 ) [6] was treated with concentrated hydrochloric acid in the cold under conditions similar to those used in the conversion of 3 into 6 by way of 5. This led to the isolation of 14-anhydro-17α-strophanthidol ( 11 ), which could also be obtained by the reduction of 6 with aluminium amalgam. As is known [1] [8], strophanthidinic acid ( 13 ) can be converted into strophanthidinic acid 19,8-lactone ( 14 ) by treatment with concentrated hydrochloric acid in the cold. In view of the negative results obtained in the attempt to transform 3 into 4 under these conditions, the question arose as to whether the conversion of 17α-strophanthidinic acid ( 15 ) into 17α-strophanthidinic acid 19,8-lactone ( 16 ) by the same procedure is also impossible. 15 was prepared by treating 3 with hydrogen peroxide and was characterized as the methyl ester 17 and the methyl ester of the 3-benzoate ( 18 ). 15 and 17 have been mentioned in the literature [5], but the physical constants reported differ from those obtained in this laboratory. It was demonstrated that after treating 15 with concentrated hydrochloric acid in the cold, no 16 could be isolated but, instead, an unstable chloro compound 19 which was converted into 14-anhydro-17α-strophanthidinic acid ( 20 ). 20 was characterized as the methyl ester 21 and the 3-acetate 22 .     

Synthesis of the β-lactam antibiotic (+)- thienamycin via an intermediate π-allyltricarbonyliron lactone complex

The π-allyltricarbonyliron lactone complex (7), formed by reaction of E-1,2-epoxy-2-methyl-6,6-dimethoxyhex-3-ene(5) with co-ordinatively unsaturated iron carbonyl species, was reacted with benzylamine to give a lactam complex (8) by an S_N'-like mechanism. This complex upon oxidation with Ce(IV) afforded cis-3-isopropenyl-4-[(2',2'-dim (9) which was chemically modified into trans-3-(1'-hydroxyethyl)-4-[(2',2-dimethoxy)ethyl] azetidin-2-one (13), a key intermediate previously used in the synthesis of the antibiotic thienamycin. Similar reaction with (S)-(-)--methylbenzylamine afforded a separable mixture of diastereoisomeric iron lactam complexes (16 and 17). These complexes could be individually converted to the corresponding optically active β-lactam derivatives (27 and 28) and, hence, are precursors for the synthesis of either natural (+)-thienamycin or unnatural (-)-thienamycin.     

Synthesis of Newly Substituted Pyrazoles and Substituted Pyrazolo[3,4‐b]Pyridines Based on 5‐Amino‐3‐Methyl‐1‐Phenylpyrazole

The reaction of the aminopyrazole 1 with benzenesulfonyl chloride, arenediazonium salt, chloroacetyl chloride, ethoxy methyleneamlononitrile and with ethyl 2‐cyano‐3‐ethoxyacrylate gave the substituted 3‐methyl‐1‐phenylpyrazole 2–5a,b . Compound 5b was cyclized to 6 and to 7 by treating it with AlCl₃ and with POCl₃, respectively. Compound 6 converted to 7 by boiling it in POCl₃/PCl₅. Compound 10b was produced through reaction of 9 with acetophenone. Reaction of 1 with benzylidinemalononitrile afforded 11 . New methods for preparation of 15 and 16 are described. The reaction of 8 with malononitrile, thiosemicarbazide, phenyl hydrazine and acetophenone afforded compounds 18–21 . The reaction of 21 with malononitrile gave 22 . Compounds 23–26 were produced upon reaction of 10a with malononitrile, phenyl hydrazine, thiosemicarbazide, semicarbazide and with benzaldehyde, respectively.     

Chemical conversion of corticosteroids to 3 alpha,5 alpha-tetrahydro derivatives. Synthesis of allotetrahydrocortisol glucuronides and allotetrahydrocortisone glucuronides

The synthesis of the 3- and 21-glucuronides of allotetrahydrocortisol (allo-THF) and allotetrahydrocortisone (allo-THE) is described. 5 alpha-Dihydrocortisol (5) was prepared by selective hydrogenation of 21-acetoxy-3, 11 beta, 17 alpha-trihydroxy-3,5-pregnadien-20-one 3-ethyl ether (3), followed by acid hydrolysis and saponification. When 5 alpha-dihydrocortisol 21-tetrahydropyranyl ether (6) was treated with potassium tri-sec-butylborohydride in tetrahydrofuran under mild conditions, regioselective and stereoselective reduction at C-3 took place to give allo-THF 21-tetrahydropyranyl either (7). This compound was converted into the 3- and 21-monoacetates of allo-THF and allo-THE, key intermediates. Introduction of the glucuronyl residue at C-3 or C-21 was carried out by means of the Koenigs-Knorr reaction. Prior to saponification yielding the 3-glucuronides (20,23), the alkali-sensitive ketol side chain at C-17 was protected as 20-semicarbazones.     

Altered selectivity of reduction of steroidal carbonyls

The reduction of steroidal ketones in different solvents yielded different products. These conditions which altered the normal path, yielded a selective reduction of the Δ⁴-3 carbonyl without the concomitant reduction of the C-17 or C-20 ketones; this permitted a one step partial synthesis of 3β-hydroxy-Δ⁴-pregnen-20-one (I), 3β-hydroxy-5-pregnan-20-one (II), and of 3β,11β-dihydroxyandrostan-17-one (IV).     

Uses of cyclohexan-1,3-dione for the synthesis of tetrahydrochromeno[3,4-c]chromen derivatives with anti-tumor activities

Cyclohexan-1,3-dione ( 1 ) was used as the key starting material, which reacted with salicylaldehyde ( 2 ) and either malononitrile ( 3a ) or ethyl cyanoacetate ( 3b ) in ethanol containing a catalytic amount of triethylamine to give the 3,4,7,12b-tetrahydrochromeno[3,4-c]chromen-1-one derivatives 5a , b . The latter compounds underwent Gewald's thiophene synthesis through the reaction with either malononitrile or ethyl cyanoacetate to give compounds 6a-d , respectively. On the other hand, compound 5a was used for the synthesis of annulated chromeno[3,4-c]chromen derivatives through its reaction with different chemical reagents. The synthesized compounds were evaluated against the six cancer cell lines A549, HT-29, MKN-45, U87MG, SMMC-7721, and H460 using the standard MTT assay in vitro, with foretinib as the positive control, many compounds expressed high inhibitions. The most active compounds 5b , 6b , 6d , 7 , 9b , 11a , 11b , 13 , 17 , 18b , 20b , 21b , 21e , and 21f were selected for inhibition of five tyrosine kinases and some selected compounds for Pim-1 kinase inhibition. The results showed that compounds 6b , 6d , 11a , 13 , 17 , 20b , and 21e were the most potent compounds with the tyrosine kinases and compounds 6d , 11a , 20b , and 21e were the most potent inhibitors of Pim-1 kinase.     

Untersuchungen zur synthese des schwefelisosteren psilocins und einiger 4-hydroxybenzo(b)thiophenderivate

The synthesis of thiapsilocin 13 and/or 13a from 2-hydroxy-acetophenone (1) via 2–12 and the spectroscopic properties of these new compounds have been recorded; the other research about the benzo(b)thiophenederivatives 14, 16 follow, the molecules 15a, 15b, 17, 18, 19, 20, 21 have been synthesized.