Stekeospecific transformation of D-sugar to L-sugar in complex aminoglycoside. Synthesis of a kanamycin B analog having 2,6-diamino-2,4,6-trideoxy-L-arabino-hexopyranose

A 4′-ene derivative of kanamycin B ($\text{4}$) was derived from the epoxide ($\text{1}$) by oxidative elimination of the 4′-phenylseleno group into the allylic alcohol ($\text{3}$). The title compound, 0-(2,6-diamino-2,4,6-trideoxy-β-L-arabino-hexopyranosyl)-(1→4)-0-[3-amino-3-deoxy-α-D-glucopyranosyl-(1→6)]-2-deoxystreptamine ($\text{6}$) was obtained from $\text{4}$ by stereospecific hydrogenation followed by removal of the masking groups, changing the D-sugar moiety of the 4-0-glycoside portion into an L-sugar.     

A 1,2-phenyl shift to the double bond of a vinyl cation

Reaction of HCl with 3-phenylpropyne ($\text{1}$) afforded 1,2-dichloro-2- phenylpropane($\text{6}$) among other products. The reaction proceeds by a 1,2-phenyl shift to the 5-phenyl-1-propene-2-yl cation ($\text{2}$).     

A short and efficient synthesis of 4-hydroxy-5-(1-hydroxyalkyl)-γ-butyrolactones

The cycloaddition of α,β-epoxyaldehydes or ketones ($\text{2}$) with the ketene acetal MeHC=C(OMe)₂ ($\text{1}$) gives epoxyoxetanes ($\text{3}$) in high yields. Without isolation they can be transformed into 4-hydroxy-5-(1-hydroxyalkyl)-γ-butyrolactones ($\text{6}$) via the epoxy esters $\text{4}$ and trihydroxy esters ($\text{5}$). The lactones $\text{6}$ appear to be valuable precursors for the synthesis of 5-(1-hydroxyalkyl)-3-methyl-2-5H-furanones ($\text{7}$) and 3-methyl-5-ylidene-2-5H-furanones ($\text{8}$)     

Chiral synthesis of (2s,3s,7s)-3,7-dimethylpentadecan-2-yl acetate and propionate,potential sex pheromone components of the pine saw-fly neodiprion sertifer (geoff.)

A synthesis of (2S,3S,7S)-3,7-dimethylpentadecan-2-yl acetate ($\text{2}$) and propionate ($\text{3}$) is described. (2S)-2-Methyldecan-1-yl lithium ($\text{5}$) was reacted with (3S,4S)-3,4-dimethyl-γ-butyrolactone ($\text{6}$) to yield the ketoalcohol $\text{19}$ which upon Huang-Minlon reduction furnished (2S,3S,7S)-3,7-dimethylpentadecan-2-ol ($\text{1}$). Acylations gave the esters $\text{2}$ and $\text{3}$. The (2S)-2-methyldecan-1-yl lithium was obtained via asymmetric synthesis. The chiral lactone $\text{6}$ was obtained from (2S,3S)-trans-2,3-epoxybutane and dimethyl malonate.     

The synthesis of γ-fluoroisoleucine

Condensation of 3-fluoro-2-butanone ($\text{2}$) with alkyl diethylphosphonoacetates ($\text{4a–d}$) gave alkyl 4-fluoro-3-methyl-2-pentenoates ($\text{5a–d}$). Addition of bromine yielded alkyl-2,3-dibromo-4-fluoro-3-methylpentanoates ($\text{6a,b}$) which were dehydrobrominated to alkyl 2-bromo-4-fluoro-3-methyl-2- pentenoates ($\text{7a,b}$). Since these compounds could not be hydrogenated to the desired alkyl 2-bromo-4-fluoro-3-methylpentanoates ($\text{8a,b}$), another route was taken. The esters $\text{5a–d}$ were hydrogenated to alkyl 4-fluoro-3- methylpentanoates ($\text{11a–c}$) which were converted to their carbanions. Treatment with bromine gave esters $\text{8a–c}$, and iodine gave alkyl 4-fluoro-2-iodo- 3-methylpentanoates ($\text{12a,b}$). Esters $\text{8a–c}$ and $\text{12a,b}$ were converted to alkyl 2-azido-4-fluoro-3-methylpentanoates ($\text{13a–c}$) whose hydrogenation gave alkyl 2-amino-4-fluoro-3-methylpentanoates ($\text{14a–c}$). Hydrolysis afforded γ-fluoroisoleucine ($\text{1}$).     

Oxygenation of 4-(N-alkylimino)methyl-2,6-di-t-butylphenols mediated by Co(II)-Schiff base complex

4-(N-Alkylimino)methyl-2,6-di-$\text{t}$-butylphenols ($\text{1}$), Schiff bases of 3,5-di-$\text{t}$-butyl-4-hydroxybenzaldehyde can be oxygenated in the presence of Co(Salpr), a five coordinate Co(II)-Schiff base complex to give N-alkyl-3-$\text{t}$-butyl-5-formyl-2-hydroxy-2-pivaloyl-1,2-dihydropyridines ($\text{2}$ as the main product together with 3-formyl-2,5-di-$\text{t}$-butyl-2,4-cyclopentadienone ($\text{3}$) and 2,6-di-$\text{t}$-butyl-4-formyl-6-hydroxy-4,5-epoxy-2-cyclohexenone ($\text{4}$). These products result from dioxygen incorporation into the ortho position of $\text{1}$.     

Reactions of sulfoxonium allylides with nitrile oxides and ring transformations of their reaction products

Reactions of allylides ($\text{1}$) with nitrile oxides ($\text{2}$) afforded furanylglyoxylate oxime ($\text{3}$) and 6H-l,2-oxazine ($\text{4}$). Ring transformations of $\text{3}$ and $\text{4}$ gave $\text{4}$ and pyrrolinone ($\text{6}$), respectively.     

Cycloaddition of single oxygen and triazolinedione (TAD) with spirocyclopentadienyl-1,3,5-cycloheptatrienes1: tropilidene versus norcaradiene reactivity

4-Methyl-1,2,4-triazoline-3,5-dione (MTAD) gives with 7-spiro-fluorenyl-1,3,5-cycloheptatriene ($\text{1d}$) initially he norcaradine-type urazole ($\text{N3d}$) which at ambient temperatures rearranges into ($\text{6d}$), while ¹0₂ gives the tropilidene-type endoperoxide ($\text{T4d}$).     

Adenosine cyclic 3′,5′-(RP)- and (SP)-phosphoramidates,the first representatives of nucleoside cyclic 3′,5′-phosphoramidates derived from ammonia

Adenosine cyclic 3′,5′-phosphoramidate $\text{2}$ was synthesized by reacting adenosine cyclic 3′,5′-phosphate $\text{1}$ with POCl₃, in trimethyl phosphate for 1 h at O°C, followed by in situ treatment of the reaction mixture with a suspension of (NH₄)₂CO₃ in anhydrous DMF or pyridine or DMF/pyridine mixture for 30 min at 25° C. Diastereoisomers ($\text{R}$_P)-$\text{2}$ and ($\text{S}$_P)-$\text{2}$ the relative quantities of which depended on the solvent of (NH₄)₂CO₃ treatment, were separated by reversed phase partition chromatography. Hydrolysis of (R_P)-$\text{2}$ and (S_P)-$\text{2}$ proceeded with predominant (90% in 0.1 N HCl, 100% in 0.1 N NaOH) -P-O-C bond breaking.     

The total synthesis of i-oxygenated eudesmanolides

A route towards I-oxygenated eudesmanolides, via a (2+2) photocycloaddition reaction for constructing the decalin framework is described. The following natural substances have been synthesized. (=)-dihydroreynosin ($\text{1}$), (±)-1- oxo-dihydronmagnolialide ($\text{2}$), (±)-maritimin ($\text{3}$), (±)-dihydromagnolialide ($\text{4}$), (±)-magnolialide ($\text{5}$), (±)-dihydrosantamarine ($\text{6}$). Also a synthesis of (±)--santonin ($\text{7}$) is presented.     

4,6-Thioanhydro-hexopyranosides,synthesis and chemical behaviour of methyl 2-0-p-toluenesulfonyl-4,6-thioanhydro-α-d-gulopyranoside

Methyl 4-0-benzoyl-6-bromo-6-deoxy-α-D-glucopyranoside ($\text{1}$, Figure 1) was converted, via the corresponding ditosylate $\text{2}$, into methyl 2,3-di-0-p-toluenesulfonyl-4-0-benzoyl-6-S-acetyl-6-thio-α-D-glucopyranoside ($\text{3}$) by a selective nucleophilic displacement of 6-bromo-group with thioacetate. Unexpectedly, on treating the compound $\text{3}$ with an excess of sodium methoxide in benzene-methanol (1:1) at room temperature, methyl 2-0-p-toluenesulfonyl-4,6-thioanhydro-α-D-gulopyranoside ($\text{4}$) was obtained in a yield of 84%. In order to determine the structure of the relatively unstable oily product $\text{4}$, some stable crystalline derivatives ($\text{5}$, $\text{6}$ and $\text{7}$) were prepared. Detailed analysis of the ¹H-NMR-spectra (200 MHz) of $\text{6}$ and $\text{7}$ gave the conclusive evidence for the structure of $\text{4}$ A self-imposing mechanism of the clean and smooth transformation of $\text{3}$ to $\text{4}$ is proposed, involving: a) formation of $\text{9}$ (Figure 2) as a crucial intermediate and b) a highly regioselective epoxide opening in $\text{9}$ (at C-4) by an intramolecular nucleophilic attack of the mercaptide anion from C-6.     

Trimethymetall-urotropinaddukte des aluminiums,galliums, indiums und thalliums

Reactions of urotropine (C₆H₁₂N₄) with trimethylmetal derivatives of Al, Ga, In und Tl in various ($\text{1}\text{1}$$\text{1}\text{4}$) molar ratios lead to stable and monomeric $\text{1}\text{1}$, $\text{1}\text{2}$ or $\text{1}\text{3}$ adducts in good yields, but no $\text{1}\text{4}$ addition product could be isolated. The vibrational spectra (IR and Raman) of all compounds are recorded and partly assigned. Some characteristic frequencies of the C₆N₄-skeletons clearly show the symmetry changes in the series of the $\text{1}\text{1}$ → $\text{1}\text{2}$ → $\text{1}\text{3}$ adducts (C_3ν → C_2ν → C_3ν). The X-ray structure determinations of C₆H₁₂N₄·.GaMe₃ (MeCH₃) and C₆H₁₂N₄·.2GaMe₃, are in good agreement with the vibrational spectra. Both compounds crystallize in monoclinic space groups (P2₁ and C2/c). The GaN distances are around 214 pm, and the values for the C₆N₄-skeletons are not significantly different from those for free urotropine.     

Formal total synthesis of β-pipitzol

(±)-$\text{O}$-methylperezone ($\text{1b}$) was obtained by selective oxidative demethylation of (±)-leucoperezone trimethyl ether ($\text{4a}$). Compound ($\text{4a}$) was prepared by condensation of 2,3,5-trimethoxytoluene ($\text{5e}$) with 6-methyl-5-hepten-2-one, followed by reductive removal of the tertiary alcohol. The aromatic precursor $\text{5e}$ was prepared in four steps from 2,3-dimethoxytoluene ($\text{5a}$) and, alternatively, in three steps from 5-bromoveratraldehyde ($\text{6a}$). Racemic $\text{1b}$ and $\text{4a}$ were directly compared with the optically active molecules prepared from natural R(-)-perezone ($\text{1a}$).     

N-halogeno-compounds. Part 9 [1]. Azoxy- and azo-arenes derived from 4-(dichloroamino)tetrafluoropyridine; crystal structure of trans-2,3,5,6-tetrafluoro-4-(2,4,6-trimethylphenyl-onn-azoxy)pyridine

The nitrosoarenes ArNO (Ar = C₆H₅, 2-MeC₆H₄, 2,4,6- Me₃C₆H₂ and C₆F₅) have been condensed with 4-(dichloroamino)- tetrafluoropyridine to provide the azoxy-compounds py_FN$\text{N}\text{+}$($\text{N}\text{-}$)Ar (py_F = 2,3,5,6-tetrafluoro-4-pyridyl); de-oxygenation of the first three with triphenylphosphine or triethyl phosphite gave the corresponding azo-compounds, and the reverse reaction was achieved in the case of py_FNNC₆H₂Me₃-2,4,6 using peroxytrifluoroacetic acid. Thermolysis of 4-azidotetrafluoropyridine in the presence of pentafluoronitrosobenzene provided the perfluorinated azoxy-compound py_FN$\text{N}\text{+}$($\text{O}\text{-}$)C₆F₅. X-Ray methods have been used to determine the molecular geometry of py_FN$\text{N}\text{+}$($\text{O}\text{-}$)C₆H₂Me₃-2,4,6.     

Stereoselektive synthese von α-glucosiden mit 1,1′ -diacetal-struktur

Reaction of ($\text{1b}$) and ($\text{1d}$) with the acetal ($\text{2a}$) in presence of trimethylsilyl trifluoromethanesulfonate at ?70° C gives the α-glucosides ($\text{3a}$) and ($\text{4a}$), whereas ($\text{1a}$) and ($\text{1c}$) lead to the β-glucosides ($\text{4c}$) and ($\text{4b}$). At 0° C reaction of ($\text{1a}$) with the acetals ($\text{2b-g}$) gives exclusively the α-glucosides ($\text{3b-g}$).     

A variable temperature study of the 19-F N.M.R. spectrum of perfluorohexamethyltetrazan: Novel restricted rotation and hindered inversion at the nitrogen atoms [1]

At low temperatures, the ¹⁹F n.m.r. spectrum of the tetrazan (CF₃)₂NN(CF₃)N(CF₃)N(CF₃)₂ shows the presence of two isomers with a free energy difference in stability Δ$\text{G}$ of 2.2 kJ mol^-1. Both isomers show three types of CF₃ group which coalesce at -15°C to three systems of equal intensity (Δ$\text{G}$≠ 52 kJ mol^-1). At 40 °C the two signals assigned to the terminal CF₃ groups coalesce to a single band (Δ$\text{G}$≠ 65 kJ mol^-1).The behaviour is discussed in terms of restricted inversion at the nitrogen atoms, and hindered rotation about the N-N bonds.The hydrazines (CF₃)₂NN(CF₃)NO and (CF₃)₂NN(CF₃)NO₂ have temperature independent spectra.     

Mercury in organic chemistry. 19. Rhodium promoted methylation of organomercurials

Alkenyl-, alkynyl- and arylmercurials are methylated in excellent yield upon treatment with stoichiometric amounts of CH₃RhI₂(PPh₃)₂ ($\text{1}$). Catalytic methylation of these organomercurials is possible using $\text{1}$ and methyl iodide, but side reactions interfere.     

Sym-benzvaleno-benzo-benzvalene,a double valence isomer of anthracene

Dilithio-s-indacene ($\text{1}$) on reaction with excess chlorocarbene produces s-benzvaleno-benzo-benzvalene ($\text{3}$). Unlike benzvalene, it does not aromatize on heating but decomposes stepwise to 1,5- and 1,7-bis-methylene-dihydro-indacene ($\text{6}$ and $\text{7}$).     

Synthese de l'acide β fluoroacrylique (fluoro-3 propenoique)

Regioselective Bayer-Villiger oxidation of 2-chloro-2-fluoroethyl-isopropyl ketone ($\text{1}$) gives isopropyl-3-chloro-3 fluoropropionate ($\text{2}$). The dehalogenation of ester ($\text{2}$) with trimethylamine gives isopropyl-3-fluoropropenoate ($\text{3}$). Ester cleavage by trimethylsilyl iodide, in the presence of cyclohexene oxide, gives $\text{trans}$-3-fluoropropenoic acid ($\text{4}$).