Intramolecular photoreactions of 6-(ω-alkenyl)-4-methoxy-2-pyrones

6-(ω-Alkenyl)-2-pyrones 3a-c and 8a, b were prepared and the photochemical reactions were investigated. Photosensitized reactions of 3b, c gave intramolecular [2+2]-cycloadducts 11b, c as tricyclic lactones, site-and regio-specifically. They are not frontier-orbital-controlled adducts. On the other hand, 3a, 8a, b afforded cyclobutenecarboxylic acids, 10a, 14a, b , respectively. The end-ester group at the side-chain is thought not to be effective for the intramolecular phptoaddition.     

Intramolecular photoreactions of 4-(ω-alkenyloxy)-6-methyl-2-pyrones

Photoirradiations of 4-(ω-alkenyloxy)-2-pyrones 1 gave site- and regio-specific intramolecular [2 + 2]-cycloadducts 2 being oxatricyclic lactones, and/or Dewar-type valence-isomer derivatives 4. The reaction path depended upon the alkenyl chain length. Namely the two or three carbon chain gave rise to intramolecular [2 + 2]-cycloaddition, while the four carbon chain caused both valence-isomerization and cycloaddition. Hydrolysis of the cycloadducts 2 gave oxabicycloalkanecarboxylic acids 7.     

Nucleotides. Part XXXV. Synthesis of 3′-deoxyadenylyl-(2′–5′)-3′-deoxyadenyIyl-(2′–ω)-9-(ω-hydroxyalkyl)adenines

Via the phosphotriester approach, new structural analogs of (2′–5′)oligoadenyiates, namely 3′-deoxyadenylyl-(2′–5′)-3′-dcoxyadenylyl-(2′–ω)-9-(ω-hydroxyalkyl)adenines 18 – 21 , have been synthesized (see Scheme) which should preserve biological activity and show higher stability towards phosphodiesterases. The newly synthesized oligonucleotides 18 – 21 have been characterized by ¹H-NMR spectra, TLC, and HPLC analysis.     

Synthesis and Biological Activity of ω-(5-Aryl-1,3,4-oxadiazol-2-thio)- and ω-(5-Aryl-1,3,4-oxadiazol-2-thioacetoxyl)-ω-(1-H-1,2,4-triazol-1-yl)acetophenones

Eighteen novel ω-(5-Aryl-1,3.4-oxadiazol-2-thio)-ω-(1-H-1,2,4-triazol-1-yl)acetophenones ( 4a-4i ) and ω-(5-Aryl-1,3,4-oxadiazol-2-thioacetoxyl)-ω-(1-H-1,2,4-triazol-1-yl)acetophenones ( 5a-5i ) were synthesized. All the compounds synthesized were confirmed by elemental analyses and spectral data. The biological activity of representative compounds was evaluated.     

Synthese von ω-(5-Oxo-1-cyclopentenyl)alkansäure-methylestern aus 2-Nitrocycloalkanonen

Synthesis of Methyl ω-(5-Oxo-1-cyclopentenyl)alkanoates Starting from 2-Nitrocycloalkanones A convenient synthesis of methyl ω-(5-oxo-1-cyclopentenyl)alkanoates 1 is described. 2-Nitrocycloalkanones 2 are converted to 2-(3,3-dimethoxypropy1)-2-nitrocycloalkanones 4 . Treatment of 4 with MeOH/MeONa led to the ring-opened nitronates 5 which underwent a Nef reaction to form the corresponding oxo derivatives 6 . Partial hydrolysis of followed by base-catalyzed aldol reaction gave the desired products in high yields.     

2-Amino-4-aryl-6-(ω-carboxyalkyl)-5H-pyrrolo[3,4-d]pyrimidin-7-(6H)ones. Preparation via a one-pot synthesis of 1-(ω-carboxyalkyl)-4-carbethoxy-2,3-dioxopyrrolidines

1-(ω-Carboxyalkyl)-4-carboethoxy-2,3-dioxopyrrolidines were prepared by a one-pot synthesis from β-alanine or γ-aminobutyric acid, ethyl acrylate and diethyl oxalate. In a second one-pot process these products were hydrolyzed, decarboxylated and condensed with aromatic aldehydes under the influence of hydrochloric acid to yield 1-(ω-carboxyalkyl)-4-arylidene-2,3-dioxo-pyrolidines, which yielded 2-amino-4-aryl-6-(ω-carboxyalkyl)-5H-pyrrolo[3,4-d]pyrimidin-7-(6H)-ones upon treatment with guanidine. It was shown that 3,4-dihydro derivatives of certain 2-amino-4-aryl-5H-pyrrolo[3,4-d]pyrimidin-7-(6H)ones, formed initially in the guanidine reaction, readily undergo conversion to 5H-pyrrolo[3,4-d]pyrimidin-7-(6H)ones.     

Liquid-crystalline behaviour of 4-(ω-aminoalkyloxy)-4'-cyanobiphenyls and their side chain epoxy polymers

Liquid-crystalline side chain polymers were obtained from the ring-opening reaction of epoxy resin with mesogenic amines, 4-(ω-aminoalkyloxy)-4'-cyanobiphenyl. The amines with the alkyl group ranging from five to nine methylene units were synthesized, and were found to exhibit an enantiotropic nematic phase. Polymerization of these amines with ethylene glycol diglycidyl ether at 100°C yielded the polymers of low glass transition and melting temperatures. The mesomorphic properties of the amines and the resulting epoxy polymers are reported.     

Some fatty acids having an O-heterocycle in their terminal positions. II. ω-(3-Coumarinyl)alkanoic acids and ω-(2-chromonyl)alkanoic acids

Some ω-3-coumarinyl)alkanoic acids 1a , n = 3-6 were synthesized by cyclization of corresponding ethyl o-formylphenyl alkanedioate 3 with DBU followed by hydrolysis. By a similar cyclization, some ω-(2-chromonyl)alkanoic acids 2a , n = 3-6 were also obtained from the cyclization of corresponding o-acetylphenyl ethyl alkanedioate 4 .     

Nucleotides Part LI. Synthesis and biological activities of (2′-5′)adenylate trimer conjugates with 2′-terminal 3′-O(ω-hydroxyalkyl) and 3′-O-(ω-carboxyalkyl) spacers

An efficient strategy for the synthesis of (2′-5′)adenylate trimer conjugates with 2′-terminal 3′-O-(ω-hydroxyalkyl) and 3′-O-(ω-carboxyalkyl) spacers is reported. Npeoc-protected adenosine building blocks 37--40 for phosphoramidite chemistry carrying a 3′-O-[11-(levulinoyloxy)undecyl], 3′-O-{2-[2-(levulinoyloxy)ethoxy]ethyl}, 3′-O-[5-(2-cyanoethoxycarbonyl)pentyl], and 3′-O-{5-[(9H-fluoren-9-ylmethoxy)carbonyl]pentyl} moiety, respectively, were prepared (npeoc = 2-(4-nitrophenyl)ethoxycarbonyl). Condensation with the cordycepin (3′-deoxyadenosine) dimer 1 led to the corresponding trimers 42, 43, 47 , and 48. Whereas the levulinoyl (lev) and 9H-fluoren-9-ylmethyl (fm) blocking groups could be cleaved off selectively from the trimers 42, 43 , and 48 yielding the intermediates 44, 45 , and 49 for the synthesis of the 3′-O-(ω-hydroxyalkyl)trimers 53, 54 and the cholesterol conjugates 59--61 , the 2-cyanoethyl (ce) protecting group of 47 , however, could not be removed in a similar manner from the carboxy function. Trimer 47 served as precursor for the preparation of the trimer 55 with a terminal 3′-O-(5-carboxypentyl)adenosine moiety. The metabolically stable 3′-O-alkyl-(2′--5′)A derivatives were tested regarding inhibition of HIV-1 syncytia formation and HIV-1 RT activity. Only the conjugate 59 showed significant effects, whereas the trimers 53--55 and the conjugates 60 and 61 were less potent inhibitors, even at 100-fold larger concentrations.     

Kinetics and steric limitation of quaternization of poly(4-vinylpyridine) with mesogenic ω-(4′-methoxy-4-biphenylyloxy)alkyl bromides

The kinetics and characteristics of the quaternization of poly(4-vinylpyridine) with very large alkylating agents are studied with the main aim to demonstrate the occurrence of a limitation of the reaction due to steric effect. Kinetics are carried out in sulfolane at different temperatures with two ω-(4'-methoxy-4-biphenylyloxy)alkyl bromides. An important limitation of the reaction is demonstrated: 30% of the pyridine groups are inaccessible at 333 K, 23% at 355.5 K, and 4% at 363 K. Post-quaternization experiments with butyl bromide of already partially quaternized P4VP also demonstrate this limitation. The occurrence of global steric hindrance and hydrophobic effects affecting the conformation of the chain in solution is proposed to explain the limited accessibility of the pyridine groups. The results question the classical neighboring group model generally used to describe the slowing down of the quaternization reaction with increasing quaternization ratio. The thermal stability of the quaternized polymers and the colors of the reaction medium are also discussed. © 1992 John Wiley & Sons, Inc.     

Synthesen von ω-substituierten ω-Nitrocarbonsäureestern aus α-Nitrocycloalkanonen

Synthesis of ω-Nitroalkanoates Substituted in ω-Position from α-Nitrocycloalkanones α-Nitrocycloalkanones substituted in α-position by a functionalized alkyl residue underwent ring opening to the corresponding chain derivatives by intermolecular nucleophilic attack; ω-nitroalkanoates substituted in ω-position were obtained (Scheme 1). The so formed methyl 6-nitro-9-oxodecanoate ( 3 ) was used to prepare methyl 8-(2-methyl-1,3-dioxolan-2-yl)octanoate ( 15 ), an intermediate in the synthesis of the sex phermone of the honey bee.