Simple Synthesis of 7‐Formyl‐indole

A simple route to 7‐formyl‐indole (5) is described in which appropriately functionalized o‐nitrotoluenes (1) are converted to 7‐hydroxymethyl‐indole (4) using the Batcho–Leimgruber process. Condensation of 3‐methyl‐2‐nitrobenzyl alcohol (1a) with N,N‐dimethylformamide dimethyl acetal yields the enamine 2a, which upon catalytic hydrogenation affords 4 in 22% yield. When the hydroxyl function in 1 is protected with pivaloyl or tetrahydropyranyl group, the yields of 4 are increased to 39% and 48%, respectively. Finally, 4 is oxidized with pyridinium chlorochromate (PCC) to afford 5 in 86% yield.     

Synthesis of N‐Protected/Free Indole‐7‐Carboxaldehyde

A direct method for the preparation of N‐protected/free indole‐7‐carboxaldehyde is reported from the corresponding N‐protected 7‐bromomethylindoles using three different conditions.     

Synthesis of O‐β‐D‐Glucopyranosides of 7‐Hydroxy‐3‐(imidazol‐2‐yl)‐4H‐chromen‐4‐ones

The 7‐hydroxy‐3‐formyl‐4H‐chromen‐4‐one 1 reacted with various cyclic 1,2‐dicarbonyl compounds in the presence of ammonium acetate to furnish 7‐hydroxy‐3‐([4,5‐fused] imidazol‐2‐yl)‐4H‐chromen‐4‐ones 2a–f, which on glucosylation with α‐acetobromoglucose affords 2,3,4,6‐tetra‐O‐acetyl‐β‐D‐glucopyranosyloxy‐3‐([4,5‐fused] imidazol‐2‐yl)‐4H‐chromen‐4‐ones 3a–f. 7‐O‐β‐D‐Glucopyranosyloxy‐3‐([4,5‐fused] imidazol‐2‐yl)‐4H‐chromen‐4‐ones 4a–f were prepared by deacetylation with anhydrous zinc acetate in absolute methanol. The structure of these new O‐β‐D‐glucosides was established on the basis of chemical, elemental, and spectral analysis. These compounds were evaluated for their in vitro biological activity.

     

Highly Regioselective One‐Pot Synthesis of 7‐Hydroxy‐6‐methylphthalide from 3‐Hydroxy‐4‐methylbenzylalcohol

7‐Hydroxy‐6‐methylphthalide 2 was synthesized with high regioselectivity and moderate yield using a novel one‐pot synthesis that employed 3‐hydroxy‐4‐methylbenzylalcohol 1 and formaldehyde in the presence of tin(IV) chloride as catalyst and triethylamine as base. The proposed mechanism of the formation of 2 involves ortho‐formylation followed by hemiacetal formation and oxidation.     

Synthesis of 7‐Sulfamoyl‐substituted 2‐Oxo‐2,3,4,5‐tetrahydro‐1H‐benzo[b]azepines

Sulfochlorination of 2‐оxo‐2,3,4,5‐tetrahydro‐1H‐benzo[b]azepine led to regioselective formation of the corresponding 7‐chlorosulfonyl derivative. Starting from this reagent, a large number of substituted 2‐oxo‐7‐sulfamoyl‐2,3,4,5‐tetrahydro‐1H‐benzo[b]azepines were obtained. This approach is amenable to combinatorial production of the title compounds, which possess promising therapeutic potential.     

Acronycine Analog: New Selective Synthesis of 6‐Methoxy‐3,3‐dimethyl‐3H,7H‐pyrano[2,3‐c]xanthen‐7‐one

A new, convenient, and selective route to the dimethylpyrano[2,3‐c]xanthen‐7‐one, analog of acronycine, via aromatization and dehydrogenation reactions from the corresponding saturated hexahydro intermediate is described.     

Simple Synthesis of 7‐Amino‐4,5‐dihydrobenzo[f][1,4]oxazepin‐3‐ones

A simple method for the synthesis of 7‐amino‐4,5‐dihydro‐benzo[f][1,4]oxazepin‐3‐ones from 5‐nitrobenzaldehydes and 2‐haloesters was described. The three‐step procedure involves the synthesis of methyl 2‐(2‐formyl‐4‐nitrophenoxy)alkanoates, followed by reaction with hydrazine hydrate and reductive cyclization of the formed aldazines. 2‐Hydroxyethyl derivatives of the title amines were prepared in good yields.     

Strategies towards the Synthesis of 6‐N,N‐Diethylcarbamyloxy‐1,4‐dimethoxy‐ 7‐naphthylboronic Acid

After acetylation, condensation between Danishefsky's diene and benzoquinone afforded a stable methoxytriacetoxydihydronaphthalene intermediate, which was subsequently transformed by the Snieckus DOM protocol into the regiospecific 7‐naphthylboronic acid.     

Efficient and Simple Synthesis of Substituted 3‐Phenyl‐7‐methoxybenzopyrans as Pseudo‐Vitamin‐D3 Analogs

An efficient and simple synthesis of substituted 3‐phenyl‐7‐methoxybenzopyrans as pseudo‐vitamin‐D₃ analogs in good yields under mild reaction conditions is described.     

Synthesis of 7‐Alkoxy/Hydroxy‐α‐methyltryptamines

Abstract

A simple method for the preparation of 7‐alkoxy/hydroxy‐α‐methyl‐DL‐tryptamines is reported. The key steps of the synthesis are the Japp–Klingemann coupling of 2‐piperidone‐3‐carboxylic acid 3 with diazonium salts 4, the Fischer‐type cyclization of hydrazones 5 to β‐carboline derivatives 6 and their hydrolysis to title compounds 8.     

Analysis of Insulin by High Performance Liquid Chromatographic Method with Precolumn Derivatization with 4‐Chloro‐7‐Nitrobenzo‐2‐Oxa‐1,3‐Diazole

Abstract

A high performance liquid chromatographic method (HPLC) with precolumn derivatization and fluorescence detection for insulin was developed and applied for the quantification of insulin in spiked serum. To covalence couple with insulin, 4‐chloro‐7‐nitrobenzo‐2‐oxa‐1,3‐diazole (NBD‐Cl) was selected as fluorescent reagent. The optimal derivatization conditions were as follows: temperature 50; time 2 h, in the dark; 0.1 M phosphate buffer (pH 9.0). Analytical separation was carried out on a C18 column and the mobile phase including acetonitrile‐water containing 0.1% trifluoroacetic acid (TFA) (v/v∶ 30/70). The excitation/emission wavelengths were 470/540 nm. Under the conditions, the retention time and capacity factor of the adduct of insulin‐NBD were 10.03 min (flow rate 1 mL/min) and 3, respectively. The recovery of insulin in serum was 95.06% and the detection limit was 90 nM. In the investigated concentration ranges (0.46 µM～16.10 µM), R² was 0.9934, which indicated the potential for the application of NBD‐Cl derivatization to the analysis of insulin in the biological matrices, although with the shortcoming of long analytical time.     

Unexpected Rearrangement in the Reaction of 7‐Mercapto‐4‐methylcoumarin with 1‐Mono‐ and 1,1‐Dimethyl Propargyl Alcohols

The reaction of 7‐mercapto‐4‐methylcoumarin (4) with 1‐mono‐ and 1,1‐dimethyl propargyl alcohols in H₃PO₄ afforded the corresponding β‐(7‐coumarinthio)ketones with a rearrangement of the carbon chain of propargyl. A possible mechanism of this rearrangement was proposed.     

An Efficient Synthesis of Derivatives of 2‐Acetamido‐4‐amino‐2,4,6‐trideoxy‐D‐galactopyranose

Abstract

Methyl 2‐acetamido‐4‐amino‐2,4,6‐trideoxy‐α‐D‐galactopyranoside (10) was synthesized from D‐glucosamine hydrochloride in eight steps in an overall yield of 31%. Key steps include the selective benzoylation at O‐3 of methyl 2‐acetamido‐2,6‐dideoxy‐α‐D‐glucopyranoside in 89% yield and the subsequent Mitsunobu reaction using diphenylphosphoryl azide as the azide source which proceeded in 92% yield. Di‐ and mono‐benzyloxycarbonyl derivatives of 10 were also prepared.     

Preparation of Some Derivatives of N‐tert‐Butyldecahydro‐3‐isoquinoline Carboxamide

N‐tert‐Butyldecahydro‐3‐isoquinoline carboxamide (1) is a key structural fragment present in a variety of medicinally important HIV protease inhibitors. Derivatives of this carboxamide were prepared by alkylation with either 2‐iodoethanol, allyl bromide, or bromoacetaldehyde dimethylacetal. The corresponding aldehyde of the dimethylacetal derivative was prepared by reaction with BBr₃ in CH₂Cl₂.     

Preparation of Alkyl Carbamate of 1‐Protected Indole‐3‐methylamine as a Precursor of Indole‐3‐methylamine

A series of alkyl carbamates 3 of 1‐protected indole‐3‐methylamines, alkyl carbamates 6 of thiophenylmethylamines, and pyrrolylmethylamines were prepared from the corresponding acetamides 2 and 5 in good to excellent yields via diacetoxyiodobenzene‐promoted Hofmann rearrangement. For a successful Hofmann rearrangement, an electron‐withdrawing group on position 1 of indolylacetamide and pyrrolylacetamide was required. The alkyl carbamate 3g was demonstrated to serve well as a stable precursor of 1‐protected indole‐3‐methylamine 1.     

Synthesis of New (4‐Acetonylidene‐2,6,8,9‐tetramethyl‐7H‐imidazo[1,5,4‐e,f][1,5]benzodiazepine) Derivatives

Imidazobenzodiazepine derivatives were obtained by cyclization of the condensation products 7‐amino‐2,5,6‐trimethylbenzimidazole with acetylacetone and ethyl acetoacetate. By careful examination of spectroscopic data and the open‐chain intermediate isolation, we have identified the formed compound structure.     

Synthesis of 2,3‐Dihydroxy‐1‐Epilupinine

The 1,3‐dipolar cycloaddition of unsaturated D‐threo‐hexaldonolactone 3 and a six‐membered cyclic nitrone 11 led to a single adduct 15, which could be transformed into (1S, 2S, 3S, 9aS)‐2,3‐dihydroxy‐1‐hydroxymethyl‐quinolizidine 28 related to epilupinine via a reaction sequence involving rearrangement of the six‐membered lactone ring into a five‐membered one, removal of the terminal carbon atom from the sugar chain, cleavage of the N‐O bond, and the intramolecular alkylation of the nitrogen atom.      

One‐Pot Synthesis of Ene‐Lactams via N‐Debenzylation of Keto‐Containing N‐2,4‐Dimethoxylbenzylamides

Abstract

A general method of ene‐lactam preparation is described. Ene‐lactams can be prepared efficiently from keto‐containing N‐2,4‐dimethoxylbenzylamides in good to excellent yields. This method is applicable for the preparation of substituted δ‐, γ‐, and ?‐ene‐lactams and bicyclic ene‐lactams.     

Bromination of 4‐Dichloromethyl‐4‐methylcyclohexa‐2,5‐dien‐1‐ones

Bromination of 4‐dichloromethyl‐4‐methylcyclohexa‐2,5‐dien‐1‐one and 4‐dichloromethyl‐3,4‐dimethylcyclohexa‐2,5‐dien‐1‐one has been studied. The reaction conditions required for the formation of mono‐, di‐, and tribrominated products have been optimized.