Diverse Methods with Stereoselective Induction in the Asymmetric Biginelli Reaction.

The relevance of the asymmetric Biginelli reaction (ABR) has been increased in this century, due to the pharmacological application of its products. This review focuses predominantly on articles published in the period from 2015 to 2024 on asymmetric synthetic advances in the formation of dihydropyrimidinones (DHPMs), dihydropyrimidinethiones (DHPMTs), and related compounds. The relevant bibliography on general processes in the Biginelli reaction and some methods of separation of isomers have also been referenced.

Multifunctionalized Carbon Dots as an Active Nanocarrier for Drug Delivery to the Glioblastoma Cell Line.

Nanoparticle-based nanocarriers represent a viable alternative to conventional direct administration in cancer cells. This advanced approach employs the use of nanotechnology to transport therapeutic agents directly to cancer cells, thereby reducing the risk of damage to healthy cells and enhancing the efficacy of treatment. By approving nanoparticle-based nanocarriers, the potential for targeted, effective treatment is greatly increased.

The Development of the Bengamides as New Antibiotics against Drug-Resistant Bacteria.

The bengamides comprise an interesting family of natural products isolated from sponges belonging to the prolific family. Their outstanding antitumor properties, coupled with their unique mechanism of action and unprecedented molecular structures, have prompted an intense research activity directed towards their total syntheses, analogue design, and biological evaluations for their development as new anticancer agents. Together with these biological studies in cancer research, in recent years, the bengamides have been identified as potential antibiotics by their impressive biological activities against various drug-resistant bacteria such as and .

Insights into the Photodecomposition of Azidomethyl Methyl Sulfide: A S/S Conical Intersection on Nitrene Potential Energy Surfaces Leading to the Formation of -Methyl--sulfenylmethanimine.

UV photodecomposition of azidomethyl methyl sulfide (AMMS) yields a transient -methylthiaziridine which rapidly evolves to -methyl--sulfenylmethanimine at 10 K. This species was detected by infrared matrix isolation spectroscopy. The mechanism of the photoreaction of AMMS has been investigated by a combined approach, using low-temperature matrix isolation FTIR spectroscopy in conjunction with two theoretical methods, namely, complete active space self-consistent field and multiconfigurational second-order perturbation.

P-doped carbon nano-powders for fingerprint imaging.

A simple, fast, and laboratory efficient doped P carbon nanoparticles synthesis is developed for fingerprint imaging, using 1,3-dihydroxyacetone and di-phosphorous pentoxide. Fluorescence nanoparticles, with an average size of 230 nm were obtained, without additional energy input or external heating. ATR, solid NMR, XPS and fluorescence spectroscopy revealed their surface functionalization; a reaction mechanism is proposed.

Rationalizing the catalytic activity of copper in the cycloaddition of azide and alkynes (CuAAC) with the topology of ∇(2)ρ(r) and ∇∇(2)ρ(r).

The distinct role of the Cu(I) in the Huisgen dipolar cycloaddition of azides to alkynes (denoted as CuAAC) is disclosed by following the evolution of the topology of the Laplacian of the electronic charge density, ∇(2)ρ(r), and its gradient vector field, ∇∇(2)ρ(r), along the reaction coordinate with several density functionals (wB97XD, LCwPBE, M06-2X, M06-L, B3LYP) and the 6-311++G(d,p) basis set. Remarkably, in view of the topology of ∇(2)ρ(r) and ∇∇(2)ρ(r), the mechanism appears to be diverse (asynchronous concerted or stepwise) depending on the reaction conditions. Overall, the catalyst orchestrates first the formation of the external N-C and subsequently the internal one by following alternatively a pericyclic-like or a pseudopericyclic-like mechanism.

Advances in the synthesis of calystegines and related products and their biochemical properties.

The revision of the structures and properties of Calystegines shows that they can be regarded as carbohydrate mimics, with related biological activities and peculiar characteristics. Not only they can be isolated from food plants, but they can be obtained from a variety of monosaccharide derivatives and of non-carbohydrate products. Although several synthetic calystegine analogs have been reported as glycosidase inhibitors, new, more potent and effective inhibitors are required.

6-Azido-3-O-benzyl-6-de-oxy-N,N-diethyl-1,2-O-isopropyl-idene-d-glycero-α-d-gluco-heptofuran-uronamide.

Reaction of 3-O-benzyl-1,2-O-isopropyl-idene-α-xylo-pentodialdo-1,4-furan-ose with N,N-diethyl-2-(dimethyl-sulfuranil-idene)acetamide gave stereoselectively an ep-oxy-amide, which was regioselectively opened by NaN(3) in dimethyl formamide to give the title compound, C(21)H(30)N(4)O(6). X-ray crystallography confirmed the relative stereochemistry of the title compound and the absolute configuration was determined by the use of d-glucose as the starting material. There are two mol-ecules in the asymmetric unit (Z' = 2).

7-Azido-N,N-diethyl-4,5-O-isopropyl-idene-4-C-methyl-3,6-anhydro-7-de-oxy-d-glycero-d-manno-heptonamide.

The reaction of 5-azido-5-de-oxy-2,3-O-isopropyl-idene-2-C-methyl-d-ribose with N,N-diethyl-2-(dimethyl-sulfuranyl-idene)acetamide gave the title compound, C(15)H(26)N(4)O(5), as the major product arising from initial formation of an epoxide which was subsequently opened by intra-molecular attack of the free 4-hydroxyl group. X-ray crystallography confirmed the relative stereochemistry of the title compound and the absolute configuration was determined by the use of d-ribose as the starting material. The crystal structure contains chains of mol-ecules running parallel to the a axis, being linked by weak bifurcated O-H⋯(N,N) hydrogen bonds.

Easy and Stereoselective One-Step Incorporation of Two Asymmetric Carbons in Pyranose Derivatives to Acyclic Epoxyamides: New, Potentially Useful Acyclic Chiral Templates.

We reacted N,N-diethyl-2-(dimethylsulfuranylidene)acetamide with 4,6-O-alkylidene-glycopyranoses under several experimental conditions and obtained, stereoselectively, derivatives of acyclic 3-(polyhydroxyalkyl)-alpha,beta-epoxyamides. In this way, and in one stage, we introduced, highly stereoselectively, two new chiral carbons with a substituted asymmetric epoxide group that could then be regioselectively transformed and, in addition, obtained highly functionalized acyclic structures starting from easily obtained cyclohemiacetalic monosaccharides. The configuration of the new chiral carbons of the resulting trans-epoxyamides was determined by comparing the IR, NMR, and polarimetric data with another epoxyamide of known configuration.