Urszula Bąchor scite author profile

In this review, we present reports on the immunoregulatory properties of isoxazole derivatives classified into several categories, such as immunosuppressive, anti-inflammatory, immunoregulatory, and immunostimulatory compounds. The compounds were tested in various models using resident cells from rodents and humans, cell lines, and experimental animal disease models corresponding to human clinical situations. Beneficial features of the described isoxazole derivatives include low toxicity and good bioactivity at low doses. In a majority of studies, the activities of investigated compounds were comparable or even higher than registered reference drugs. Whenever possible, a plausible mechanism of action of the investigated compounds and their potential therapeutic utility were proposed. Among the described compounds, particular attention was paid to the class of immune stimulators with a potential application in chemotherapy patients.

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Synthesis, immunosuppressive properties, mechanism of action and X-ray analysis of a new class of isoxazole derivatives

Bąchor¹,

Ryng²,

Mączyński³

et al. 2019

Acta Poloniae Pharmaceutica - Drug Research

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Heterocyclic compounds play an important role in drug design. They are main elements of a wide range of natural products, such as nucleic acids, amino acids, alkaloids, and vitamins. The pharmacological benefits of employing isoxazole moiety are due to the fact that this structure acts as a key pharmacophore for the biological activity of such drugs as valdecoxib (COX-2 inhibitor) (1) or leflunomide (antirheumatic drug) (2). The compounds containing isoxazole moiety are also promising therapeutic agents in neurodegenerative diseases due to their similarity to the α-amino-3hydroxy-5-methyl-4-isoxazolepropionic acid, that is a specific agonist for the AMPA receptor (3). Based on the structure of these drugs, the series of compounds containing the isoxazole moiety were synthesized by Ryng et al. and their immunological profiles were examined (4-7). Of interest, among all compounds synthesized by our team, the modification in position 4 of the isoxazole structure led to unexpected biological activity. Our previous studies describing the synthesis of N-phenyl-5-amino-3methylisoxazole-4-carboxamides, containing different substituents in the phenyl ring, revealed the structure-activity relationship in some immunological tests (8). These results prompted us to continue the search for new derivatives of 4-substituted isoxazoles. The syntheses resulted in obtaining a series of amides as well as 4-ureilene derivatives of 5amino-3-methyl-4-isoxazolecarboxylic acid exhibit

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Selected β2-, β3- and β2,3-Amino Acid Heterocyclic Derivatives and Their Biological Perspective

Bąchor¹,

Mączyński²

2021

Molecules

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Heterocyclic moieties, especially five and six-membered rings containing nitrogen, oxygen or sulfur atoms, are broadly distributed in nature. Among them, synthetic and natural alike are pharmacologically active compounds and have always been at the forefront of attention due to their pharmacological properties. Heterocycles can be divided into different groups based on the presence of characteristic structural motifs. The presence of β-amino acid and heterocyclic core in one compound is very interesting; additionally, it very often plays a vital role in their biological activity. Usually, such compounds are not considered to be chemicals containing a β-amino acid motif; however, considering them as this class of compounds may open new routes of their preparation and application as new drug precursors or even drugs. The possibility of their application as nonproteinogenic amino acid residues in peptide or peptide derivatives synthesis to prepare a new class of compounds is also promising. This review highlights the actual state of knowledge about β-amino acid moiety-containing heterocycles presenting antiviral, anti-inflammatory, antibacterial compounds, anaplastic lymphoma kinase (ALK) inhibitors, as well as agonist and antagonists of the receptors.

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New water-soluble isoxazole-linked 1,3,4-oxadiazole derivative with delocalized positive charge

et al. 2021

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The In Vitro Impact of Isoxazole Derivatives on Pathogenic Biofilm and Cytotoxicity of Fibroblast Cell Line

Bąchor

Junka

Brożyna

et al. 2023

IJMS

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The microbial, biofilm-based infections of chronic wounds are one of the major challenges of contemporary medicine. The use of topically administered antiseptic agents is essential to treat wound-infecting microorganisms. Due to observed microbial tolerance/resistance against specific clinically-used antiseptics, the search for new, efficient agents is of pivotal meaning. Therefore, in this work, 15 isoxazole derivatives were scrutinized against leading biofilm wound pathogens Staphylococcus aureus and Pseudomonas aeruginosa, and against Candida albicans fungus. For this purpose, the minimal inhibitory concentration, biofilm reduction in microtitrate plates, modified disk diffusion methods and antibiofilm dressing activity measurement methods were applied. Moreover, the cytotoxicity and cytocompatibility of derivatives was tested toward wound bed-forming cells, referred to as fibroblasts, using normative methods. Obtained results revealed that all isoxazole derivatives displayed antimicrobial activity and low cytotoxic effect, but antimicrobial activity of two derivatives, 2-(cyclohexylamino)-1-(5-nitrothiophen-2-yl)-2-oxoethyl 5-amino-3-methyl-1,2-oxazole-4-carboxylate (PUB9) and 2-(benzylamino)-1-(5-nitrothiophen-2-yl)-2-oxoethyl 5-amino-3-methyl-1,2-oxazole-4-carboxylate (PUB10), was noticeably higher compared to the other compounds analyzed, especially PUB9 with regard to Staphylococcus aureus, with a minimal inhibitory concentration more than x1000 lower compared to the remaining derivatives. The PUB9 and PUB10 derivatives were able to reduce more than 90% of biofilm-forming cells, regardless of the species, displaying at the same time none (PUB9) or moderate (PUB10) cytotoxicity against fibroblasts and high (PUB9) or moderate (PUB10) cytocompatibility against these wound cells. Therefore, taking into consideration the clinical demand for new antiseptic agents for non-healing wound treatment, PUB9 seems to be a promising candidate to be further tested in advanced animal models and later, if satisfactory results are obtained, in the clinical setting.

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Urszula Bąchor

Isoxazole Derivatives as Regulators of Immune Functions

Synthesis, immunosuppressive properties, mechanism of action and X-ray analysis of a new class of isoxazole derivatives

Selected β2-, β3- and β2,3-Amino Acid Heterocyclic Derivatives and Their Biological Perspective

New water-soluble isoxazole-linked 1,3,4-oxadiazole derivative with delocalized positive charge

The In Vitro Impact of Isoxazole Derivatives on Pathogenic Biofilm and Cytotoxicity of Fibroblast Cell Line

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