Discovery of Nitro-azolo[1,5-a]pyrimidines with Anti-Inflammatory and Protective Activity against LPS-Induced Acute Lung Injury

Spasov, A.; Kosolapov, V.; Babkov, D.; Klochkov, V.; Sokolova, E.; Miroshnikov, M.; Borisov, A.; Velikorodnaya, Y.; Smirnov, A.; Savateev, K.; Fedotov, V.; Kotovskaya, S.; Rusinov, V.

doi:10.3390/ph15050537

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Название:	Discovery of Nitro-azolo[1,5-a]pyrimidines with Anti-Inflammatory and Protective Activity against LPS-Induced Acute Lung Injury
Авторы:	Spasov, A. Kosolapov, V. Babkov, D. Klochkov, V. Sokolova, E. Miroshnikov, M. Borisov, A. Velikorodnaya, Y. Smirnov, A. Savateev, K. Fedotov, V. Kotovskaya, S. Rusinov, V.
Дата публикации:	2022
Издатель:	MDPI
Библиографическое описание:	Discovery of Nitro-azolo[1,5-a]pyrimidines with Anti-Inflammatory and Protective Activity against LPS-Induced Acute Lung Injury / A. Spasov, V. Kosolapov, D. Babkov et al. // Pharmaceuticals. — 2022. — Vol. 15. — Iss. 5. — 537.
Аннотация:	Acute lung injury remains a challenging clinical condition, necessitating the development of novel, safe and efficient treatments. The prevention of macrophage M1-polarization is a viable venue to tackle excessive inflammation. We performed a phenotypic screening campaign to identify azolopyrimidine compounds that effectively inhibit LPS-induced NO synthesis and interleukin 6 (IL-6) secretion. We identified lead compound 9g that inhibits IL-6 secretion with IC50 of 3.72 µM without apparent cytotoxicity and with minimal suppression of macrophage phagocytosis in contrast to dexamethasone. In a mouse model of LPS-induced acute lung injury, 30 mg/kg i.p. 9g ameliorated anxiety-like behavior, inhibited IL-6 release, and limited neutrophil infiltration and pulmonary edema. A histological study confirmed the protective activity of 9g. Treatment with compound 9g prevented the migration of CD68+ macrophages and the incidence of hemorrhage. Hence, we have identified a promising pharmacological approach for the treatment of acute lung injury that may hold promise for the development of novel drugs against cytokine-mediated complications of bacterial and viral infections. © 2022 by the authors. Licensee MDPI, Basel, Switzerland.
Ключевые слова:	ACUTE LUNG INJURY AZOLO[1,5-A]PYRIMIDINES CYTOKINE IL-6 INFLAMMATION MACROPHAGE 2 (5 NITROFUR 2 YL) 5 METHYL 6 NITRO 1,2,4 TRIAZOLO[1,5 A]PYRIMIDIN 7 ONE AMINOGUANIDINIUM 2 (5 NITROFUR 2 YL) 5 METHYL 6 NITRO 1,2,4 TRIAZOLO[1,5 A]PYRIMIDIN 7 ONE GUANIDINIUM 2 [[5 METHYL 6 NITROTETRAZOLO[1,5 A]PYRIMIDIN 7 YL]AMINO]ETHANOL 3 [[5 METHYL 6 NITROTETRAZOLO[1,5 A]PYRIMIDIN 7 YL]AMINO]ETHANOL 3 [[5 METHYL 6 NITROTETRAZOLO[1,5 A]PYRIMIDIN 7 YL]AMINO]PROPANE 1,2 DIOL 4 [2 [[6 NITRO 2 [PROP 2 YN 1 YLSULFANYL][1,2,4]TRIAZOLO[1,5 A]PYRIMIDIN 7 YL]AMINO]ETHYL]PHENOL ANTIINFLAMMATORY AGENT CD68 ANTIGEN DEXAMETHASONE INTERLEUKIN 6 LIPOPOLYSACCHARIDE N (4 CHLOROPHENETHYL) 6 NITRO 2 (PROP 2 YN 1 YL SULFANYL)[1,2,4]TRIAZOLO[1,5 A]PYRIMIDIN 7 AMINE N ISOPROPYL 5 METHYL 6 NITROTETRAZOLO[1,5 A]PYRIMIDIN 7 AMINE N TERT BUTYL 5 METHYL 6 NITROTETRAZOLO[1,5 A]PYRIMIDIN 7 AMINE N [2 (4 CHLOROPHENYL)ETHYL] 5 METHYL 6 NITROTETRAZOLO[1,5 A]PYRIMIDIN 7 AMINE N [2 (4 HYDROXYPHENYL)ETHYL] 5 METHYL 6 NITROTETRAZOLO[1,5 A]PYRIMIDIN 7 AMINE NITRIC OXIDE NITRO AZOLO[1,5 A]PYRIMIDINE DERIVATIVE PYRIMIDINE DERIVATIVE UNCLASSIFIED DRUG ACUTE LUNG INJURY ANIMAL CELL ANIMAL EXPERIMENT ANIMAL MODEL ANIMAL TISSUE ANTIINFLAMMATORY ACTIVITY ARTICLE CARBON NUCLEAR MAGNETIC RESONANCE CONTROLLED STUDY CYTOKINE RELEASE CYTOTOXICITY DRUG ISOLATION DRUG SCREENING DRUG STRUCTURE DRUG SYNTHESIS ENZYME INHIBITION LUNG EDEMA MACROPHAGE MALE MOUSE NEUTROPHIL CHEMOTAXIS NONHUMAN PHAGOCYTOSIS PROTON NUCLEAR MAGNETIC RESONANCE STRUCTURE ACTIVITY RELATION
URI:	http://elar.urfu.ru/handle/10995/117866
Условия доступа:	info:eu-repo/semantics/openAccess
Идентификатор SCOPUS:	85129695328
Идентификатор WOS:	000801257500001
Идентификатор PURE:	30209529
ISSN:	14248247
DOI:	10.3390/ph15050537
Сведения о поддержке:	Ministry of Education and Science of the Russian Federation, Minobrnauka: 075-15-2020-777 Funding: This research was funded by the Ministry of Science and Higher Education of the Russian Federation (Agreement on the provision of grants from the federal budget in the form of subsidies under paragraph 4 of Article 78.1 of the Budget Code of the Russian Federation, Moscow, 1 October 2020 No. 075-15-2020-777).
Располагается в коллекциях:	Научные публикации ученых УрФУ, проиндексированные в SCOPUS и WoS CC

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