Synthesis of Polycyclic Hetero-Fused 7-Deazapurine Heterocycles and Nucleosides through C-H Dibenzothiophenation and Negishi Coupling

Yang, Chao; Poštová Slavětínská, Lenka; Fleuti, Marianne; Klepetářová, Blanka; Tichý, Michal; Gurská, S.; Pavliš, P.; Džubák, P.; Hajdúch, M.; Hocek, Michal

doi:https://dx.doi.org/10.1021/jacs.2c07517

Number of the records: 1

Synthesis of Polycyclic Hetero-Fused 7-Deazapurine Heterocycles and Nucleosides through C-H Dibenzothiophenation and Negishi Coupling

1.

SYSNO ASEP	0563594
Document Type	J - Journal Article
R&D Document Type	Journal Article
Subsidiary J	Článek ve WOS
Title	Synthesis of Polycyclic Hetero-Fused 7-Deazapurine Heterocycles and Nucleosides through C-H Dibenzothiophenation and Negishi Coupling
Author(s)	Yang, Chao (UOCHB-X)_ORCID Poštová Slavětínská, Lenka (UOCHB-X)_RID Fleuti, Marianne (UOCHB-X)_ORCID Klepetářová, Blanka (UOCHB-X)_{RID, ORCID} Tichý, Michal (UOCHB-X)_{RID, ORCID} Gurská, S. (CZ) Pavliš, P. (CZ) Džubák, P. (CZ) Hajdúch, M. (CZ) Hocek, Michal (UOCHB-X)_{RID, ORCID}
Source Title	Journal of the American Chemical Society. - : American Chemical Society - ISSN 0002-7863 Roč. 144, č. 42 (2022), s. 19437-19446
Number of pages	10 s.
Language	eng - English
Country	US - United States
Keywords	enzymatic incorporation ; antiviral activity ; analogs
OECD category	Biochemistry and molecular biology
R&D Projects	LX22NPO5102 GA MŠMT - Ministry of Education, Youth and Sports (MEYS)
	LM2018133 GA MŠMT - Ministry of Education, Youth and Sports (MEYS)
Research Infrastructure	CZ-OPENSCREEN III - 90130 - Ústav molekulární genetiky AV ČR, v. v. i.
Method of publishing	Open access
Institutional support	UOCHB-X - RVO:61388963
UT WOS	000873799700001
EID SCOPUS	85140486506
DOI	10.1021/jacs.2c07517
Annotation	A new approach for synthesizing polycyclic heterofused 7-deazapurine heterocycles and the corresponding nucleosides was developed based on C-H functionalization of diverse (hetero)aromatics with dibenzothiophene-S-oxide followed by the Negishi cross-cooupling with bis(4,6-dichloropyrimidin-5-yl)zinc. This cross-coupling afforded a series of (het)aryl-pyrimidines that were converted to fused deazapurine heterocycles through azidation and thermal cyclization. The fused heterocycles were glycosylated to the corresponding 2′-deoxy- and ribonucleosides, and a series of derivatives were prepared by nucleophilic substitutions at position 4. Four series of new polycyclic thieno-fused 7-deazapurine nucleosides were synthesized using this strategy. Most of the deoxyribonucleosides showed good cytotoxic activity, especially for the CCRF-CEM cell line. Phenyl- and thienyl-substituted thieno-fused 7-deazapurine nucleosides were fluorescent, and the former one was converted to 2′-deoxyribonucleoside triphosphate for enzymatic synthesis of labeled oligonucleotides.
Workplace	Institute of Organic Chemistry and Biochemistry
Contact	asep@uochb.cas.cz ; Kateřina Šperková, Tel.: 232 002 584 ; Jana Procházková, Tel.: 220 183 418
Year of Publishing	2023
Electronic address	https://doi.org/10.1021/jacs.2c07517

Number of the records: 1