In vitro anticancer activity and mechanism of action of an aziridinyl galactopyranoside

Burgos Morón, Estefanía; Pastor Carrillo, Nuria María; Orta Vázquez, Manuel Luis; Jiménez Alonso, Julio José; Palo Nieto, Juan Carlos; Vega Holm, Margarita; Vega Pérez, José Manuel; Iglesias Guerra, Fernando; Mateos Cordero, Santiago; López Lázaro, Miguel; Calderón Montaño, José Manuel

doi:10.3390/biomedicines10010041

Artículo

dc.creator	Burgos Morón, Estefanía	es
dc.creator	Pastor Carrillo, Nuria María	es
dc.creator	Orta Vázquez, Manuel Luis	es
dc.creator	Jiménez Alonso, Julio José	es
dc.creator	Palo Nieto, Juan Carlos	es
dc.creator	Vega Holm, Margarita	es
dc.creator	Vega Pérez, José Manuel	es
dc.creator	Iglesias Guerra, Fernando	es
dc.creator	Mateos Cordero, Santiago	es
dc.creator	López Lázaro, Miguel	es
dc.creator	Calderón Montaño, José Manuel	es
dc.date.accessioned	2022-01-24T15:34:00Z
dc.date.available	2022-01-24T15:34:00Z
dc.date.issued	2022
dc.identifier.citation	Burgos Morón, E., Pastor Carrillo, N.M., Orta Vázquez, M.L., Jiménez Alonso, J.J., Palo Nieto, J.C., Vega Holm, M.,...,Calderón Montaño, J.M. (2022). In vitro anticancer activity and mechanism of action of an aziridinyl galactopyranoside. Biomedicines, 10 (1), 41.
dc.identifier.issn	2227-9059	es
dc.identifier.uri	https://hdl.handle.net/11441/129134
dc.description.abstract	We recently screened a series of new aziridines β-D-galactopyranoside derivatives for selective anticancer activity and identified 2-methyl-2,3-[N-(4-methylbenzenesulfonyl)imino]propyl 2,3-di-O-benzyl-4,6-O-(S)-benzylidene-β-D-galactopyranoside (AzGalp) as the most promising com-pound. In this article, we explore the possible mechanisms involved in the cytotoxicity of this aziridine and evaluate its selective anticancer activity using cancer cells and normal cells from a variety of tissues. Our data show that AzGalp induces DNA damage (comet assay). Cells deficient in the nucleotide excision repair (NER) pathway were hypersensitive to the cytotoxicity of this com-pound. These results suggest that AzGalp induces bulky DNA adducts, and that cancer cells lacking a functional NER pathway may be particularly vulnerable to the anticancer effects of this aziridine. Several experiments revealed that neither the generation of oxidative stress nor the inhibition of glycolysis played a significant role in the cytotoxicity of AzGalp. Combinations of AzGalp with oxaliplatin or 5-fluorouracil slightly improved the ability of both anticancer drugs to selectively kill cancer cells. AzGalp also showed selective cytotoxicity against a panel of malignant cells versus normal cells; the highest selectivity was observed for two acute promyelocytic leukemia cell lines. Additional preclinical studies are necessary to evaluate the anticancer potential of AzGalp.	es
dc.description.sponsorship	Universidad de Sevilla VIPPIT-2019-I.5	es
dc.description.sponsorship	Junta de Andalucía 2017/CTS-657, 2019/CTS-657, 2021/CTS-657	es
dc.format	application/pdf	es
dc.format.extent	14 p.	es
dc.language.iso	eng	es
dc.publisher	Multidisciplinary Digital Publishing Institute (MDPI)	es
dc.relation.ispartof	Biomedicines, 10 (1), 41.
dc.rights	Attribution-NonCommercial-NoDerivatives 4.0 Internacional	*
dc.rights.uri	http://creativecommons.org/licenses/by-nc-nd/4.0/	*
dc.subject	Aziridine	es
dc.subject	Cancer	es
dc.subject	Cytotoxic	es
dc.subject	Cytotoxicity	es
dc.subject	Nucleotide excision repair	es
dc.subject	Selectivity	es
dc.title	In vitro anticancer activity and mechanism of action of an aziridinyl galactopyranoside	es
dc.type	info:eu-repo/semantics/article	es
dcterms.identifier	https://ror.org/03yxnpp24
dc.type.version	info:eu-repo/semantics/publishedVersion	es
dc.rights.accessRights	info:eu-repo/semantics/openAccess	es
dc.contributor.affiliation	Universidad de Sevilla. Departamento de Farmacología	es
dc.contributor.affiliation	Universidad de Sevilla. Departamento de Biología Celular	es
dc.contributor.affiliation	Universidad de Sevilla. Departamento de Química Orgánica y Farmacéutica	es
dc.relation.projectID	VIPPIT-2019-I.5	es
dc.relation.projectID	2017/CTS-657	es
dc.relation.projectID	2019/CTS-657	es
dc.relation.projectID	2021/CTS-657	es
dc.relation.publisherversion	https://doi.org/10.3390/biomedicines10010041	es
dc.identifier.doi	10.3390/biomedicines10010041	es
dc.journaltitle	Biomedicines	es
dc.publication.volumen	10	es
dc.publication.issue	1	es
dc.publication.initialPage	41	es

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