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Differential Proliferation Effect of the Newly Synthesized Valine, Tyrosine and Tryptophan–Naphthoquinones in Immortal and Tumorigenic Cervical Cell Lines

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dc.contributor 170687 es_ES
dc.contributor 5505 es_ES
dc.contributor 206747 es_ES
dc.coverage.spatial Global es_ES
dc.creator Córdova Rivas, Sergio
dc.creator Araujo Huitrado, Jorge Gustavo
dc.creator Rivera Avalos, Ernesto
dc.creator Escalante García, Ismailia Leilani
dc.creator Durón Torres, Sergio Miguel
dc.creator López Hernández, Yamile
dc.creator Hernández López, Hiram
dc.creator López, Lluvia
dc.creator De Loera, Denisse
dc.creator López, Jesús Adrian
dc.date.accessioned 2021-05-25T23:35:06Z
dc.date.available 2021-05-25T23:35:06Z
dc.date.issued 2020-04
dc.identifier info:eu-repo/semantics/publishedVersion es_ES
dc.identifier.issn 1420-3049 es_ES
dc.identifier.uri http://ricaxcan.uaz.edu.mx/jspui/handle/20.500.11845/2517
dc.description.abstract We previously showed that microwave assisted synthesis is the best method for the synthesis of naphthoquinone amino acid and chloride-naphthoquinone amino acid derivatives by a complete evaluation of reaction conditions such as stoichiometry, bases, and pH influence. Following the same strategy, we synthesized chloride and non-chloride tyrosine, valine, and tryptophan-naphthoquinones achieving 85–95%, 80–92%, and 91–95% yields, respectively. The cyclic voltammetry profiles showed that both series of naphthoquinone amino acid derivatives mainly display one redox reaction process. Overall, chloride naphthoquinone amino acid derivatives exhibited redox potential values (E1/2) more positive than non-chloride compounds. The six newly synthesized compounds were tested in HPV positive and negative as well as in immortal and tumorigenic cell lines to observe the effects in different cellular context simulating precancerous and cancerous status. A dose-response was achieved to determine the IC50 of six newly synthesized compounds in SiHa (Tumorigenic and HPV16 positive), CaLo (Tumorigenic and HPV18 positive), C33-A (Tumorigenic and HPV negative) and HaCaT (Keratinocytes immortal HPV negative) cell lines. Non-chloride tryptophan-naphthoquinone (3c) and chloride tyrosine-naphthoquine (4a) effects were more potent in tumorigenic SiHa, CaLo, and C33-A cells with respect to non-tumorigenic HaCaT cells. Interestingly, there seems to be a differential effect in non-chloride and chloride naphthoquinone amino acid derivatives in tumorigenic versus non tumorigenic cells. Considering all naphthoquinone amino acid derivatives that our group synthesized, it seems that hydrophobic and aromatic amino acids have the greatest effect on cell proliferation inhibition. These results show promising compounds for cervical cancer treatment es_ES
dc.language.iso spa es_ES
dc.publisher MDPI es_ES
dc.relation https://www.mdpi.com/1420-3049/25/9/2058 es_ES
dc.relation.uri generalPublic es_ES
dc.rights Atribución-NoComercial-CompartirIgual 3.0 Estados Unidos de América *
dc.rights.uri http://creativecommons.org/licenses/by-nc-sa/3.0/us/ *
dc.source Molecules 2020, 25, 2058 es_ES
dc.subject.classification BIOLOGIA Y QUIMICA [2] es_ES
dc.subject.other naphthoquinone es_ES
dc.subject.other amino acids es_ES
dc.subject.other alternative methods es_ES
dc.subject.other microwave es_ES
dc.subject.other ultrasound es_ES
dc.subject.other anticancer es_ES
dc.title Differential Proliferation Effect of the Newly Synthesized Valine, Tyrosine and Tryptophan–Naphthoquinones in Immortal and Tumorigenic Cervical Cell Lines es_ES
dc.type info:eu-repo/semantics/article es_ES


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