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    Por favor, use este identificador para citar o enlazar este ítem: http://hdl.handle.net/10259/9573

    Título
    Deregulation of lactate permeability using a small-molecule transporter (Lactrans-1) disturbs intracellular pH and triggers cancer cell death
    Autor
    Arias Betancur, Alain
    Fontova Pale, PereAutoridad UBU Orcid
    Alonso Carrillo, DanielAutoridad UBU Orcid
    Carreira Barral, IsraelAutoridad UBU Orcid
    Duis, Janneke
    García Valverde, MaríaAutoridad UBU Orcid
    Soto Cerrato, Vanessa
    Quesada Pato, RobertoAutoridad UBU Orcid
    Pérez Tomás, Ricardo
    Publicado en
    Biochemical Pharmacology. 2024, V. 229, 116469
    Editorial
    Elsevier
    Fecha de publicación
    2024-11
    ISSN
    0006-2952
    DOI
    10.1016/j.bcp.2024.116469
    Resumen
    Due to the relevance of lactic acidosis in cancer, several therapeutic strategies have been developed targeting its production and/or regulation. In this matter, inhibition approaches of key proteins such as lactate dehydrogenase or monocarboxylate transporters have showed promising results, however, metabolic plasticity and tumor heterogeneity limits their efficacy. In this study, we explored the anticancer potential of a new strategy based on disturbing lactate permeability independently of monocarboxylate transporters activity using a small molecule ionophore named Lactrans-1. Derived from click-tambjamines, Lactrans-1 facilitates transmembrane lactate transportation in liposome models and reduces cancer cell viability. The results showed that Lactrans-1 triggered both apoptosis and necrosis depending on the cell line tested, displaying a synergistic effect in combination with first-line standard chemotherapeutic cisplatin. The ability of this compound to transport outward lactate anions was confirmed in A549 and HeLa cells, two cancer cell lines having distinct rates of lactate production. In addition, through cell viability reversion experiments it was possible to establish a correlation between the amount of lactate transported and the cytotoxic effect exhibited. The movement of lactate anions was accompanied with intracellular pH disturbances that included basification of lysosomes and acidification of the cytosol and mitochondria. We also observed mitochondrial swelling, increased ROS production and activation of oxidative stress signaling pathways p38-MAPK and JNK/SAPK. Our findings provide evidence that enhancement of lactate permeability is critical for cellular pH homeostasis and effective to trigger cancer cell death, suggesting that Lactrans-1 may be a promising anticancer therapy.
    Palabras clave
    Lactate
    Anionophores
    Click-tambjamines
    Cancer metabolism
    pH deregulation
    Small molecules
    Materia
    Bioquímica
    Biochemistry
    Química orgánica
    Chemistry, Organic
    URI
    http://hdl.handle.net/10259/9573
    Versión del editor
    https://doi.org/10.1016/j.bcp.2024.116469
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    • Artículos BIOORG
    Atribución 4.0 Internacional
    Documento(s) sujeto(s) a una licencia Creative Commons Atribución 4.0 Internacional
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    Nombre:
    Arias-bp_2024.pdf
    Tamaño:
    8.182Mb
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