Cytotoxicity-related lipidomic changes induced in double-hit Diffuse Large B-Cell Lymphoma after treatment with statins in vitro

dc.audience.educationlevelInvestigadores/Researcherses_MX
dc.contributor.advisorHernández Hernández, José Ascención
dc.contributor.authorPherez Farah, Alfredo
dc.contributor.catalogerdnbsrpes_MX
dc.contributor.committeememberOrtiz López, Rocío
dc.contributor.committeememberMéndez Reguera, Elsa Aniela
dc.contributor.committeememberVillela Martínez, Luis Mario
dc.contributor.departmentEscuela de Medicina y Ciencias de la Saludes_MX
dc.contributor.institutionCampus Monterreyes_MX
dc.contributor.mentorLópez Sánchez, Rosa del Carmen
dc.date.accepted2022-05-30
dc.date.accessioned2023-07-14T15:17:52Z
dc.date.available2023-07-14T15:17:52Z
dc.date.issued2022-05-31
dc.description.abstractDiffuse Large B-Cell Lymphoma (DLBCL) is the most common hematologic malignancy in the world and one of the deadliest. Since the introduction of anti-CD20 blocking antibodies prognosis has dramatically improved; however, over 40% of cases are resistant or recur after an initial remission. These outcomes largely depend on its underlying genomics, which makes it difficult to approach because it is also one of the most genetically diverse neoplasms. Therefore, research beyond its already extensively described molecular biology is necessary. Metabolic reprogramming at the lipid level is one of the least understood hallmarks of cancer, but its relevance is becoming increasingly evident because it accurately depicts cellular phenotype and because of the bioactive nature of many lipid species such as sphingosine and ceramide. Statins are widely prescribed drugs. Although they are classically used as cholesterol lowering medications, they are incredibly pleiotropic agents and are known to have antilymphomagenic properties. However, the underlying mechanisms leading to these effects are still unclear. In this work, it was hypothesized that statins induce a metabolic shift that promotes the accumulation of cytotoxic lipids, triggering cell death. To approach this, an aggressive lymphoma cell line was treated with different combinations of statin-containing therapeutic regimens. Cell cycle was assessed with flow cytometry, and several lipid species were quantified through mass spectrometry. Our data suggests that atorvastatin synergizes with R-CHOP to produce G1/S cell cycle arrest, and that this effect might be partially driven by sphingosine. This is the first work to evaluate the sphingolipidomic effect of statins in the cancer context and gives rise to clinical research that could lead to novel biomarkers and drug repurposing.es_MX
dc.description.degreeMaestro en Ciencias en Ciencias Biomédicases_MX
dc.format.mediumTextoes_MX
dc.identificator2es_MX
dc.identificator3es_MX
dc.identifier.citationPherez Farah, A (2022). Cytotoxicity-related lipidomic changes induced in double-hit Diffuse Large B-Cell Lymphoma after treatment with statins in vitro. [Master Thesis, Tecnológico de Monterrey]. Tecnológico de Monterrey Repositoryes_MX
dc.identifier.orcidhttps://orcid.org/0000-0003-2213-3405es_MX
dc.identifier.urihttps://hdl.handle.net/11285/651030
dc.language.isoenges_MX
dc.publisherInstituto Tecnológico y de Estudios Superiores de Monterreyes_MX
dc.relation.isFormatOfpublishedVersiones_MX
dc.rightsopenAccesses_MX
dc.rights.urihttp://creativecommons.org/licenses/by/4.0es_MX
dc.subject.classificationBIOLOGÍA Y QUÍMICAes_MX
dc.subject.classificationMEDICINA Y CIENCIAS DE LA SALUDes_MX
dc.subject.keywordLymphomaes_MX
dc.subject.keywordSphingolipidses_MX
dc.subject.keywordMetabolomicses_MX
dc.subject.lcshMedicinees_MX
dc.titleCytotoxicity-related lipidomic changes induced in double-hit Diffuse Large B-Cell Lymphoma after treatment with statins in vitroes_MX
dc.typeTesis de maestría

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