Your search keyword '"Edgar Yebrán Villegas-Vázquez"' showing total 5 results

1. The high methylation level of a novel 151-bp CpG island in the ESR1 gene promoter is associated with a poor breast cancer prognosis

Author

Laura Itzel Quintas-Granados, Hernán Cortés, Manuel González-Del Carmen, Gerardo Leyva-Gómez, Lilia Patricia Bustamante-Montes, Miguel Rodríguez-Morales, Edgar Yebran Villegas-Vazquez, Israel López-Reyes, Sofía Lizeth Alcaraz-Estrada, Jorge Sandoval-Basilio, Ernesto Soto-Reyes, Javad Sharifi-Rad, Gabriela Figueroa-González, and Octavio Daniel Reyes-Hernández

Subjects

Breast cancer, ESR1 methylation, Mexican women, Menopausal stage, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282, Cytology, QH573-671

Abstract

Abstract Background The ESR1 gene suffers methylation changes in many types of cancers, including breast cancer (BC), the most frequently diagnosed cancer in women that is also present in men. Methylation at promoter A of ESR1 is the worse prognosis in terms of overall survival; thus, the early detection, prognostic, and prediction of therapy involve some methylation biomarkers. Methods Therefore, our study aimed to examine the methylation levels at the ESR1 gene in samples from Mexican BC patients and its possible association with menopausal status. Results We identified a novel 151-bp CpG island in the promoter A of the ESR1 gene. Interestingly, methylation levels at this CpG island in positive ERα tumors were approximately 50% less than negative ERα or control samples. Furthermore, methylation levels at ESR1 were associated with menopausal status. In postmenopausal patients, the methylation levels were 1.5-fold higher than in premenopausal patients. Finally, according to tumor malignancy, triple-negative cancer subtypes had higher ESR1 methylation levels than luminal/HER2+ or luminal A subtypes. Conclusions Our findings suggest that methylation at this novel CpG island might be a promising prognosis marker

Published

2021

2. Unrevealing Lithium Repositioning in the Hallmarks of Cancer: Effects of Lithium Salts (LiCl and Li2CO3) in an In Vitro Cervical Cancer Model

Author

Juan Carlos García-Acosta, Alejando Israel Castillo-Montoya, Gareth Omar Rostro-Alonso, Edgar Yebrán Villegas-Vázquez, Laura Itzel Quintas-Granados, Luis Sánchez-Sánchez, Hugo López-Muñóz, Lizbeth Cariño-Calvo, Israel López-Reyes, Lilia Patricia Bustamante-Montes, Gerardo Leyva-Gómez, Hernán Cortés, Nadia Judith Jacobo-Herrera, Rosario García-Aguilar, Octavio Daniel Reyes-Hernández, and Gabriela Figueroa-González

Subjects

lithium chloride, lithium carbonate, cervical cancer cells, apoptosis induction, cell cycle arrest, migration inhibition, Organic chemistry, QD241-441

Abstract

Lithium, a natural element, has been employed as a mental stabilizer in psychiatric treatments; however, some reports indicate it has an anticancer effect, prompting the consideration of repurposing lithium for cancer treatment. The potential anticancer use of lithium may depend on its form (salt type) and the type of cancer cells targeted. Little is known about the effects of Li2CO3 or LiCl on cancer cells, so we focused on exploring their effects on proliferation, apoptosis, migration, and cell cycle as part of the hallmarks of cancer. Firstly, we established the IC50 values on HeLa, SiHa, and HaCaT cells with LiCl and Li2CO3 and determined by crystal violet that cell proliferation was time-dependent in the three cell lines (IC50 values for LiCl were 23.43 mM for SiHa, 23.14 mM for HeLa, and 15.10 mM for HaCaT cells, while the IC50 values for Li2CO3 were 20.57 mM for SiHa, 11.52 mM for HeLa, and 10.52 mM for HaCaT cells.) Our findings indicate that Li2CO3 and LiCl induce DNA fragmentation and caspase-independent apoptosis, as shown by TUNEL, Western Blot, and Annexin V/IP assay by flow cytometry. Also, cell cycle analysis showed that LiCl and Li2CO3 arrested the cervical cancer cells at the G1 phase. Moreover, lithium salts displayed an anti-migratory effect on the three cell lines observed by the wound-healing assay. All these findings imply the viable anticancer effect of lithium salts by targeting several of the hallmarks of cancer.

Published

2024

3. Lithium: A Promising Anticancer Agent

Author

Edgar Yebrán Villegas-Vázquez, Laura Itzel Quintas-Granados, Hernán Cortés, Manuel González-Del Carmen, Gerardo Leyva-Gómez, Miguel Rodríguez-Morales, Lilia Patricia Bustamante-Montes, Daniela Silva-Adaya, Carlos Pérez-Plasencia, Nadia Jacobo-Herrera, Octavio Daniel Reyes-Hernández, and Gabriela Figueroa-González

Subjects

lithium, cancer, apoptosis, autophagy, anti-cancer effects, nano-delivery, Science

Abstract

Lithium is a therapeutic cation used to treat bipolar disorders but also has some important features as an anti-cancer agent. In this review, we provide a general overview of lithium, from its transport into cells, to its innovative administration forms, and based on genomic, transcriptomic, and proteomic data. Lithium formulations such as lithium acetoacetate (LiAcAc), lithium chloride (LiCl), lithium citrate (Li3C6H5O7), and lithium carbonate (Li2CO3) induce apoptosis, autophagy, and inhibition of tumor growth and also participate in the regulation of tumor proliferation, tumor invasion, and metastasis and cell cycle arrest. Moreover, lithium is synergistic with standard cancer therapies, enhancing their anti-tumor effects. In addition, lithium has a neuroprotective role in cancer patients, by improving their quality of life. Interestingly, nano-sized lithium enhances its anti-tumor activities and protects vital organs from the damage caused by lipid peroxidation during tumor development. However, these potential therapeutic activities of lithium depend on various factors, such as the nature and aggressiveness of the tumor, the type of lithium salt, and its form of administration and dosage. Since lithium has been used to treat bipolar disorder, the current study provides an overview of its role in medicine and how this has changed. This review also highlights the importance of this repurposed drug, which appears to have therapeutic cancer potential, and underlines its molecular mechanisms.

Published

2023

4. Cacalol Acetate as Anticancer Agent: Antiproliferative, Pro-Apoptotic, Cytostatic, and Anti-Migratory Effects

Author

Gareth Omar Rostro-Alonso, Alejandro Israel Castillo-Montoya, Juan Carlos García-Acosta, Erick Fernando Aguilar-Llanos, Laura Itzel Quintas-Granados, Edgar Yebrán Villegas-Vazquez, Rosario García-Aguilar, Samantha Andrea Porras-Vázquez, Lilia Patricia Bustamante-Montes, Jesús J. Alvarado-Sansininea, Manuel Jiménez-Estrada, Lizbeth Cariño-Calvo, Manuel González-del Carmen, Hernán Cortés, Gerardo Leyva-Gómez, Gabriela Figueroa-González, and Octavio Daniel Reyes-Hernández

Subjects

cacalol, cacalol acetate, antiproliferation, apoptotic effect, cervical cancer cells, Biology (General), QH301-705.5

Abstract

Cacalol (C), a sesquiterpene isolated from Psacalium decompositum, has demonstrated anti-inflammatory and antioxidant activities. Its cytotoxic, antiproliferative, and pro-apoptotic effects have been previously shown in an in vitro breast cancer model. A derivative, cacalol acetate (CA), shows potential in regulating these processes, which has not been previously reported. This study focused on an in vitro cervical cancer model, assessing CA’s antiproliferative, pro-apoptotic, cytostatic, and anti-migratory activities using the HeLa cell line. The natural anticancer agent indole-3-carbinol (I3C) was used as a control for comparison. CA demonstrated significant antitumor activities, including inhibiting cell growth, inducing apoptosis, arresting cells in the G2 phase of the cell cycle, and inhibiting cell migration. These effects were notably greater compared to I3C. I3C, while following a similar trend, did not induce Cas-3 expression, suggesting a different apoptotic pathway. Neither CA nor I3C increased p62 and LC3B levels, indicating they do not stimulate autophagy marker expression. Both compounds inhibited HeLa cell migration and induced cell cycle arrest. Despite both holding promise as anticancer agents for cervical cancer, CA’s lower cytotoxicity and stronger regulation of tumor phenotypes make it a more promising agent compared to I3C.

Published

2024

5. An Ancestry Perspective of the Evolution of PBS1 Proteins in Plants

Author

Roberto Ruiz-Medrano, Edgar Yebrán Villegas-Vázquez, and Beatriz Xoconostle-Cázares

Subjects

0106 biological sciences, 0301 basic medicine, Hypersensitive response, Ancestral reconstruction, Models, Molecular, Lineage (genetic), QH301-705.5, Protein Conformation, Embryophyte, Protein Serine-Threonine Kinases, 01 natural sciences, Catalysis, Article, PBS1, Inorganic Chemistry, 03 medical and health sciences, Structure-Activity Relationship, Gene Expression Regulation, Plant, Arabidopsis, evolution, Pseudomonas syringae, Amino Acid Sequence, cleavage site motif, Physical and Theoretical Chemistry, Biology (General), Molecular Biology, Peptide sequence, QD1-999, Spectroscopy, Conserved Sequence, Phylogeny, Plant Physiological Phenomena, Plant Proteins, Genetics, biology, Phylogenetic tree, Organic Chemistry, General Medicine, Plants, biology.organism_classification, Biological Evolution, Computer Science Applications, Chemistry, RPS5, 030104 developmental biology, resistance recognition motif, 010606 plant biology & botany, Signal Transduction

Abstract

The AVRPPHB SUSCEPTIBLE1 (PBS1) and RESISTANCE TO PSEUDOMONAS SYRINGAE 5 (RPS5) proteins are involved in signal transduction to evoke innate plant immune response. In Arabidopsis, PBS1 is cleaved by the AvrPphB (Pseudomonas phaseolicola Avirulence protein B) protease, activating RPS5 and turning in a hypersensitive response (HR). We searched for PBS1 orthologs to trace their origin and evolution. PBS1 orthologs were found in embryophytes and in other plant taxa but with lower similarity. PBS1 phylogenetic analysis indicates high divergence, suggesting that the decoy function described for Arabidopsis PBS1 might be associated with a small fraction of orthologs. Ancestral reconstruction analysis suggests an elevated diversity in the amino acid sequence within the described motifs. All the orthologs contain the conserved PBS1 kinase subdomains, whereas the cleavage motif is present in several embryophyte orthologs but absent in most other taxa. The putative resistance recognition motifs in PBS1 orthologs are highly diverse. PBS1 cleavage site motif is exposed in some 3D structure predictions, whereas it is not in others, suggesting different modes of regulation and functions in PBS1 orthologs. Our findings suggest that PBS1 originated in the lineage that gave rise to embryophytes, with the angiosperm sequences forming a separate clade from pteridophyte proteins.

Published

2021