Your search keyword '"Rojas-García, A.E."' showing total 9 results

1. Transcriptional regulation of human paraoxonase 1 by PXR and GR in human hepatoma cells.

Author

Ponce-Ruiz, N., Rojas-García, A.E., Barrón-Vivanco, B.S., Elizondo, G., Bernal-Hernández, Y.Y., Mejía-García, A., and Medina-Díaz, I.M.

Subjects

*GENETIC transcription regulation, *PARAOXONASE, *HEPATOCELLULAR carcinoma, *TRETINOIN, *PEROXISOME proliferator-activated receptors, *CATALYST supports

Abstract

Human paraoxonase 1 (PON1) is A-esterase synthesized in the liver and secreted into the plasma, where it associates with HDL. PON1 acts as an antioxidant preventing lipid oxidation and detoxifies a wide range of substrates, including organophosphate compounds. The variability of PON1 (enzyme activity/serum levels) has been attributed to internal and external factors. However, the molecular mechanisms involved in the transcriptional regulation of PON1 have not been well-studied. The aim of this study was to evaluate and characterize the transcriptional activation of PON1 by nuclear receptors (NR) in human hepatoma cells. In silico analysis was performed on the promoter region of PON1 to determine the response elements of NR. Real-time PCR was used to evaluate the effect of specific NR ligands on the mRNA levels of genes regulated by NR and PON1. The results indicated that NR response elements had 95% homology to pregnenolone (PXR), glucocorticoids (GR), retinoic acid (RXR) and peroxisomes proliferator-activated receptor alpha (PPARα). Treatments with Dexamethasone (GR ligand), Rifampicin (PXR ligand) and TCDD (AhR ligand) increased the mRNA levels of PON1 at 24 and 48 h. We showed that the activation of GR by Dexamethasone results in PON1 gene induction accompanied by an increase in activity levels. In conclusion, these results demonstrate that GR regulates PON1 gene transcription through directly binding to NR response elements at − 95 to − 628 bp of the PON1 promoter. This study suggests new molecular mechanisms for the transcriptional regulation of PON1 through a process involving the activation of PXR. [ABSTRACT FROM AUTHOR]

Published

2015

2. PON1 lactonase activity and its association with cardiovascular disease.

Author

Murillo-González, F.E., Ponce-Ruiz, N., Rojas-García, A.E., Rothenberg, S.J., Bernal-Hernández, Y.Y., Cerda-Flores, R.M., Mackness, Mike, Barrón-Vivanco, B.S., González-Arias, C.A., Ponce-Gallegos, J., and Medina-Díaz, I.M.

Subjects

*CARDIOVASCULAR diseases risk factors, *CARDIOVASCULAR diseases, *GENETIC polymorphisms, *PARAOXONASE, *LOGISTIC regression analysis

Abstract

• Patients with CVD had lower activity of PON1 Lactonase (LACase) than control patients. • LACase activity might be a new potential biomarker in CVD. • LACase activity is not influenced by the genetic polymorphisms of PON1. Paraoxonase 1 (PON1) is important in the development of atherosclerosis, and it has become the subject of intensive research. Our aim was to evaluate the association of serum PON1 activity and polymorphisms with cardiovascular disease (CVD) using four different substrates. Activity of PON1-related to arylesterase (AREase and 4-CMPAse), paraoxonase (PONase), and lactonase (LACase), and polymorphisms (A-162G, T-108C, L55M, and Q192R) were evaluated in subjects with CVD, cardiovascular risk factor (CFR), and controls. An ordered logistic-regression analysis of PON1 phenotypes was performed in the CVD group with respect to the control group. Logistic-regression analysis showed that CC-108 genotype was associated with CRF and CVD. The CVD group had the lowest activities of PON1. The LACase might be a better biomarker for CVD (OR, 0.52; 95% CI, 0.44–0.61) followed by CMPAse (OR, 0.82; 95% CI, 0.77–0.86), AREase (OR, 0.98; 95% CI, 0.97–0.99) and PONase (OR, 0.99, 95% CI, 0.99–0.99). Logistic regression of PON1 phenotypes by haplotypes showed that LACase activity was not influenced by the polymorphisms and that it could be a new potential biomarker in the development of CVD. Larger scale longitudinal studies are required. [ABSTRACT FROM AUTHOR]

Published

2020

3. Transcriptional regulation of human Paraoxonase 1 by nuclear receptors.

Author

Ponce-Ruiz, N., Murillo-González, F.E., Rojas-García, A.E., Mackness, Mike, Bernal-Hernández, Y.Y., Barrón-Vivanco, B.S., González-Arias, C.A., and Medina-Díaz, I.M.

Subjects

*NUCLEAR receptors (Biochemistry), *PARAOXONASE, *CALCIUM-dependent protein kinase, *LACTONASE, *HIGH density lipoproteins

Abstract

Paraoxonase 1 (PON1) is a calcium-dependent lactonase synthesized primarily in the liver and secreted into the plasma, where it is associates with high density lipoproteins (HDL). PON1 acts as antioxidant preventing low-density lipoprotein (LDL) oxidation, a process considered critical in the initiation and progression of atherosclerosis. Additionally, PON1 hydrolyzes and detoxifies some toxic metabolites of organophosphorus compounds (OPs). Thus, PON1 activity and expression levels are important for determining susceptibility to OPs intoxication and risk of developing diseases related to inflammation and oxidative stress. Increasing evidence has demonstrated the modulation of PON1 expression by many factors is due to interaction with nuclear receptors (NRs). Here, we briefly review the studies in this area and discuss the role of nuclear receptors in the regulation of PON1 expression, as well as how understanding these mechanisms may allow us to manipulate PON1 levels to improve drug efficacy and treat disease. [ABSTRACT FROM AUTHOR]

Published

2017

4. PON1 status and homocysteine levels as potential biomarkers for cardiovascular disease.

Author

Ponce-Ruiz, N., Murillo-González, F.E., Rojas-García, A.E., Barrón-Vivanco, B.S., Bernal-Hernández, Y.Y., González-Arias, C.A., Ortega-Cervantes, L., Ponce-Gallegos, J., López-Guarnido, O., and Medina-Díaz, I.M.

Subjects

*CARDIOVASCULAR diseases, *HOMOCYSTEINE, *PARAOXONASE, *BIOMARKERS, *HYPERTENSION

Abstract

Cardiovascular disease (CVD) is the leading cause of death. The mainly risks factors for CVD are diabetes, hypertension and high levels of homocysteine (Hcys), among others. Paraoxonase 1 (PON1) has been proposed as an antiatherogenic target for its ability to hydrolyzing oxi-Low-Density-Lipoproteins (LDL) and Hcys-thiolactone. Thus, the aim of the present study was to evaluate the association of Hcys levels, and the activities and concentration of PON1, as well as vitamin B from the diet with a risk for CVD. A case-control study was carry out in patients with cardiovascular diseases (CVD), Arterial hypertension, but not CVD (AH), and in healthy controls (control group) from the Mexican Institute of Social Security. Lipid profile, intake of vitamin B, Hcys, serum amyloid A (SAA), PON1 concentration, and PON1 activities (Arylesterase activity (ARE), Lactonase activity (LAC), and CMPA activity (CMPA)) were evaluated. The CVD group had the highest concentration of Hcys and SAA than in the AH and control groups (p < 0.01). ARE, LAC, and CMPA activities and PON1 concentration were lowest in the CVD group. A positive-independent association between Hcys levels and CVD was found (OR = 2.09; 95% CI: 1.69–2.56) and this increase when it was adjusted by age, BMI, ApoA1, vitamin B intake, SAA, and PON1 (OR = 14.41; 95% CI: 1.75–118.71). LAC and CMPA, as well as PON1 concentration, were inversely associated with CVD. LAC activity, PON1 concentration, and Hcys levels might be good biomarkers for CVD and their association could be modified by the intake of vitamin B. • Patients with cardiovascular disease (CVD) had higher Hcys and SAA levels than controls. • Activities and concentration of PON1 were low in patients with CVD. • Hcys levels were associated with an increase in the OR of belonging to the CVD group. • LAC activity, PON1 concentration, and Hcys levels might be good biomarkers for CVD. [ABSTRACT FROM AUTHOR]

Published

2020

5. Cholinesterases activity and paraoxonase 1 Q192R polymorphism of workers exposed to pesticides.

Author

Molina-Pintor, I.B., Bernal-Hernández, Y.Y., Rojas-García, A.E., Medina-Díaz, I.M., Moreno, J.F. Herrera, Puentes, G.A. Álvarez, and Barrón-Vivanco, B.S.

Subjects

*CHOLINESTERASES, *PESTICIDE toxicology, *INDUSTRIAL toxicology, *GENETIC polymorphisms, *PARAOXONASE

Published

2016

6. Paraoxonase 1 and its relationship with pesticide biomarkers in indigenous Mexican farmworkers.

Author

Bernal-Hernández, Y.Y., Medina-Díaz, I.M., Barrón-Vivanco, B.S., Girón-Pérez, M.I., Quintanilla-Vega, B., Paredes-Céspedes, D.M., López-Martínez, G., and Rojas-García, A.E.

Subjects

*PARAOXONASE, *PESTICIDE toxicology, *DISEASES in agricultural laborers, *MEXICANS, *BIOMARKERS, *DISEASES

Published

2016

7. PON1 activity in patients with cardiovascular disease.

Author

Murillo-González, F.E., Ponce-Ruíz, N., Xotlanihua-Gervacio, M.C., Ponce-Gallegos, J., Rojas-García, A.E., Bernal-Hernández, Y.Y., Barrón-Vivanco, B.S., and Medina-Díaz, I.M.

Subjects

*CARDIOVASCULAR disease treatment, *HIGH density lipoproteins, *BIOCHEMICAL substrates, *PARAOXONASE, *BLOOD serum analysis, *BLOOD lipids

Published

2016

8. Paraoxonase 1 as biomarker of exposure and susceptibility to pesticide sprayers.

Author

Xotlanihua Gervacio, M.C., Molina Pintor, I.B., Benítez Trinidad, A.B., Bernal Hernandez, Y.Y., Barrón Vivanco, B.S., Medina Díaz, I.M., and Rojas García, A.E.

Subjects

*PARAOXONASE, *PESTICIDE toxicology, *BIOMARKERS, *MICROBIAL sensitivity tests, *GENETIC polymorphisms, *QUANTITATIVE research, *CROSS-sectional method

Published

2016

9. Chronic ischemic patients and paraoxonase activity.

Author

Ponce-Ruiz, N., Murillo-González, F.E., Ponce-Gallegos, J., Xotlanihua-Gervacio, M.C., Rojas-García, A.E., Barrón-Vivanco, B.S., Bernal-Hernández, Y.Y., González-Arias, C.A., and Medina-Díaz, I.M.

Subjects

*PARAOXONASE, *ISCHEMIA, *HIGH density lipoproteins, *AROMATIC compounds, *TOXICOLOGICAL chemistry, *PATIENTS

Published

2016