Your search keyword '"V. Montesinos-Cruz"' showing total 3 results

1. Effect of Heat Stress on the Expression of HSP70, UCP3 and CYP450 Genes in Liver; Longissimus Dorsi and Semitendinosus Muscle of Growing Pigs

Author

V. Montesinos-Cruz, M. Cervantes, M. Cota, L. Buenabad, and A. Morales

Subjects

0301 basic medicine, chemistry.chemical_classification, Reactive oxygen species, medicine.medical_specialty, General Veterinary, CYP3A, 010501 environmental sciences, medicine.disease, 01 natural sciences, Hsp70, 03 medical and health sciences, 030104 developmental biology, Endocrinology, chemistry, Internal medicine, Heat shock protein, medicine, Uncoupling protein, Animal Science and Zoology, Semitendinosus muscle, Cell damage, 0105 earth and related environmental sciences, UCP3

Abstract

High Ambient Temperature (AT) provokes Heat Stress (HS) in animals, which is characterized by increased body temperature, Reactive Oxygen Species (ROS) production and cell damage. Uncoupling Proteins (UCP) may contribute to dissipate body heat, cytochrome P450 (CYP3A4) reduces ROS and Heat Shock Proteins (HSP) prevent protein denaturalization. This study analyzed the expression of HSP70, UCP3 and CYP3A in liver, Longissimus Dorsi (LD) and Semitendinosus (ST) muscles of pigs exposed to HS conditions. A 21-d experiment was conducted with 18 pigs (32.6±3.2 kg body weight) divided into 3 treatments: (1) HS, pigs exposed to natural AT (29.5-37.2°C) fed ad libitum; (2) TNad, thermoneutral conditions (24.0±2.0°C) fed ad libitum; (3) TNpf, thermoneutral fed same amount as HS pigs. Hepatic expression of HSP70 in HS pigs was 4-fold higher than in TNad pigs (p=0.039); no differences were observed between HS and TNpf, or between TNad and TNpf pigs (p>0.10). There were no differences in HSP70 expression in both muscles (p>0.10) because of HS or feed intake. Expression of UCP3 in LD and ST did not differ (p>0.10) between treatments; neither the expression of CYP3A in liver was affected by HS, or feed intake level (p>0.10). Apparently, pigs became adapted to HS because expression of mitochondrial UCP3 and CYP3A was not affected after 21 d of HS exposure and the increased HSP70 expression in liver could have helped cells to maintain their proteins integrity.

Published

2019

2. Characterization of protein corona around of SiO2-PEG-Tf NP in human plasma and its influence in active targeting

Author

Claudia M. García-Cuellar, V. Escamilla-Rivera, A. Solorio-Rodríguez, M. Uribe-Ramírez, A. De Vizcaya-Ruiz, and V. Montesinos-Cruz

Subjects

0301 basic medicine, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Chromatography, Human plasma, Chemistry, 030220 oncology & carcinogenesis, PEG ratio, Protein Corona, General Medicine, Toxicology

Published

2016

3. Survival Mechanisms and Xenobiotic Susceptibility of Keratinocytes Exposed to Metal-Derived Nanoparticles.

Author

Montesinos-Cruz V, Rose J, Pappa A, Panayiotidis MI, De Vizcaya-Ruiz A, and Franco R

Subjects

Cell Proliferation drug effects, Cell Survival drug effects, Cells, Cultured, Cerium chemistry, Humans, Keratinocytes metabolism, Oxidative Stress drug effects, Particle Size, Silver chemistry, Surface Properties, Titanium chemistry, Xenobiotics metabolism, Cerium pharmacology, Keratinocytes drug effects, Nanoparticles chemistry, Silver pharmacology, Titanium pharmacology, Xenobiotics antagonists & inhibitors

Abstract

Metal-derived nanoparticles (Mt-NPs) are increasingly used in cosmetology due to their ultraviolet shielding (titanium dioxide [TiO 2 ]), antioxidant (cerium dioxide [CeO 2 ]), and biocidal (silver [Ag]) properties. In the absence of overt toxicity (i.e., cell death), Mt-NPs are considered safe for cosmetic applications. However, there is little understanding about the mechanisms involved in the survival of keratinocytes exposed to subtoxic levels of Mt-NPs. Human keratinocytes (HaCaT) were exposed subacutely to subtoxic concentrations (≤30 μg/mL, 48-72 h) of rutile (r) TiO 2 (cylindrical), CeO 2 (cubic) and Ag (spherical) with a core/hydrodynamic size of <50/<100 nm and >98% purity. Mt-NP uptake was indirectly quantified by changes in the light side scatter, where the kinetics (time/dose-response) suggested that the three types of Mt-NPs were similarly uptaken by keratinocytes. rTiO 2 and CeO 2 , but not Ag-NPs, increased autophagy, whose inhibition prompted cell death. No increase in the steady-state levels of reactive oxygen species (ROS) was induced by exposure to any of the Mt-NPs tested. Interestingly, intracellular Ag-NP aggregates observed an increased far-red autofluorescence (≥740 nm em), which has been ascribed to their binding to thiol molecules such as glutathione (GSH). Accordingly, inhibition of GSH synthesis, but not the impairment of oxidized GSH recycling, sensitized keratinocytes to Ag-NPs suggesting that GSH homeostasis, and its direct scavenging of Ag-NPs, but not ROS, is essential for keratinocyte survival upon exposure to Ag-NP. rTiO 2 and Ag, but not CeO 2 -NPs, compromised metabolic flux (glycolysis and respiration), but ATP levels were unaltered. Finally, we also observed that exposure to Mt-NPs sensitized keratinocytes to non-UV xenobiotic exposure (arsenite and paraquat). Our results demonstrate the differential contribution of autophagy and GSH homeostasis to the survival of human keratinocytes exposed to subtoxic concentrations of Mt-NPs and highlight the increased susceptibility of keratinocytes exposed to Mt-NPs to a second xenobiotic insult.

Published

2020