Publications by authors named "A Blasco Alberto"

Background: The effective use of combination antiretroviral therapy (ART) has significantly improved the life expectancy of people living with the human immunodeficiency virus (HIV). However, complications have shifted from opportunistic infections to issues such as drug toxicity and resistance, as well as an increase in premature cardiovascular diseases (CVD). These conditions are attributed to chronic immune activation and persistent inflammation caused by HIV, along with lipid abnormalities and insulin resistance.

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  • * Mice lacking specific circadian receptors (REV-ERBα/β) show increased obesity risk and liver fat when their clocks are disrupted, but pairing their peripheral liver clocks with central ones can help reverse these issues.
  • * The research suggests that keeping the internal clocks of different body parts synchronized, rather than just aligning them with external light cues, might be key to treating metabolic problems linked to circadian cycle disruptions.
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Circadian desynchrony induced by shiftwork or jet lag is detrimental to metabolic health, but how synchronous or desynchronous signals are transmitted among tissues is unknown. We report that liver molecular clock dysfunction is signaled to the brain through the hepatic vagal afferent nerve (HVAN), leading to altered food intake patterns that are corrected by ablation of the HVAN. Hepatic branch vagotomy also prevents food intake disruptions induced by high-fat diet feeding and reduces body weight gain.

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  • Very high-power short-duration (vHPSD) radiofrequency ablation for pulmonary vein isolation shows reduced ablation times and better patient tolerance compared to traditional methods.
  • In a study of 58 patients undergoing vHPSD, results indicated significantly shorter procedural and RF times, along with reduced need for anesthetic drugs compared to a control group.
  • The vHPSD method allowed for effective PV isolation under mild conscious sedation, with a notably lower pain experience reported by patients.
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P2X7 is an ATP-activated purinergic receptor implicated in pro-inflammatory responses. It is associated with the development of several diseases, including inflammatory and neurodegenerative conditions. Although several P2X7 receptor antagonists have recently been reported in the literature, none of them is approved for clinical use.

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