Publications by authors named "C Girardet"

The neural functions of adropin, a secreted peptide highly expressed in the brain, have not been investigated. In humans, adropin is highly expressed in astrocytes and peaks during critical postnatal periods of brain development. Gene enrichment analysis of transcripts correlating with adropin expression suggests processes relevant to aging-related neurodegenerative diseases that vary with age and dementia state, possibly indicating survivor bias.

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Article Synopsis
  • - The study investigates how environmental factors during the perinatal period affect adults born with intrauterine growth retardation (IUGR) and their risk for cardio-metabolic diseases using a mouse model.
  • - Researchers found that overfeeding IUGR mice during lactation led to obesity and insulin resistance by three months, while underfed mice stayed thin and insulin-sensitive, highlighting the impact of nutrition on metabolic health.
  • - Molecular changes in insulin signaling were identified in the adult mice, with specific epigenetic markers and a decrease in a particular microRNA potentially serving as early indicators of future metabolic issues, indicating their relevance in precision medicine strategies.
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African animal trypanosomosis are parasitic diseases caused by several protozoa of the genus , transmitted by hematophagous insects, essentially tsetse flies, but also, less frequently by Tabanidae and Stomoxidae. They are geolocated in a part of the continent and affect livestock animals and carnivores; dogs are especially sensitive to them. They do not seem to present a zoonotic risk.

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The micropeptide adropin encoded by the clock-controlled energy homeostasis-associated gene is implicated in the regulation of glucose metabolism. However, its links to rhythms of nutrient intake, energy balance, and metabolic control remain poorly defined. Using surveys of Gene Expression Omnibus data sets, we confirm that fasting suppresses liver adropin expression in lean C57BL/6J (B6) mice.

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More than 75% of breast cancers are estrogen receptor alpha (ERα) positive (ER+), and resistance to current hormone therapies occurs in one-third of ER+ patients. Tumor resistance is still ERα-dependent, but mutations usually confer constitutive activation to the hormone receptor, rendering ERα modulator drugs such as tamoxifen and aromatase inhibitors ineffective. Fulvestrant is a potent selective estrogen receptor degrader (SERD), which degrades the ERα receptor in drug-resistant tumors and has been approved for the treatment of hormone-receptor-positive metastatic breast cancer following antiestrogen therapy.

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