Your search keyword '"Gyurina, Katalin"' showing total 3 results

1. Adipose Tissue Macrophages of the Human Fetus.

Author

Radványi, Ádám, Gyurina, Katalin, Rácz, Emese, Kovács, Ilona, Méhes, Gábor, and Röszer, Tamás

Subjects

*ADIPOSE tissues, *FETAL tissues, *CHILDHOOD obesity, *INSULIN resistance, *AUTOMATED teller machines

Abstract

Prenatal adipose tissue development affects body composition and growth trajectory in early infancy, therefore it is a key determinant of adiposity in childhood. Childhood overweight and obesity increase the probability of being obese as an adult. After birth and in adulthood, adipose tissue macrophages (ATMs) are relevant constituents of the fat depots, and they are necessary for physiological adipose tissue development and fat metabolism. In obesity, however, ATMs may induce chronic inflammation leading to insulin resistance, pancreatic beta cell damage and self-immunity. Despite being relevant regulators of adipose tissue development and functioning, it is unknown whether ATMs are present in the fetal adipose tissue, therefore it is elusive whether they may affect the prenatal establishment of fat depots. Here we studied the distribution of ATMs in the human fetus between gestational weeks 17 and 38 and labeled ATMs in the early postnatal life. We found that CD45+/CD14+/CD68+ ATMs infiltrated the fetal adipose tissue from the 17th week of gestation and remained persistent throughout the second and third trimesters. ATMs were phagocytic in the neonate and expressed interleukin-6, along with other pro-inflammatory gene products. These findings show that ATMs colonize the adipose tissue early in gestation, raising the possibility that intrauterine ATM–adipocyte communication may exist, eventually allowing ATMs to affect prenatal adipose tissue development. [ABSTRACT FROM AUTHOR]

Published

2024

2. Loss of Uncoupling Protein 1 Expression in the Subcutaneous Adipose Tissue Predicts Childhood Obesity.

Author

Gyurina, Katalin, Yarmak, Mariia, Sasi-Szabó, László, Molnár, Sarolta, Méhes, Gábor, and Röszer, Tamás

Subjects

*ADIPOSE tissues, *UNCOUPLING proteins, *CHILDHOOD obesity, *WEIGHT loss, *PROTEIN expression, *BODY mass index, *BROWN adipose tissue, *FETUS

Abstract

Stimulation of thermogenesis by inducing uncoupling protein 1 (UCP1) expression in adipocytes is thought to promote weight loss by increasing energy expenditure, and it is postulated that the human newborn has thermogenic subcutaneous fat depots. However, it remains unclear whether a relevant number of UCP1-expressing (UCP1+) adipocytes exist in the early postnatal life. Here we studied the distribution of UCP1 and the expression of thermogenic genes in the subcutaneous adipose tissues of the human fetus, infant and child. We show that the deep layer of human fetal and neonatal subcutaneous fat, particularly the abdominal wall, is rich in UCP1+ adipocytes. These adipocytes develop in the late third trimester and persist throughout childhood, expressing a panel of genes linked to mitochondrial biogenesis and thermogenesis. During the early childhood adiposity rebound—a critical phase that determines obesity risk later in life—the absence of adipose tissue UCP1 expression in children with normal body mass index (BMI) correlates with an obesity-associated gene expression signature. Finally, UCP1 expression is negatively correlated with BMI z-score and adipocyte size in infants and children. Overall, our results show that the absence of UCP1 expression in adipose tissue is an early indicator of adipose tissue expansion in children. [ABSTRACT FROM AUTHOR]

Published

2023

3. Stimulator of Interferon Genes (STING) Triggers Adipocyte Autophagy.

Author

Varga, Kornél Z., Gyurina, Katalin, Radványi, Ádám, Pál, Tibor, Sasi-Szabó, László, Yu, Haidong, Felszeghy, Enikő, Szabó, Tamás, and Röszer, Tamás

Subjects

*FAT cells, *ADIPOGENESIS, *INTERFERON receptors, *ADIPOSE tissues, *INTERFERONS, *MITOCHONDRIAL DNA, *AUTOPHAGY, *TYPE I interferons

Abstract

Innate immune signaling in adipocytes affects systemic metabolism. Cytosolic nucleic acid sensing has been recently shown to stimulate thermogenic adipocyte differentiation and protect from obesity; however, DNA efflux from adipocyte mitochondria is a potential proinflammatory signal that causes adipose tissue dysfunction and insulin resistance. Cytosolic DNA activates the stimulator of interferon response genes (STING), a key signal transducer which triggers type I interferon (IFN-I) expression; hence, STING activation is expected to induce IFN-I response and adipocyte dysfunction. However, we show herein that mouse adipocytes had a diminished IFN-I response to STING stimulation by 2′3′-cyclic-GMP-AMP (cGAMP). We also show that cGAMP triggered autophagy in murine and human adipocytes. In turn, STING inhibition reduced autophagosome number, compromised the mitochondrial network and caused inflammation and fat accumulation in adipocytes. STING hence stimulates a process that removes damaged mitochondria, thereby protecting adipocytes from an excessive IFN-I response to mitochondrial DNA efflux. In summary, STING appears to limit inflammation in adipocytes by promoting mitophagy under non-obesogenic conditions. [ABSTRACT FROM AUTHOR]

Published

2023