Publications by authors named "S E Shoelson"
Apoptotic cells are rapidly engulfed and removed by phagocytes after displaying cell surface eat-me signals. Among many phospholipids, only phosphatidylserine (PS) is known to act as an eat-me signal on apoptotic cells. Using unbiased proteomics, we identified externalized phosphatidylinositides (PIPs) as apoptotic eat-me signals recognized by CD14 phagocytes.
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- Oxytocin plays a key role in childbirth by stimulating uterine contractions, enabling lactation, and promoting maternal bonding behaviors, with mice lacking oxytocin or its receptor showing failure to nurture.
- This maternal behavior can be restored in some cases with oxytocin replacement, indicating that the hormone can enter the brain and influence behavior despite general restrictions on polypeptides crossing the blood-brain barrier.
- Research highlights that receptor for advanced glycation end-products (RAGE) on brain capillary cells is crucial for transporting oxytocin into the brain, and without RAGE, male mice exhibit issues with maternal bonding and increased hyperactivity, underscoring RAGE’s importance in oxytocin's parenting and social bonding effects.
NFκB Regulates Muscle Development and Mitochondrial Function.
J Gerontol A Biol Sci Med Sci
March 2020
Nuclear factor (NF)κB is a transcription factor that controls immune and inflammatory signaling pathways. In skeletal muscle, NFκB has been implicated in the regulation of metabolic processes and tissue mass, yet its affects on mitochondrial function in this tissue are unclear. To investigate the role of NFκB on mitochondrial function and its relationship with muscle mass across the life span, we study a mouse model with muscle-specific NFκB suppression (muscle-specific IκBα super-repressor [MISR] mice).
View Article and Find Full Text PDFOlder adults universally suffer from sarcopenia and approximately 60-70% are diabetic or prediabetic. Nonetheless, the mechanisms underlying these aging-related metabolic disorders are unknown. NFκB has been implicated in the pathogenesis of several aging-related pathologies including sarcopenia and type 2 diabetes and has been proposed as a target against them.
View Article and Find Full Text PDFTBC1D4 (also known as AS160) is a Rab·GTPase-activating protein (RabGAP) which functions in insulin signaling. TBC1D4 is critical for translocation of glucose transporter 4 (GLUT4), from an inactive, intracellular, vesicle-bound site to the plasma membrane, where it promotes glucose entry into cells. The TBC1D4 protein is structurally subdivided into two N-terminal phosphotyrosine-binding (PTB) domains, a C-terminal catalytic RabGAP domain, and a disordered segment in between containing potential Akt phosphorylation sites.
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