Publications by authors named "Leon Bae"

G Protein-Coupled Receptors (GPCRs) represent the largest superfamily of cell-surface proteins. However, the expression and function of majority of GPCRs remain unexplored in breast cancer (BC). We interrogated the expression and phosphorylation status of 398 non-sensory GPCRs using the landmark BC proteogenomics and phosphoproteomic dataset from The Cancer Genome Atlas.

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Article Synopsis
  • Patients with severe thermal injuries are at risk for infections that hinder recovery and can lead to sepsis, partly due to reduced dendritic cells (DCs) in their immune response.
  • Treatment with the DC growth factor Fms-like tyrosine kinase-3 ligand (FL) boosts both conventional DCs (cDCs) and plasmacytoid DCs (pDCs), improving immune response and survival after burn injuries in a mouse model.
  • The study finds that while both DC types play important roles, pDCs specifically are crucial for FL's benefits, although they do not directly affect neutrophil migration, which is primarily influenced by cDCs.
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Adequate wound healing is vital for burn patients to reduce the risk of infections and prolonged hospitalization. Dendritic cells (DCs) are antigen presenting cells that release cytokines and are central for the activation of innate and acquired immune responses. Studies have showed their presence in human burn wounds; however, their role in burn wound healing remains to be determined.

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Previous work has shown that the essential R210 of subunit a in the Escherichia coli ATP synthase can be switched with a conserved glutamine Q252 with retention of a moderate level of function, that a third mutation P204T enhances this function, and that the arginine Q252R can be replaced by lysine without total loss of activity. In this study, the roles of P204T and R210Q were examined. It was concluded that the threonine in P204T is not directly involved in function since its replacement by alanine did not significantly affect growth properties.

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