Publications by authors named "J D Bartleson"

Microgravity is associated with immunological dysfunction, though the mechanisms are poorly understood. Here, using single-cell analysis of human peripheral blood mononuclear cells (PBMCs) exposed to short term (25 hours) simulated microgravity, we characterize altered genes and pathways at basal and stimulated states with a Toll-like Receptor-7/8 agonist. We validate single-cell analysis by RNA sequencing and super-resolution microscopy, and against data from the Inspiration-4 (I4) mission, JAXA (Cell-Free Epigenome) mission, Twins study, and spleens from mice on the International Space Station.

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Article Synopsis
  • The immune system has the potential to control cancer, but the role of certain immune sensors in cancer aggressiveness, specifically NLRC4, remains largely unexplored in humans.
  • This study found that decreased levels of NLRC4 in colorectal cancer (CRC) cells are linked to poorer immune cell infiltration and worse patient outcomes, indicating its importance in tumor progression.
  • Enhancing NLRC4 expression in CRC cells led to immune reprogramming that improved the function of immune cells, suggesting that targeting NLRC4 could provide a new approach to boosting antitumor responses in various types of carcinoma.
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The mutualistic relationship of gut-resident microbiota and the host immune system promotes homeostasis that ensures maintenance of the microbial community and of a largely non-aggressive immune cell compartment. The consequences of disturbing this balance include proximal inflammatory conditions, such as Crohn's disease, and systemic illnesses. This equilibrium is achieved in part through the induction of both effector and suppressor arms of the adaptive immune system.

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Immune responses are governed by signals from the tissue microenvironment, and in addition to biochemical signals, mechanical cues and forces arising from the tissue, its extracellular matrix and its constituent cells shape immune cell function. Indeed, changes in biophysical properties of tissue alter the mechanical signals experienced by cells in many disease conditions, in inflammatory states and in the context of ageing. These mechanical cues are converted into biochemical signals through the process of mechanotransduction, and multiple pathways of mechanotransduction have been identified in immune cells.

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