Publications by authors named "D Loane"

Traumatic brain injury (TBI) is a global health problem affecting millions of individuals annually, potentially resulting in persistent neuropathology, chronic neurological deficits, and death. However, TBI not only affects neural tissue, but also affects the peripheral immune system's homeostasis and physiology. TBI disrupts the balanced signaling between the brain and the peripheral organs, resulting in immunodysregulation and increasing infection susceptibility.

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Rodent models are important research tools for studying the pathophysiology of traumatic brain injury (TBI) and developing new therapeutic interventions for this devastating neurological disorder. However, the failure rate for the translation of drugs from animal testing to human treatments for TBI is 100%. While there are several potential explanations for this, previous clinical trials have relied on extrapolation from preclinical studies for critical design considerations, including drug dose optimization, post-injury drug treatment initiation and duration.

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Article Synopsis
  • - The study explores the complex pathophysiology and outcomes of Traumatic Brain Injury (TBI), highlighting that current classifications do not adequately reflect the underlying biological processes involved.
  • - Using advanced proteomic techniques, researchers analyzed plasma samples from 88 participants to identify 16 proteins with significant expression differences in TBI patients compared to non-injured controls, focusing on various markers related to neurons, astrocytes, and inflammation.
  • - Their findings indicated correlations between specific plasma proteins and brain injury measures, suggesting that certain biomarkers like UCH-L1 and total tau could serve as potential indicators for TBI severity and progression.
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Background: It is well established that traumatic brain injury (TBI) causes acute and chronic alterations in systemic immune function and that systemic immune changes contribute to posttraumatic neuroinflammation and neurodegeneration. However, how TBI affects bone marrow (BM) hematopoietic stem/progenitor cells chronically and to what extent such changes may negatively impact innate immunity and neurological function has not been examined.

Methods: To further understand the role of BM cell derivatives on TBI outcome, we generated BM chimeric mice by transplanting BM from chronically injured or sham (i.

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