Even though this is for cardiac induced ischemia our competent? researchers should evaluate this for possible use in saving neurons post stroke. But that won't occur; THERE IS NO LEADERSHIP IN STROKE. Everything in stroke is a complete fucking failure!
TREM1-Mediated Neuroinflammation Is Critical to Global Ischemia-Induced Neurodegeneration and Cognitive Deficits
By
RACHAEL URQUHART
___________________________________
A DISSERTATION
Submitted to the faculty of the Graduate School of the Creighton University in
Partial Fulfillment of the Requirements for the degree of Doctor of Philosophy in
the Department of Pharmacology and Neuroscience
________________________
Abstract
Global cerebral ischemia occurs when blood flow to the entire brain is
significantly reduced; this occurs most commonly following cardiac arrest. Following
global ischemia, there is delayed and selective loss of neurons in the hippocampal
CA1, a critical brain region for learning and memory, ultimately leading to cognitive
impairments. While therapies for cardiac arrest primarily focus on restoring blood flow
and cardiac function, there are currently no effective treatments that address the global
ischemia-induced neurological deficits. Understanding the molecular mechanisms
underlying the pathophysiology of global ischemia is therefore critical for identifying
novel therapeutic targets and developing interventions to mitigate these devastating
outcomes.
Although the mechanisms underlying the global ischemia pathology are not yet
fully understood, it is established that the significant delay between insult and neuronal
death is consistent with a role for transcriptional changes. In this study, to determine
how dysregulation of genes contributes to global ischemia pathology, we performed
RNA sequencing on hippocampal CA1 from rats subjected to global ischemia via 4-
vessel occlusion. RNA-seq and Ingenuity Pathway analysis determined that, following
global ischemia, genes related to neuroinflammation, and the triggering receptor
expressed on myeloid cells-1 (TREM1) signaling are significantly upregulated in the
hippocampal CA1. TREM1 is a pivotal myeloid-derived immune cell surface receptor
with known roles in systemic inflammatory conditions, including myocardial ischemia
and sepsis. In recent years, TREM1 has been implicated in neurological conditions,
suggesting a role for neuroinflammation in the pathology of neurological disorders and
iv
diseases. To date, there are no known studies that have explored the connection
between TREM1-mediated neuroinflammation and global ischemia pathology.
Here we show global ischemia induces upregulation of TREM1 and related
inflammatory cytokines and further increases microglial activation, astrogliosis, and
loss of blood-brain barrier structure and function. In contrast, TREM1 inhibition via
inhibitory decoy receptor peptide LR12, recuses these events indicating that TREM1
plays a critical role in global ischemia-induced neuroinflammation. Moreover,
administration of LR12 decreases neurodegeneration and attenuates cognitive deficits
associated with global ischemia. This is the first study to establish a causal relationship
between TREM1-mediated neuroinflammation and global ischemia pathology,
suggesting TREM1 as a potential therapeutic target for treating global ischemia-
induced neurodegeneration and cognitive deficits.
In the first chapter of this dissertation, I provide an overview and background
on global cerebral ischemia, neuroinflammation, and the TREM1 signaling pathway,
and discuss recent studies related to these topics. In the second chapter, I present
and interpret the data, analyses, and findings, followed by a discussion of the
conclusions and potential directions for future research.
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