Georgina Martin scite author profile

Traumatic brain injury (TBI) increases Alzheimer’s disease (AD) risk and leads to the deposition of neurofibrillary tangles and amyloid deposits similar to those found in AD. Agonists of Liver X receptors (LXRs), which regulate the expression of many genes involved in lipid homeostasis and inflammation, improve cognition and reduce neuropathology in AD mice. One pathway by which LXR agonists exert their beneficial effects is through ATP-binding cassette transporter A1 (ABCA1)-mediated lipid transport onto apolipoprotein E (apoE). To test the therapeutic utility of this pathway for TBI, we subjected male wild-type (WT) and apoE−/− mice to mild repetitive traumatic brain injury (mrTBI) followed by treatment with vehicle or the LXR agonist GW3965 at 15 mg/kg/day. GW3965 treatment restored impaired novel object recognition memory in WT but not apoE−/− mice. GW3965 did not significantly enhance the spontaneous recovery of motor deficits observed in all groups. Total soluble Aβ40 and Aβ42 levels were significantly elevated in WT and apoE−/− mice after injury, a response that was suppressed by GW3965 in both genotypes. WT mice showed mild but significant axonal damage at 2 d post-mrTBI, which was suppressed by GW3965. In contrast, apoE−/− mice showed severe axonal damage from 2 to 14 d after mrTBI that was unresponsive to GW3965. Because our mrTBI model does not produce significant inflammation, the beneficial effects of GW3965 we observed are unlikely to be related to reduced inflammation. Rather, our results suggest that both apoE-dependent and apoE-independent pathways contribute to the ability of GW3965 to promote recovery from mrTBI.

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Respiratory Presentation of Pediatric Patients in the 2014 Enterovirus D68 Outbreak

Martin

Cook

et al. 2016

Canadian Respiratory Journal

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Background. In the fall of 2014, a North American outbreak of enterovirus D68 resulted in a significant number of pediatric hospital admissions for respiratory illness throughout North America. This study characterized the clinical presentation and risk factors for a severe clinical course in children admitted to British Columbia Children's Hospital during the 2014 outbreak. Methods. Retrospective chart review of patients with confirmed EV-D68 infection admitted to BCCH with respiratory symptoms in the fall of 2014. Past medical history, clinical presentation, management, and course in hospital was collected and analyzed using descriptive statistics. Comparison was made between those that did and did not require ICU admission to identify risk factors. Results. Thirty-four patients were included (median age 7.5 years). Fifty-three percent of children had a prior history of wheeze, 32% had other preexisting medical comorbidities, and 15% were previously healthy. Ten children (29%) were admitted to the pediatric intensive care unit. The presence of complex medical conditions (excluding wheezing) (P = 0.03) and copathogens was associated with PICU admission (P = 0.02). Conclusions. EV-D68 infection resulted in severe, prolonged presentations of asthma-like illness in the hospitalized pediatric population. Patients with a prior history of wheeze and preexisting medical comorbidities appear to be most severely affected, but the virus can also cause wheezing in previously well children.

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Diffuse Intracerebral Hemorrhage in an Infant With a Novel Homozygous Variant Leading to Severe Protein C Deficiency

Martin¹,

Thomas

Wei

et al. 2020

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Protein C is a circulating anticoagulant that inhibits factor Va and VIIIa and promotes fibrinolysis. Compound heterozygous or homozygous variants in the Protein C gene (PROC) lead to severe deficiency of protein C and affected neonates typically present shortly after birth with purpura fulminans. We describe an infant who suffered a diffuse intracranial hemorrhage as a neonate and presented with purpura fulminans as an older infant which led to investigations that were consistent with severe protein C deficiency. We demonstrate subacute findings on neuroimaging and suggest this condition should be considered with neonatal presentations of bilateral intraparenchymal hemorrhage.

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HB Extremadura or α₂β₂133(H11)VAU→LEU, A New Mildly Unstable Hemoglobin in a Spanish Female

Villegas

Martin²,

Wilson

et al. 1989

Hemoglobin

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P4‐218: The liver X receptor agonist GW3965 improves cognitive deficits, reduces beta‐amyloid elevation and suppresses neuronal damage following mild repetitive closed head injury in mice

Namjoshi

Martin

Donkin

et al. 2012

Alzheimer's & Dementia

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Georgina Martin

The Liver X Receptor Agonist GW3965 Improves Recovery from Mild Repetitive Traumatic Brain Injury in Mice Partly through Apolipoprotein E

Respiratory Presentation of Pediatric Patients in the 2014 Enterovirus D68 Outbreak

Diffuse Intracerebral Hemorrhage in an Infant With a Novel Homozygous Variant Leading to Severe Protein C Deficiency

HB Extremadura or α₂β₂133(H11)VAU→LEU, A New Mildly Unstable Hemoglobin in a Spanish Female

P4‐218: The liver X receptor agonist GW3965 improves cognitive deficits, reduces beta‐amyloid elevation and suppresses neuronal damage following mild repetitive closed head injury in mice

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Georgina Martin

The Liver X Receptor Agonist GW3965 Improves Recovery from Mild Repetitive Traumatic Brain Injury in Mice Partly through Apolipoprotein E

Respiratory Presentation of Pediatric Patients in the 2014 Enterovirus D68 Outbreak

Diffuse Intracerebral Hemorrhage in an Infant With a Novel Homozygous Variant Leading to Severe Protein C Deficiency

HB Extremadura or α2β2133(H11)VAU→LEU, A New Mildly Unstable Hemoglobin in a Spanish Female

P4‐218: The liver X receptor agonist GW3965 improves cognitive deficits, reduces beta‐amyloid elevation and suppresses neuronal damage following mild repetitive closed head injury in mice

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Product

Resources

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HB Extremadura or α₂β₂133(H11)VAU→LEU, A New Mildly Unstable Hemoglobin in a Spanish Female