Improving Skin Wound Healing Using Functional Electrospun Wound Dressings and 3D Printed Tissue Engineering Constructs

Nun, Nicholas

12 April 2021

No description available.

Animals

Biochemistry

Biomedical Engineering

Biomedical Research

Chemistry

Experiments

Histology

Materials Science

Microbiology

Molecules

Organic Chemistry

Plastics

Polymer Chemistry

Polymers

wound healing

electrospinning

wound dressing

3d printing

tissue engineering

antimicrobial

peptide conjugation

quantitative histology

polyester

in vivo

animal model

infection model

bioplotting

acute wound rat model

infected wound mouse model

Caractéristiques cardiométaboliques d’une souris inactivée pour le cotransporteur potassium-chlorure de type 3

Garneau, Alexandre

11 1900

La polyneuropathie sensitivomotrice héréditaire (PNSMH) est une maladie rare qui entraîne un ralentissement du développement moteur et mental, une déficience sensitivomotrice et des syndromes neuropsychiatriques, et qui s’accompagne souvent d’une agénésie du corps calleux. Par ailleurs, plusieurs évaluations rapportent une petite stature ou une masse corporelle anormalement basse chez les patients. La PNSMH est causée par des mutations perte de fonction du cotransporteur K⁺-Cl⁻ de type 3 (KCC3). Des évaluations cliniques détaillées et la caractérisation de souris inactivées pour Kcc3 (Kcc3ᴷᴼ) ont permis d’établir qu’un défaut d’export K⁺-Cl⁻ cause les atteintes neurologiques anatomiques et fonctionnelles dans la maladie. Chez les souris Kcc3ᴷᴼ, des manifestations extraneurologiques ont également été relevées : masse corporelle réduite, pression artérielle (PA) élevée, polydipsie et polyurie. Puisque la physiopathologie des désordres extraneurologiques découlant de la perte de fonction de KCC3 reste incomplètement décrite, mes travaux avaient pour objectif d’en comprendre les mécanismes sous-jacents en utilisant un modèle Kcc3ᴷᴼ. Une caractérisation initiale de notre lignée de souris Kcc3ᴷᴼ constitutive et systémique a montré des anomalies vasculaires et cardiaques accompagnant une élévation de PA diastolique. Cette lignée affichait également une polydipsie et une polyurie isoosmotique, de même qu’une réduction de masse corporelle et d’adiposité sans réduction d’apport alimentaire. Une caractérisation métabolique détaillée de notre modèle a ensuite permis de révéler des réductions de masse grasse et de masse maigre. Cette minceur résulte sûrement en partie des augmentations d’activité locomotrice et de dépense énergétique mesurées. Une nette amélioration de la tolérance au glucose a aussi été trouvée, ainsi que des concentrations réduites de triacylglycérols plasmatiques. Enfin, nous avons noté que notre modèle est résistant à l’obésité induite par une diète hyperlipidique et affiche une élévation concomitante de l’expression d’enzymes lipogéniques et lipolytiques dans le gras viscéral, engendrant potentiellement une dissipation calorique. En revisitant la fonction cardiovasculaire dans notre modèle par des méthodes de pointe, nous n’avons pas observé de changement de PA ni de différence de réactivité artériolaire en conditions basales, mais nous avons noté une élévation de distensibilité artériolaire passive. Chez notre modèle, nous n’avons pas non plus remarqué de sensibilité particulière de la PA au sel alimentaire, mais une excrétion urinaire fortement accrue de solutés sous diète hypersodée ainsi qu’une préférence marquée pour le sel. Ces observations sont compatibles avec un défaut de réabsorption hydrosodée par le rein pouvant d’ailleurs prévenir les élévations de PA. En somme, nos travaux ont permis de mieux comprendre les atteintes cardiométaboliques qui accompagnent le tableau neurologique d’un modèle murin de PNSMH. Nous avons notamment relevé des bénéfices inattendus dans le métabolisme glucidique et lipidique suivant l’inactivation de Kcc3. Nous soupçonnons également que l’absence de KCC3 dans le rein engendre une fuite ionique urinaire s’accentuant sous diète hypersodée et pouvant influencer la PA en limitant l’expansion volémique. Nos observations d’anomalies pléiotropiques liées à l’inactivation de Kcc3 font de ce gène une nouvelle cible pharmacologique potentielle et justifient la nécessité d’étudier l’anatomophysiologie cardiométabolique des patients atteints de PNSMH de façon plus approfondie. / Hereditary motor and sensory neuropathy (HMSN) is a rare disease that leads to delayed motor and mental development, loss of sensory and motor function and neuropsychiatric syndromes, and that is often accompanied by partial or complete agenesis of the corpus callosum. Additionally, several cases of short stature or low body weight have been reported in patients. HMSN is caused by loss-of-function mutations in K⁺-Cl⁻ cotransporter type 3 (KCC3). Detailed clinical reports and characterizations of mice inactivated for Kcc3 (Kcc3ᴷᴼ) have allowed to establish that defective K⁺-Cl⁻ export causes the anatomical and functional neurologic impairments in the disease. In Kcc3ᴷᴼ mice, extra-neurological abnormalities have also been noted: lower body weight, high blood pressure (BP), polydipsia and polyuria. Because the pathophysiology of extra-neurological traits arising from KCC3 loss of function remains incompletely described, my work aimed at understanding the mechanisms at play using a Kcc3ᴷᴼ model. An initial characterization of a constitutive and systemic Kcc3ᴷᴼ mouse line showed vascular and cardiac abnormalities along with a rise in diastolic BP. This model also showed polydipsia and iso-osmolar polyuria along with reduced body weight and adiposity but no decrease in food intake. A detailed metabolic characterization of our model further revealed reductions in fat and lean body masses. This leanness results certainly in part from increased locomotor activity and energy expenditure as measured. A marked improvement in glucose tolerance was also found in addition to lower plasmatic triglyceride concentrations. Lastly, we also demonstrated that our model is resistant to high-fat-diet-induced obesity and shows concomitant increase in expression of both lipogenic and lipolytic enzymes in visceral fat, thereby potentially generating caloric dissipation. When revisiting the cardiovascular function of our model with cutting-edge methods, we measured normal BP and arteriolar reactivity in baseline conditions. However, we noted an increase in passive arteriolar distensibility. In our model, we did not notice sensitivity of BP to dietary salt but found a marked increase in urinary solute excretion under high-salt diet and a strong preference for salt. These observations are consistent with a defect in hydromineral reabsorption by the nephron that may prevent BP from rising. In short, our work allowed to better understand the cardiometabolic characteristics that accompany the neurologic portrait of an HMSN mouse model. In particular, we noted unexpected benefits in carbohydrate and lipid metabolism upon Kcc3 inactivation. We also suspect that KCC3 ablation in the kidney leads to urinary hydromineral wasting that can be more salient under dietary salt loading and can influence BP by blunting extracellular volume expansion. The pleiotropic abnormalities arising from Kcc3 inactivation identify this gene as a new potential pharmacological target and argue for improving efforts at describing the cardiometabolic features of patients with HMSN.

modèle animal

cotransporteur K-Cl de type 3

homéostasie du glucose

métabolisme des lipides

dépense énergétique

hémodynamique

régulation hydrosodée

fonction rénale

réactivité artériolaire

hereditary motor and sensory neuropathy

animal model

K-Cl cotransporter type 3

glucose homeostasis

lipid metabolism

energy expenditure

hemodynamics

hydromineral regulation

renal function

arteriolar reactivity

Inhibiting Axon Degeneration in a Mouse Model of Acute Brain Injury Through Deletion of Sarm1

Henninger, Nils

24 May 2017

Traumatic brain injury (TBI) is a leading cause of disability worldwide. Annually, 150 to 200/1,000,000 people become disabled as a result of brain trauma. Axonal degeneration is a critical, early event following TBI of all severities but whether axon degeneration is a driver of TBI remains unclear. Molecular pathways underlying the pathology of TBI have not been defined and there is no efficacious treatment for TBI. Despite this significant societal impact, surprisingly little is known about the molecular mechanisms that actively drive axon degeneration in any context and particularly following TBI. Although severe brain injury may cause immediate disruption of axons (primary axotomy), it is now recognized that the most frequent form of traumatic axonal injury (TAI) is mediated by a cascade of events that ultimately result in secondary axonal disconnection (secondary axotomy) within hours to days. Proposed mechanisms include immediate post-traumatic cytoskeletal destabilization as a direct result of mechanical breakage of microtubules, as well as catastrophic local calcium dysregulation resulting in microtubule depolymerization, impaired axonal transport, unmitigated accumulation of cargoes, local axonal swelling, and finally disconnection. The portion of the axon that is distal to the axotomy site remains initially morphologically intact. However, it undergoes sudden rapid fragmentation along its full distal length ~72 h after the original axotomy, a process termed Wallerian degeneration. Remarkably, mice mutant for the Wallerian degeneration slow (Wlds) protein exhibit ~tenfold (for 2–3 weeks) suppressed Wallerian degeneration. Yet, pharmacological replication of the Wlds mechanism has proven difficult. Further, no one has studied whether Wlds protects from TAI. Lastly, owing to Wlds presumed gain-of-function and its absence in wild-type animals, direct evidence in support of a putative endogenous axon death signaling pathway is lacking, which is critical to identify original treatment targets and the development of viable therapeutic approaches. Novel insight into the pathophysiology of Wallerian degeneration was gained by the discovery that mutant Drosophila flies lacking dSarm (sterile a/Armadillo/Toll-Interleukin receptor homology domain protein) cell-autonomously recapitulated the Wlds phenotype. The pro-degenerative function of the dSarm gene (and its mouse homolog Sarm1) is widespread in mammals as shown by in vitro protection of superior cervical ganglion, dorsal root ganglion, and cortical neuron axons, as well as remarkable in-vivo long-term survival (>2 weeks) of transected sciatic mouse Sarm1 null axons. Although the molecular mechanism of function remains to be clarified, its discovery provides direct evidence that Sarm1 is the first endogenous gene required for Wallerian degeneration, driving a highly conserved genetic axon death program. The central goals of this thesis were to determine (1) whether post-traumatic axonal integrity is preserved in mice lacking Sarm1, and (2) whether loss of Sarm1 is associated with improved functional outcome after TBI. I show that mice lacking the mouse Toll receptor adaptor Sarm1 gene demonstrate multiple improved TBI-associated phenotypes after injury in a closed-head mild TBI model. Sarm1-/- mice developed fewer beta amyloid precursor protein (βAPP) aggregates in axons of the corpus callosum after TBI as compared to Sarm1+/+ mice. Furthermore, mice lacking Sarm1 had reduced plasma concentrations of the phosphorylated axonal neurofilament subunit H, indicating that axonal integrity is maintained after TBI. Strikingly, whereas wild type mice exhibited a number of behavioral deficits after TBI, I observed a strong, early preservation of neurological function in Sarm1-/- animals. Finally, using in vivo proton magnetic resonance spectroscopy, I found tissue signatures consistent with substantially preserved neuronal energy metabolism in Sarm1-/- mice compared to controls immediately following TBI. My results indicate that the Sarm1-mediated prodegenerative pathway promotes pathogenesis in TBI and suggest that anti-Sarm1 therapeutics are a viable approach for preserving neurological function after TBI.

Armadillo domain proteins

animal model

axon

axon

axon degeneration

behavior

beta amyloid precursor protein

brain Injuries

cerebral blood flow

corpus callosum

cytoskeletal proteins

cytoskeleton

functional outcome

histology

inbred C57BL

knockout

laser Doppler

magnetic resonance imaging

male

metabolism

mouse

neurofilament

neurosciences

pathology

proton magnetic resonance spectroscopy

recovery of function

spreading depolarization

spreading depression

translational research

traumatic axonal injury

traumatic brain injury

Wallerian degeneration

white matter

Critical Care

Emergency Medicine

Medical Cell Biology

Medical Neurobiology

Molecular and Cellular Neuroscience

Nervous System Diseases

Neurology

Other Neuroscience and Neurobiology

Sports Medicine

Sports Sciences

Translational Medical Research

Trauma