Exploring the Multiplex Detection Capabilities of Raman Spectroscopy on Mock Street Samples Containing Illicitly Manufactured Fentanyls

Williams Burnett, Mia Laverne

18 May 2020

No description available.

Chemistry

Toxicology

Fentanyl

Toxicology

Analytical

Raman Spectroscopy

IMFs

Illicitly Manufactured

Fentanyls

First Responders

Drug Overdose

Opiates

Opiate Crisis

Opioids

Fentanyl Patch

Agonist

Antagonist

peak

Impact of Nicotine and PPARd-agonist on Human Mesenchymal Stem Cells

Bhat, Samerna

20 May 2013

No description available.

Biomechanics

Biomedical Research

Cellular Biology

mesenchymal stem cell

smoking

nicotine

PPARd-agonist

HO-1

BMP-2

ALP

osteoblast

Alizarin red staining

Porcine skin explants as a new model to investigate microvesicle particle generation

Singh, Shikshita

16 May 2023

No description available.

Pharmacology

Toxicology

microvesicle particle generation

porcine skin

human skin

UVB radiation

Platelet Activating Factor

acid sphingomyelinase

carbamyl PAF agonist

phorbol ester

Enabling the Next Generation of Human Induced Pluripotent Stem Cell Derived Hematopoietic Stem Cell-Based Therapies

Wong, Casey

23 August 2023

Human induced pluripotent stem cells (iPSCs) represent a scalable cell source for the generation of hematopoietic progenitor cells (iHPCs); however, a lack of efficient iHPC expansion in vitro currently limits translational applications. To address this translational bottleneck, we assessed a panel of stem cell agonist cocktails (SCACs), originally developed to enhance cord-blood derived HSPC (CB-HSPC) expansion, on iHPC expansion. Three SCACs and GAS6 (X2A, X2A+GAS6, SM6, or SMA) were supplemented during iHPC differentiation and subsequent expansion using the STEMdiff™ Hematopoietic Kit. This monolayer differentiation strategy yielded a population of CD34⁺CD43⁺ and CD45⁺CD34⁺ iHPC. SCAC supplementation during iHPC differentiation yielded up to 2.5-fold higher frequency of CD34⁺CD43⁺ hematopoietic progenitors and up to 2.9-fold higher frequency of CD45⁺CD34⁺CD45RA⁻CD90⁺ HSC-like cells compared to non-treated controls. Subsequent SCAC supplementation during 2 weeks of expansion culture also significantly increased iHPC expansion (X2A+GAS6: 3.8-fold, X2A: 3.5-fold, SM6: 2.8-fold, SMA: 2.0-fold). The expanded iHPCs retained high levels of CD34⁺CD43⁺ expression but we observed an increase in the expansion of HSC-like cell fraction. The collective expansion observed with the SCACs was 1.5- to 2.8-fold higher than UM171 treatment alone. Furthermore, all SCAC-supplemented iHPCs retained multilineage potency, producing erythroid and granulocyte-macrophage progenitors in CFU assays. However, prolonged expansion, beyond 7 days, reduced multilineage potential, indicating a limited expansion window. Although optimal timing and composition of SCAC supplementation remains to be refined, these results highlight that exploiting the additive and synergistic effects of multiple small molecules represents a promising approach for enhancing iHPC expansion yields and biomanufacturing.

Stem cell agonist cocktail

Small molecule

Human induced pluripotent stem cell

Hematopoietic stem progenitor cell

Multipotent progenitor cell

Expansion

StemRegenin 1

UM171

Valproic acid

AA2P

Déterminants de la rétention en traitement par agonistes opioïdes chez les personnes faisant usage de drogues par injection à Montréal, Canada

Vlad, Dragos

01 1900

Contexte: La crise des surdoses d’opioïdes qui sévit actuellement est un problème majeur de santé publique. Les personnes faisant usage de drogues par injection (PUDI) avec un trouble d’usage d’opioïdes (TUO) sont particulièrement vulnérables aux méfaits des opioïdes. Le traitement par agonistes opioïdes (TAO) est une intervention clé pour contrer l’épidémie de surdoses. L’engagement à long terme en traitement est un facteur important dans l’atteinte d’issues favorables. Nous avons examiné les facteurs individuels, contextuels et programmatiques qui sous-tendent la rétention en TAO dans une population de PUDI à Montréal, Canada. Méthodes: Nous avons mené une étude transversale basée sur les données provenant du questionnaire initial d’une cohorte longitudinale de PUDI à Montréal (HEPCO). Les participants recrutés avaient ≥ 18 ans et s’étaient injectés des drogues dans les derniers 6 mois. L’éligibilité au TAO était définie par l’utilisation d’opioïdes dans les 6 derniers mois et/ou l’engagement récent ou actuel en TAO. La rétention en TAO a été définie par la mesure auto-rapportée du temps passé en traitement au moment de l’entrevue, catégorisée en 4 groupes (non-engagé en TAO, <1 an, 1-3 ans, ≥3 ans). Des analyses par régression logistique multinomiale ont été menées pour identifier les facteurs associés à la rétention en traitement. Résultats: Parmi les 805 participants recrutés entre mars 2011 et janvier 2020, 546 (68%) étaient éligibles au TAO (78% hommes, âge moyen 37 ans), desquels 255 (47%) étaient engagés en TAO. Parmi ceux-ci, 29% l’étaient depuis <1 an, 21% entre 1-3 ans et 50% ≥3 ans. Dans les analyses multivariées, être une femme, l’âge, la stabilité de logement et l’infection chronique par le virus de l’hépatite C (VHC) étaient positivement associés avec une plus longue durée d’engagement en TAO (comparé aux non-engagés), alors que des associations négatives étaient observées pour la consommation régulière d’opioïdes, de cocaïne et de cannabis. Parmi les participants engagés en TAO, ceux recevant davantage de doses non-supervisées et ceux non soumis à des dépistages urinaires réguliers étaient davantage retenus en traitement. Une dose de méthadone ≥ 60 mg/jour était associée à une cote 3 fois plus élevée d’être engagé en traitement pour ≥1 an (vs <1 an), mais cette association n’était pas statistiquement significative pour la rétention ≥ 3 ans. Conclusion: La moitié des participants éligibles au TAO étaient engagés en traitement. Parmi les PUDI en TAO, une grande proportion était engagée en traitement pour ≥ 3 ans. En plus des facteurs sociodémographiques, nous avons identifié des facteurs programmatiques associés à une plus longue durée d’engagement en traitement. Des approches plus flexibles dans les programmes de TAO pourraient contribuer à une plus longue rétention en traitement. En raison du devis transversal employé, la causalité inverse ne peut être exclue; des analyses longitudinales sont nécessaires. / Background: The ongoing opioid overdose crisis is a major public health issue. People who inject drugs (PWID) with opioid use disorder (OUD) are the most vulnerable to opioid-related harms. Opioid agonist therapy (OAT) is a safe and efficient treatment for OUD and is a key intervention to curb the epidemic. Longer-term engagement in OAT has been associated with better health and social outcomes. Retention in treatment is paramount. We sought to identify individual, contextual and treatment factors associated with retention in OAT in Montréal, Canada. Methods: We conducted a cross-sectional analysis of baseline data collected within a longitudinal cohort study of PWID in Montreal (HEPCO). Eligible participants were aged ≥18 years and had injected drugs in the previous 6 months. We restricted the analysis to those eligible for OAT, inferred from self-reported illicit opioid use or OAT receipt in the past-six months. The outcome variable, retention in OAT, was defined as self-reported time spent in treatment at baseline, categorized as not on OAT, < 1 year, 1-3 years, ≥3 years. Multinomial logistic regression analyses were conducted to identify factors associated with retention. Results: Of 805 cohort participants enrolled between March 2011 and January 2020, 546 (68%) were considered eligible for OAT (mean age: 37; 78% male) and included in analyses. Of those, 255 (47%) were currently enrolled in OAT (29% in treatment for <1 year, 21% for 1-3 years and 50% for ≥ 3 years). In multivariable analyses, female gender, older age, stable housing, and chronic hepatitis C infection were positively associated with longer stay in OAT (compared to not on OAT), whereas negative associations were noted for regular opioid, cocaine and cannabis use. Among PWID enrolled in OAT, those receiving take-home doses and those who did not have regular urine drug screening were more likely to have a longer stay in treatment. Methadone dose ≥ 60 mg/day was associated with over 3-fold odds of retention ≥ 1 year (vs < 1 year), but the association was not statistically significative for ≥ 3 years retention. Conclusion: Half of participants likely to be eligible for OAT were enrolled in treatment. Among active PWID receiving OAT, high prevalence of long-term engagement in treatment was observed. In addition to sociodemographic factors, we identified treatment-related factors associated with greater treatment duration, suggesting the need for flexible implementation approaches in OAT programmes. Due to our cross-sectional design, however, reverse causation cannot be excluded; findings should be confirmed in longitudinal samples.

Traitement par agonistes opioïdes

People who inject drugs (PWID)

Opioid agonist therapy

Retention in treatment

Rétention en traitement

Design and Synthesis of Novel Benzodiazepines

MacQuarrie, Stephanie Lee

05 January 2006

Bivalent drug design is an efficient strategy for increasing potency and selectivity of many drugs. We devised a strategy to prepare agonist-benzodiazepine heterodimers that could simultaneously bind to agonist and BZD sites of the GABAAR. We synthesized a benzodiazepine-MPEG model compound that relied on physiological GABA to elicit flux. We established that a tether at the N1 position of the BZD would not prevent binding to the receptor. However, coupling of GABA amides with long chain PEG tethers studied by another group member resulted in complete loss of agonist activity. We therefore ceased research in this particular area. 1,4-Benzodiazepin-2,5-diones display a wide range of pharmacological activities. Compounds containing the tricyclic proline-derived subtype have received attention as potent anxiolytic agents and as starting materials for anthramycin-inspired anticancer agents. More recently enantiopure (S)-proline-derived 1,4-benzodiazepin-2,5-diones have been recognized as selective α5 GABAA receptor ligands. Despite the impressive diversity of 1,4-benzodiazepine-2,5-diones prepared to date, enantiopure examples possessing a quaternary stereogenic center have been largely unexplored. "Memory of chirality" (MOC) is an emerging strategy for asymmetric synthesis. This technique enables the memory of a sole chiral center in the substrate to be retained in a process that destroys that center. We have used this technique to prepare a library of quaternary proline-derived, thioproline-derived and hydroxyproline-derived 1,4-benzodiazepin-2,5-diones, in high ee. We have developed an efficient synthetic method for preparing oxaproline-derived 1,4-benzodiazepin-2,5-diones in high yields, and by applying the MOC strategy we have prepared quaternary derivatives in acceptable %ee. We envision oxaproline-derived 1,4-benzodiazepin-2,5-diones may exhibit similar or more potent pharmacological properties than proline-derived 1,4-benzodiazepin-2,5-diones. Using density functional theory (DFT) methods, we modeled the formation of an enantiopure, dynamically chiral enolate intermediate and the slow racemization of the enolate on the alkylation reaction time scale. / Ph. D.

1,4-Benzodiazepin-1,5-dione

Density Functional Theory

Memory of Chirality

Agonist

Asymmetric Synthesis

Benzodiazepine

Bivalent Ligand

GABA_A Receptor

Heterodimer

En utvärdering av 5-HT1A-receptoragonisten vilazodone för en utökad antidepressiv effekt i behandlingen av egentlig depression / Evaluation of the antidepressant effect of vilazodone for the treatment of major depression

Khalifa, Aseel

January 2017

Major depressive disorder (MDD) is a mood disorder majorly responsible for disability and mortality worldwide. With a lifetime prevalence of 15-20%, it is the main cause of functional impairment in Western societies as well as the fourth most debilitating illness in the world. Although the pathophysiology of MDD is not yet fully understood, some evidence that suggest the presence of a neuroanatomical deficiency have given rise to the theory of a specific imbalance in the monoamine neurotransmitters noradrenaline (NA) and/or serotonin (5-HT) levels in the brain. Overall, the various classes of antidepressant agents that have been developed to increase monoamine levels on the basis of this proposal have been successful. However, facts relating to prevalent escalation in the illness and recurring episodes of depression point towards a need to enhance clinical treatment. Most conventional antidepressants such as selective serotonin reuptake inhibitors (SSRI) and selective serotonin and noradrenaline inhibitors (SNRI) pose problems in symptomatic improvement. These include therapeutic lag, safety and tolerability issues, making more than 30% patients with MDD unable to reach adequate relief. In this respect, the action mechanism has moved beyond conventional SSRI and lead to the introduction of vilazodone, a novel antidepressant with an additional 5-HT1A partial agonist profile argued to be of potential benefit for a greater efficacy, faster onset of action and better tolerability. Using secondary data, this project aimed to evaluate the role of vilazodone as a SPARI-drug in the overall clinical treatment of MDD as well as its potential in addressing some of the most common obstacles in antidepressant treatment. Study results proved vilazodone’s efficacy to be superior to placebo. Patients across all studies showed significant improvement in depressive symptoms measured in MADRS and HAMD17. Vilazodone was also shown to be generally safe and tolerable but was not positively distinguished from placebo with regards to adverse effects. An overall, meaningful improvement in depressive symptoms was demonstrated in vilazodone, which reinforces its merit as an important treatment option for patients with MDD.

vilazodone

viibryd

SPARI

5-HT1A

5-HT1A agonist

SSRI

SNRI

MDD

major depression

major depressive disorder

selective serotonin reuptake inhibitor

depression drug therapy

vilazodone

viibryd

SPARI

5-HT1A

5-HT1A agonist

SSRI

SNRI

MDD

depression

egentlig depression

selektiva serotoninåterupptagshämmare

Pharmaceutical Sciences

Farmaceutiska vetenskaper

The effect of zilpaterol hydrochloride on feedlot performance and carcass characteristics in weaner steers

Mantiziba, Chipo Winnie

12 January 2015

An experiment was conducted using forty-one Bonsmara steers (age ± 7 months) to determine the effect of zilpaterol hydrochloride (ZH) on the growth performance and carcass characteristics. The trial was structured using a completely randomized design with two treatments, control and ZH group. The steers were fed ZH for 28 consecutive days at the end of the finishing period and ZH was withdrawn from the diet 2 days prior to slaughter of the animals. The steers were placed in individual pens and weighed fortnightly throughout the 4 months trial. Zilpaterol hydrochloride (ZH) was included in the diet at a rate of 8.3 mg/kg of DM. Feeding of ZH increased (P< 0.05) body weight (BW) gain and ADG (1.102 vs. 1.444) and tended to increase (P = 0.067) feed efficiency (F:G) during the last month of the finishing period. There were no significant differences (P> 0.05) in daily dry matter intakes (DMI). For the control group, high treatment weight gains were significantly associated with high initial weight (r = 0.424, P = 0.049) and also high pre-treatment body weight (r = 0.678, P= 0.001). Treatment weight gain increased as the initial and pre-treatment weight gain increased in the control group. For the steers that were fed ZH, there was no significant correlation between the treatment body weight gain with initial weight (r = 0.097, P = 0.694) and also pre- treatment live weight (r = 0.393, P = 0.096). Supplementation of ZH significantly increased (P < 0.0001) the dressing percentage (56.4% vs. 58.4%) and had no significant (P>0.05) effect on the carcass weight. The outcome of the study suggest that supplementation of ZH in the diet during the last month of the finishing period enhances growth performance and shows the repartitioning capacity of the feed additive as a beta- agonist. / Agriculture and  Animal Health / M. Sc. (Agriculture (Animal Science)

Beta- adrenergic agonist

Zilmax

Beef cattle

Carcass characteristics

Growth performance

636.2084

Beef cattle -- Feeding and feeds

Beef cattle -- Quality

Le rôle des acides gras oméga-3 sur la balance énergétique, la régulation de l’appétit, l’état émotionnel et l’implication du récepteur GPR120

Auguste, Stéphanie

05 1900

L’obésité est un facteur de risque lié à des problèmes physiques, émotionnels et comportementaux. Aujourd’hui, l’alimentation est composée d’un régime typiquement occidental «Western diet» qui est riche en acides gras saturés (AGS) et pauvre en acides gras polyinsaturés (AGPI) tel que les oméga-3 (N-3) et occasionnant un déséquilibre du ratio alimentaire N-6/N-3. Ce déséquilibre est une des causes de la prévalence des maladies mentales y compris celles des troubles de l'humeur et de l’anxiété. L’acide docosahexaénoïque (ADH, 22: 6 n-3) est l’acide gras (AG) le plus abondant dans le cerveau et son accumulation est particulièrement élevée pendant la période périnatale. Il joue un rôle important dans le développement neuronal et d'autres fonctions du cerveau tel l'apprentissage et la mémoire. Des perturbations de l’environnement périnatal peuvent influencer à très long terme l’avenir de la descendance en la rendant plus susceptible de développer des problèmes d’obésité dans un contexte nutritionnel riche. On ignore cependant si le déficit alimentaire chez la mère et particulièrement en ADH aura un impact sur la motivation alimentaire de la progéniture. L’objectif principal de cette thèse est d’étudier le rôle potentiel des N-3 sur la balance énergétique, la motivation alimentaire, la dépression et le niveau d’anxiété des descendants de souris mâles adultes assujetties à une alimentation riche en gras. Nos données ont démontré qu‘un régime maternel déficitaire en ADH durant la période périnatale incitait la descendance à fournir plus d’effort afin d’obtenir un aliment palatable. Ceci entraînerait un dérèglement de l’homéostasie énergétique en augmentant le gain de poids et en diminuant l’activité locomotrice tout en exacerbant le comportement de type anxieux dès que les souris sont exposées à un milieu obésogène. Les acides gras libres (AGL) sont des nutriments essentiels fonctionnant comme des molécules de signalisation dans le cerveau en ayant des récepteurs qui jouent un rôle important dans le contrôle du métabolisme énergétique. Parmi eux, on distingue un récepteur couplé à la protéine G (GPCR), le GPR120. Ce récepteur activé par les AGPI ω-3 intervient dans les mécanismes anti-inflammatoires et insulino-résistants via les N-3. Une mutation dans le gène GPR120 occasionnée par une réduction de l’activité de signalisation du gène est liée à l’obésité humaine. L'objectif premier de cette deuxième étude était d’évaluer l'impact de la stimulation pharmacologique de GPR120 dans le système nerveux central (SNC) sur l'alimentation, les dépenses d'énergie, le comportement de type anxieux et la récompense alimentaire. Nos résultats démontrent qu’une injection centrale aiguë d'agoniste GPR120 III réduit la prise alimentaire ad libitum et la motivation alimentaire pour un aliment riche en gras et en sucre; ainsi que les comportements de type anxieux. L’injection centrale chronique (21 jours) de ce même agoniste GPR120 III transmis par une pompe osmotique a démontré que les souris placées sous diète hypercalorique (HFD n’ont présenté aucune modification lors de la prise alimentaire ni de gain de poids mais qu’il y avait comparativement au groupe de véhicule, une réduction du comportement de type anxieux, que ce soit dans le labyrinthe en croix surélevé (LCS) ou dans le test à champ ouvert (OFT). L’ADH est reconnu pour ses propriétés anorexigènes au niveau central. De plus, la stimulation des récepteurs de GPR120 au niveau du cerveau avec un agoniste synthétique peut produire un effet intense intervenir sur le comportement lié à l'alimentation des rongeurs. Trouver une approche visant à contrôler à la fois la neuroinflammation, la récompense alimentaire et les troubles émotionnels aiderait assurément au traitement de l'obésité et du diabète de type 2. / Obesity is a risk factor for metabolic and mood disorders. The increasing abundance of the "Western diet" that is rich in saturated fatty acids (SFA) and low in polyunsaturated fatty acids (PUFA) omega-3 (N-3) can generate a physiological imbalance in the ratio of N-6/N-3 fatty acids. Such an imbalance has also been implicated in the increased prevalence of mood disorders and metabolic diseases. Docosahexaenoic acid (DHA, 22:6n-3), the most abundant fatty acid (FA) in the brain is accumulated not only during the post-natal period but also during the perinatal period. It plays an important role in neuronal development and other brain functions such as learning and memory. Disturbances of the perinatal environment can influence the sustainable future of the offspring, making it more likely to develop obesity in rich nutritional context. Some data suggest that an inadequate maternal intake of N-3 during pregnancy and the perinatal period may cause an increase in appetite signalling in the offspring as well as an increase rate of neurological and cardio-metabolic disease. It is not known if maternal dietary deficiency in N-3 will have an impact on food motivation of the offspring. The main objective of this thesis was to study the potential effect of dietary deficiency of DHA during the perinatal period on energy balance, food motivation and the anxiety-like behavior of adult male mouse offspring placed on HFD. Our data showed, as expected, that the maternal DHA deficient diet during perinatal period encouraged offspring to work harder to get a palatable food, entailed a dysregulation of energy homeostasis by increasing the body weight and reducing locomotor activity and exacerbated the anxiety-like behavior once they were exposed to an obesogenic environment. Free fatty acids (FFA) are essential nutrients that they also function as signalling molecules in the brain and have receptors that play a significant role in the control of energy metabolism. Among them is GPR120, also known as N-3 FA receptor, a g-protein coupled receptor that is reportedly activated by PUFA and shown to mediate the anti-inflammatory and insulin-sensitizing effects of N-3 FA. A mutation in the GPR120 gene that is associated with reduced GPR120 signalling activity is linked to human obesity. The objective of our second study was to test the impact of pharmacological GPR120 stimulation in the CNS on feeding, energy expenditure, anxiety-like behavior and food reward. Our results showed that an acute central injection GPR120 agonist III: reduced ad libitum food intake and the rewarding effect for high fat, high sugar food; produced a significant decrease in the anxiety-like behavior. While mice with the chronic injection (21 days) of GPR120 III agonist pump on HFD didn’t show any modification in food intake or body weight gain, but show a reduction of anxiety-like behavior in Elevated plus maze (EPM) and open-field test (OFT) compare to the vehicle group. DHA is notifies to have an anorectic action. Furthermore, stimulation of GPR120 receptors with synthetic agonist may cause an acute and profound effect on food related behavior in rodents. To find an approach that aims to control neuroinflammation, food reward and emotional disorders would greatly assist the treatment of obesity and type 2 diabetes.

oméga-3

Déficit périnatal

GPR120 agoniste

Anxiété

Récompense alimentaire

Dietary deficiency

Omega-3 fatty acid

GPR120 agonist

Anxiety

Food motivation

Reward

Vliv perinatální hypoxie na motorický vývoj laboratorního potkana a možnosti ovlivnění / The influence of perinatal hypoxia on motoric development on laboratory rat and means of therapy

Vachovcová, Sylva

January 2014

Severe perinatal hypoxia represents a substantial brain injury in human newborns. This Diploma thesis is focused on long-term motor outcome of laboratory rat after moderate perinatal hypoxia. We described some behavioral test for detection motor development and presented the influence of perinatal hypoxia on central nervous system. We also discussed an effect of agonists and antagonists of adenosine A1 receptor in brain. The aim of an experimental part was an evaluation of long-term motor behavior in rats affected by perinatal hypoxia. To cause perinatal hypoxia we put pregnant female rats to a hypoxic (10% O2) normobaric room in 11th day of their gestation. The pregnant female rats stayed in hypoxic room until they gave a birth and 6 more days after birth with their litters. For classification of motor development we used battery of tests of motor coordination. These tests correspond to the level of development of the rat. Then a group of rats with perinatal hypoxia was treated by a single administration of an agonist of adenosine A1 receptor 2-chloro-N(6)- cyclopentyladenosin (CCPA) in postnatal day 14. The animals affected by perinatal hypoxia show motor deficits in 3 from 4 selected behavioral tests. Otherwise, this motor behavior was no longer detected in young adults. The rats affected by...