Descriptor: "Cannabinoid" / Database: OAIster - Searchworks@Jio Institute Digital Library Search Results

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453 results on '"Cannabinoid"'

1. Synthetic cannabinoid quinones: Preparation, in vitro antiproliferative effects and in vivo prostate antitumor activity

Author: Morales, Paula, Vara, Diana, Zúñiga, María C., Olea-Azar, Claudio, Goya, Pilar, Jagerovic, Nadine, Gómez Cañas, María, Fernández Ruiz, José Javier, Díaz-Laviada Marturet, Inés, Morales, Paula, Vara, Diana, Zúñiga, María C., Olea-Azar, Claudio, Goya, Pilar, Jagerovic, Nadine, Gómez Cañas, María, Fernández Ruiz, José Javier, and Díaz-Laviada Marturet, Inés
Abstract: Chromenopyrazolediones have been designed and synthesized as anticancer agents using the multi biological target concept that involves quinone cytotoxicity and cannabinoid antitumor properties. In cell cytotoxicity assays, these chromenopyrazolediones have antiproliferative activity against human prostate cancer and hepatocellular carcinoma. It has been shown that the most potent, derivative 4 (PM49), inhibits prostate LNCaP cell viability (IC50 ¼ 15 mM) through a mechanism involving oxidative stress, PPARg receptor and partially CB1 receptor. It acts on prostate cell growth by causing G0/G1 phase arrest and triggering apoptosis as assessed by flow cytometry measurements. In the in vivo treatment, compound 4 at 2 mg/kg, blocks the growth of LNCaP tumors and reduces the growth of PC-3 tumors generated in mice. These studies suggest that 4 is a good potential anticancer agent against hormone sensitive prostate cancer, Depto. de Bioquímica y Biología Molecular, Fac. de Medicina, TRUE, pub
Published: 2024

2. Self-reported adverse events associated with ∆8-Tetrahydrocannabinol (Delta-8-THC) Use.

Author: Leas, Eric C, Leas, Eric C, Harati, Raquel M, Satybaldiyeva, Nora, Morales, Nicolas E, Huffaker, Shelby L, Mejorado, Tomas, Grant, Igor, Leas, Eric C, Leas, Eric C, Harati, Raquel M, Satybaldiyeva, Nora, Morales, Nicolas E, Huffaker, Shelby L, Mejorado, Tomas, and Grant, Igor
Abstract: BackgroundThere is an expanding unregulated market for a psychotropic compound called ∆8-Tetrahydrocannabinol (delta-8-THC) that is being derived from hemp, but a summary of adverse events related to delta-8-THC has not been publicly reported.MethodsThis case series assessed adverse events reported by delta-8-THC users on the Reddit forum r/Delta8 and compared these to delta-8-THC AEs in the US Food and Drug Administration Adverse Event Reporting System (FAERS). Delta-8-THC and cannabis AEs reported in FAERS were also compared. The r/Delta8 forum was selected because it includes a large sample of 98,700 registered individuals who publicly discuss their experiences using delta-8-THC. All r/Delta8 posts were obtained from August 20, 2020, through September 25, 2022. A random sample of r/Delta8 posts was drawn (n = 10,000) and filtered for posts in which delta-8-THC users reported an adverse event (n = 335). FAERS reports that listed delta-8-THC (N = 326) or cannabis (N = 7076) as a suspect product active ingredient were obtained. Adverse events claimed to result from delta-8-THC use were coded using Medical Dictionary for Regulatory Activities to system organ class and preferred term categories.ResultsThe absolute number of delta-8-THC adverse event reports (N = 2184, 95% CI = 1949-2426) and serious adverse event reports (N = 437; 95% CI = 339-541) on r/Delta 8 were higher than the adverse event reports (N = 326) and serious adverse event reports (N = 289) to FAERS. Psychiatric disorders were the most frequently cited system organ class in r/Delta8 adverse event reports, mentioned in 41.2% (95% CI = 35.8%-46.3%) of reports, followed by respiratory, thoracic and mediastinal disorders (29.3%, 95% CI = 25.1%-34.0%) and nervous system disorders (23.3%, 95% CI = 18.5%-27.5%). Anxiety (16.4%, 95% CI = 12.8-20.6), Cough (15.5%, 95% CI = 11.9-20.0) and Paranoia (9.3%, 95% CI = 6.3-12.5) were the most frequently cited preferred terms in adverse event reports. The overall preva
Published: 2023

3. The Safety and Comparative Effectiveness of Non-Psychoactive Cannabinoid Formulations for the Improvement of Sleep: A Double-Blinded, Randomized Controlled Trial.

Author: Saleska, Jessica Londeree, Saleska, Jessica Londeree, Bryant, Corey, Kolobaric, Antonija, D'Adamo, Christopher R, Colwell, Christopher S, Loewy, Derek, Chen, Jeff, Pauli, Emily K, Saleska, Jessica Londeree, Saleska, Jessica Londeree, Bryant, Corey, Kolobaric, Antonija, D'Adamo, Christopher R, Colwell, Christopher S, Loewy, Derek, Chen, Jeff, and Pauli, Emily K
Abstract: BackgroundClinical evidence on the use of cannabidiol (CBD) for sleep remains limited. Even fewer studies have tested the comparative effectiveness of cannabinoid formulations found within CBD products used for sleep or how they compare to other complementary therapies such as melatonin.MethodsParticipants (N = 1,793 adults experiencing symptoms of sleep disturbance) were randomly assigned to receive a 4-week supply of 1 of 6 products (all capsules) containing either 15 mg CBD or 5 mg melatonin, alone or in combination with minor cannabinoids. Sleep disturbance was assessed over a period of 5 weeks (baseline week and 4 weeks of product use) using Patient-Reported Outcomes Measurement Information System (PROMIS™) Sleep Disturbance SF 8A, administered via weekly online surveys. A linear mixed-effects regression model was used to assess the differences in the change in sleep disturbance through time between each active product arm and CBD isolate.ResultsAll formulations exhibited a favorable safety profile (12% of participants reported a side effect and none were severe) and led to significant improvements in sleep disturbance (p < 0.001 in within-group comparisons). Most participants (56% to 75%) across all formulations experienced a clinically important improvement in their sleep quality. There were no significant differences in effect, however, between 15 mg CBD isolate and formulations containing 15 mg CBD and 15 mg cannabinol (CBN), alone or in combination with 5 mg cannabichromene (CBC). There were also no significant differences in effect between 15 mg CBD isolate and formulations containing 5 mg melatonin, alone or in combination with 15 mg CBD and 15 mg CBN.ConclusionsOur findings suggest that chronic use of a low dose of CBD is safe and could improve sleep quality, though these effects do not exceed that of 5 mg melatonin. Moreover, the addition of low doses of CBN and CBC may not improve the effect of formulations containing CBD or melatonin isolate.
Published: 2023

4. Mechanisms of Control of Neuron Survival by the Endocannabinoid System

Author: Galve Roperh, Ismael, Aguado Sánchez, Tania, Palazuelos Diego, Javier, Guzmán Pastor, Manuel, Galve Roperh, Ismael, Aguado Sánchez, Tania, Palazuelos Diego, Javier, and Guzmán Pastor, Manuel
Abstract: Endocannabinoids act as retrograde messengers that, by inhibiting neurotransmitter release via presynaptic CB1 cannabinoid receptors, regulate the functionality of many synapses. In addition, the endocannabinoid system participates in the control of neuron survival. Thus, CB1 receptor activation has been shown to protect neurons from acute brain injury as well as in neuroinflammatory conditions and neurodegenerative diseases. Nonetheless, some studies have reported that cannabinoids can also exert neurotoxic actions. Cannabinoid neuroprotective activity relies on the inhibition of glutamatergic neurotransmission and on other various mechanisms, and is supported by the observation that the brain overproduces endocannabinoids upon damage. Coupling of neuronal CB1 receptors to cell survival routes such as the phosphatidylinositol 3-kinase/Akt and extracellular signal-regulated kinase pathways may contribute to cannabinoid neuroprotective action. These pro-survival signals occur, at least in part, by the cross-talk between CB1 receptors and growth factor tyrosine kinase receptors. Besides promoting neuroprotection, a role for the endocannabinoid system in the control of neurogenesis from neural progenitors has been put forward. In addition, activation of CB2 cannabinoid receptors on glial cells may also participate in neuroprotection by limiting the extent of neuroinflammation. Altogether, these findings support that endocannabinoids constitute a new family of lipid mediators that act as instructive signals in the control of neuron survival., Ministerio de Educación y Ciencia, Comunidad de Madrid, Picasso Program, Fundación de Investigación Médica Mutua Madrileña Automovilística, Depto. de Bioquímica y Biología Molecular, Fac. de Ciencias Biológicas, TRUE, pub
Published: 2023

5. Development of the High-Affinity Carborane-Based Cannabinoid Receptor Type 2 PET Ligand [18F]LUZ5-d8

Author: Ueberham, L., (0000-0001-9743-2325) Gündel, D., Kellert, M., (0000-0003-3168-3062) Deuther-Conrad, W., (0000-0002-4358-5171) Ludwig, F.-A., Lönnecke, P., Kazimir, A., (0000-0003-4846-1271) Kopka, K., (0000-0001-5555-7058) Brust, P., (0000-0003-3119-7945) Moldovan, R.-P., Hey-Hawkins, E., Ueberham, L., (0000-0001-9743-2325) Gündel, D., Kellert, M., (0000-0003-3168-3062) Deuther-Conrad, W., (0000-0002-4358-5171) Ludwig, F.-A., Lönnecke, P., Kazimir, A., (0000-0003-4846-1271) Kopka, K., (0000-0001-5555-7058) Brust, P., (0000-0003-3119-7945) Moldovan, R.-P., and Hey-Hawkins, E.
Abstract: The development of cannabinoid receptor type 2 (CB2R) radioligands for positron emission tomography (PET) imaging was intensively explored. To overcome the low metabolic stability and simultaneously increase the binding affinity of known CB2R radioligands, a carborane moiety was used as a bioisostere. Here we report the synthesis and characterization of carboranebased 1,8-naphthyridinones and thiazoles as novel CB2R ligands. All tested compounds showed low nanomolar CB2R affinity, with (Z)-N-[3-(4-fluorobutyl)-4,5-dimethylthiazole-2(3H)-ylidene]-(1,7-dicarba-closo-dodecaboranyl)-carboxamide (LUZ5) exhibiting the highest affinity (0.8 nM). Compound [18F]LUZ5-d8 was obtained with an automated radiosynthesizer in high radiochemical yield and purity. In vivo evaluation revealed the improved metabolic stability of [18F]LUZ5-d8 compared to that of [18F]JHU94620. PET experiments in rats revealed high uptake in spleen and low uptake in brain. Thus, the introduction of a carborane moiety is an appropriate tool for modifying literature-known CB2R ligands and gaining access to a new class of high-affinity CB2R ligands, while the in vivo pharmacology still needs to be addressed.
Published: 2023

6. Data publication, PET: Development of the High-Affinity Carborane-Based Cannabinoid Receptor Type 2 PET Ligand [18F]LUZ5-d8

Author: (0000-0001-9743-2325) Gündel, D. and (0000-0001-9743-2325) Gündel, D.
Abstract: DICOM dataset of dynamic PET aquisitions and images associated with the publication: Development of the High-Affinity Carborane-Based Cannabinoid Receptor Type 2 PET Ligand [18F]LUZ5-d8 (DOI: 10.1021/acs.jmedchem.3c00195), funded by DFG (MO 2677/4-1).
Published: 2023

7. European epidemiological patterns of cannabis- and substance-related congenital neurological anomalies: Geospatiotemporal and causal inferential study

Author: Reece, Albert Stuart, Hulse, Gary Kenneth, Reece, Albert Stuart, and Hulse, Gary Kenneth
Abstract: Introduction: Of the many congenital anomalies (CAs) recently linked with community cannabis exposure, arguably the most concerning are neurological CAs (NCAs). We therefore conducted a detailed study of this in fourteen European nations. Methods. Congenital anomaly data were from Eurocat. Drug exposure data were from European Monitoring Centre for Drugs and Drug Addiction. Income from World bank. Results: The Netherlands, Spain, France and Bulgaria reported increasing rates of many NCAs. The NCA rate (NCAR) was: severe microcephaly 2.14 x 1013 higher in nations with increasing daily cannabis use when compared to those without (p = 0.0204, minimum E-value (mEV) = 1.35). At bivariate analysis, the mEVs of the following NCAs were significantly cannabis related, craniosynostosis 5.27 x 1011, nervous system 4.87 x 1011, eye 2.73 x 107, microphthalmos 4.07 x 106, anencephalus 710.37, hydrocephalus 245.64, spina bifida 14.86 and neural tube defects 13.15. At inverse probability, weighted panel regression terms including cannabis were significantly related to the following series of anomalies: nervous system, anencephalus, severe microcephalus, microphthalmos, neural tube defect and spina bifida from p = 5.09 x 10−8, < 2.2 x 10−16, < 2.2 x 10−16, 4.84 x 10−11, < 2.2 x 10−16 and 9.69 x 10−7. At geospatial regression, this same series of anomalies had terms including cannabis significant from p = 0.0027, 1.53 x 10−7, 3.65 x 10−6, 2.13 x 10−8, 0.0002 and 9.76 x 10−12. 88.0% of 50 E-value estimates and 72.0% of mEVs > 9. This analysis therefore demonstrates both close association of cannabis exposure with multiple NCAs across space-time and also fulfills the quantitative criteria of causal inferential analysis. Conclusions: Nine NCARs on bivariate and six NCARs on multivariable regression were cannabis related and fulfilled quantitative epidemiological criteria for causality and are consistent with other series. Particular concerns relate to exponential dose–response effects d
Published: 2023

8. Perturbation of 3D nuclear architecture, epigenomic dysregulation and aging, and cannabinoid synaptopathy reconfigures conceptualization of cannabinoid pathophysiology: part 1–aging and epigenomics

Author: Reece, Albert Stuart, Hulse, Gary Kenneth, Reece, Albert Stuart, and Hulse, Gary Kenneth
Abstract: Much recent attention has been directed toward the spatial organization of the cell nucleus and the manner in which three-dimensional topologically associated domains and transcription factories are epigenetically coordinated to precisely bring enhancers into close proximity with promoters to control gene expression. Twenty lines of evidence robustly implicate cannabinoid exposure with accelerated organismal and cellular aging. Aging has recently been shown to be caused by increased DNA breaks. These breaks rearrange and maldistribute the epigenomic machinery to weaken and reverse cellular differentiation, cause genome-wide DNA demethylation, reduce gene transcription, and lead to the inhibition of developmental pathways, which contribute to the progressive loss of function and chronic immune stimulation that characterize cellular aging. Both cell lineage-defining superenhancers and the superanchors that control them are weakened. Cannabis exposure phenocopies the elements of this process and reproduces DNA and chromatin breakages, reduces the DNA, RNA protein and histone synthesis, interferes with the epigenomic machinery controlling both DNA and histone modifications, induces general DNA hypomethylation, and epigenomically disrupts both the critical boundary elements and the cohesin motors that create chromatin loops. This pattern of widespread interference with developmental programs and relative cellular dedifferentiation (which is pro-oncogenic) is reinforced by cannabinoid impairment of intermediate metabolism (which locks in the stem cell-like hyper-replicative state) and cannabinoid immune stimulation (which perpetuates and increases aging and senescence programs, DNA damage, DNA hypomethylation, genomic instability, and oncogenesis), which together account for the diverse pattern of teratologic and carcinogenic outcomes reported in recent large epidemiologic studies in Europe, the USA, and elsewhere. It also accounts for the prominent aging phenotype observ
Published: 2023

9. Sociodemographically stratified exploration of pancreatic cancer incidence in younger US patients: Implication of cannabis exposure as a risk factor

Author: Reece, Albert S., Hulse, Gary K., Reece, Albert S., and Hulse, Gary K.
Abstract: Introduction. The aetiology for the recent increase in pancreatic cancer incidence (PCI) in the US is unknown. This paper provides an epidemiological investigation of the exponential increase in PCI in young people aged 15–34 years, particularly amongst females, with a focus on the exponential rise amongst African American females, and its relationship to substance use. Methods. National pancreatic cancer data from recent reports. Tobacco, alcohol and daily cannabis use data taken from the annual nationally representative National Survey of Drug Use and Health, response rate = 74%. Results. Amongst the 15–34-year-aged cohort, PCI was found to be significantly more common in females (females: -est. = 0.1749 p = 0.0005). African American females are noted to have the highest rates of daily cannabis use amongst females in the 26–34 and 35–49-year groups. The relationship between PCI and daily cannabis use was strongly positive across all ethnicities and in both sexes. In African American females, the Pearson correlation between daily cannabis use and PCI was R = 0.8539, p = 0.0051. In an additive multivariable model for each sex and race, cannabis was the only significant term remaining in the final model in the 15–34-year-aged cohort and thus out-performed alcohol as a risk factor. The most significant term in multivariate models was the alcohol:cannabis interaction which was highly significant in all ethnicities from p = 2.50 × 10−7 for Caucasian American females and the highest E-value pair was for Hispanic American females (E-value estimate = 1.26 × 10102 and E-value lower bound 2.20 × 1074). Conclusion. These data show that cannabis fulfills quantitative criteria of causality in all age, sex and ethnicity cohorts, and thus explains both the recent surge in PCI and its ethnocentric predominance. Cannabis interacts powerfully genotoxically and cancerogenically with alcohol, with increases in cannabis use driving the current PCI surge. These results raise the importa
Published: 2023

10. Patterns of cannabis- and substance-related congenital general anomalies in Europe: A geospatiotemporal and causal inferential study

Author: Reece, Albert Stuart, Hulse, Gary Kenneth, Reece, Albert Stuart, and Hulse, Gary Kenneth
Abstract: Introduction: Recent series of congenital anomaly (CA) rates (CARs) have showed the close and epidemiologically causal relationship of cannabis exposure to many CARs. We investigated these trends in Europe where similar trends have occurred. Methods: CARs from EUROCAT. Drug use from European Monitoring Centre for Drugs and Drug Addiction. Income data from World Bank. Results: CARs were higher in countries with increasing daily use overall (p = 9.99 × 10−14, minimum E-value (mEV) = 2.09) and especially for maternal infections, situs inversus, teratogenic syndromes and VACTERL syndrome (p = 1.49 × 10−15, mEV = 3.04). In inverse probability weighted panel regression models the series of anomalies: all anomalies, VACTERL, foetal alcohol syndrome, situs inversus (SI), lateralization (L), and teratogenic syndromes (TS; AAVFASSILTS) had cannabis metric p-values from: p < 2.2 × 10−16, 1.52 × 10−12, 1.44 × 10−13, 1.88 × 10−7, 7.39 × 10−6 and −16. In a series of spatiotemporal models this anomaly series had cannabis metric p-values from: 8.96 × 10−6, 6.56 × 10−6, 0.0004, 0.0019, 0.0006, 5.65 × 10−5. Considering E-values, the cannabis effect size order was VACTERL > situs inversus > teratogenic syndromes > FAS > lateralization syndromes > all anomalies. 50/64 (78.1%) E-value estimates and 42/64 (65.6%) mEVs > 9. Daily cannabis use was the strongest predictor for all anomalies. Conclusion: Data confirmed laboratory, preclinical and recent epidemiological studies from Canada, Australia, Hawaii, Colorado and USA for teratological links between cannabis exposure and AAVFASSILTS anomalies, fulfilled epidemiological criteria for causality and underscored importance of cannabis teratogenicity. VACTERL data are consistent with causation via cannabis-induced Sonic Hedgehog inhibition. TS data suggest cannabinoid contribution. SI&L data are consistent with results for cardiovascular CAs. Overall, these data show that cannabis is linked across space and time and in a manner which fulfill
Published: 2023

11. Congenital gastrointestinal anomalies in Europe 2010–2019: A geo-spatiotemporal and causal inferential study of epidemiological patterns in relationship to cannabis- and substance exposure

Author: Reece, Albert Stuart, Hulse, Gary Kenneth, Reece, Albert Stuart, and Hulse, Gary Kenneth
Abstract: Introduction: Congenital anomalies (CA’s) of most of the gastrointestinal tract have been linked causally with prenatal or community cannabis exposure. Therefore, we studied this relationship in Europe. Methods: CA data were from Eurocat. Drug-use data were sourced from the European Monitoring Centre for Drugs and Drug Addiction. Income data were taken from the World Bank. Results: When countries with increasing rates of daily cannabis use were compared with those which were not, the overall rate of gastrointestinal CA’s (GCA’s) was higher in the former group (p = 0.0032). The five anomalies which were related to the metrics of cannabis exposure on bivariate analysis were bile duct atresia, Hirschsprungs, digestive disorders, annular pancreas and anorectal stenosis or atresia. The following sequence of GCA’s was significantly linked with cannabis metrics at inverse-probability-weighted-panel modelling, as indicated: esophageal stenosis or atresia, bile duct atresia, small intestinal stenosis or atresia, anorectal stenosis or atresia, Hirschsprungs disease: p = 1.83 × 10−5, 0.0046, 3.55 × 10−12, 7.35 × 10−6 and 2.00 × 10−12, respectively. When this GCA series was considered in geospatial modelling, the GCA’s were significantly cannabis-related from p = 0.0003, N.S., 0.0086, 6.652 × 10−5, 0.0002, 71.4% of 35 E-value estimates and 54.3% minimum E-values (mEVv’s) > 9 (high zone) and 100% and 97.1% > 1.25 (causality threshold). The order of cannabis sensitivity by median mEVv was Hirschsprungs > esophageal atresia > small intestinal atresia > anorectal atresia > bile duct atresia. Conclusions: Seven of eight GCA’s were related to cannabis exposure and fulfilled the quantitative criteria for epidemiologically causal relationships. Penetration of cannabinoids into the community should be carefully scrutinized and controlled to protect against exponential and multigenerational genotoxicity ensuing from multiple cannabinoids.
Published: 2023

12. Clinical epigenomic explanation of the epidemiology of cannabinoid genotoxicity manifesting as transgenerational teratogenesis, cancerogenesis and aging acceleration

Author: Reece, Albert Stuart, Hulse, Gary Kenneth, Reece, Albert Stuart, and Hulse, Gary Kenneth
Abstract: As global interest in the therapeutic potential of cannabis and its’ derivatives for the management of selected diseases increases, it is increasingly imperative that the toxic profile of cannabinoids be thoroughly understood in order to correctly assess the balance between the therapeutic risks and benefits. Modern studies across a number of jurisdictions, including Canada, Australia, the US and Europe have confirmed that some of the most worrying and severe historical reports of both congenital anomalies and cancer induction following cannabis exposure actually underestimate the multisystem thousand megabase-scale transgenerational genetic damage. These findings from teratogenic and carcinogenic literature are supported by recent data showing the accelerated patterns of chronic disease and the advanced DNA methylation epigenomic clock age in cannabis exposed patients. Together, the increased multisystem carcinogenesis, teratogenesis and accelerated aging point strongly to cannabinoid-related genotoxicity being much more clinically significant than it is widely supposed and, thus, of very considerable public health and multigenerational impact. Recently reported longitudinal epigenome-wide association studies elegantly explain many of these observed effects with considerable methodological sophistication, including multiple pathways for the inhibition of the normal chromosomal segregation and DNA repair, the inhibition of the basic epigenetic machinery for DNA methylation and the demethylation and telomerase acceleration of the epigenomic promoter hypermethylation characterizing aging. For cancer, 810 hits were also noted. The types of malignancy which were observed have all been documented epidemiologically. Detailed epigenomic explications of the brain, heart, face, uronephrological, gastrointestinal and limb development were provided, which amply explained the observed teratological patterns, including the inhibition of the key morphogenic gradients. Hence, thes
Published: 2023

13. Comparing Nutrient Management Strategies in Decoupled Aquaponics Systems for Growing Cannabis sativa

Author: Johnson, Jessie M. and Johnson, Jessie M.
Abstract: Aquaponics is a system of aquaculture that uses waste produced by farmed aquatic animals to supply nutrients to a hydroponic system for growing plants. The growth of Cannabis sativa in aquaponics systems displays the potential for well-managed aquaponic systems to produce a variety of crops. A small, commercial-style aquaponic system was used to test how nutrient management techniques impact the growth of Cannabis sativa in a decoupled aquaponics system. Treatments included: a recirculating treatment using aquaponic system effluent plus nutrient supplementation (AqRN), a flow-through treatment utilizing aquaponic system effluent (AqFT), a flow-through hydroponic treatment supplemented with aquaponic effluent (10% by volume) (AqHydro), and a flow-through hydroponic control treatment (Hydro). Following a 13-week growing trial, flower buds were harvested, dried, and cured to determine yields from each treatment. Cured samples (3g) were sent to a lab for analysis of cannabinoids and terpenes.Results show growing hemp in aquaponics systems can provide comparable yields to hydroponic systems. No significant difference in yield existed between AqHydro, Hydro, and AqFT treatments. The AqRN treatment showed a significantly lower trimmed yield and plants showed signs of stress and nutrient deficiency approaching the end of the trial. The AqFT produced fewer overall terpenes than the other treatments and may benefit from micro-nutrient supplementation. The AqHydro and Hydro treatments showed no significant difference in water quality or yield. However, the AqHydro treatment consumed less water, indicating that supplementation with aquaculture effluent has the potential to significantly reduce the cost of fertigation in hydroponics systems.
Published: 2023

14. Prenatal risk factors and postnatal cannabis exposure: Assessing dual models of schizophrenia-like rodents

Author: Martín-Cuevas, Celia, Ramos Herrero, Víctor, Crespo-Facorro, Benedicto, Sánchez-Hidalgo, Ana C., Martín-Cuevas, Celia, Ramos Herrero, Víctor, Crespo-Facorro, Benedicto, and Sánchez-Hidalgo, Ana C.
Abstract: Schizophrenia (SCZ) is a multifactorial neurodevelopmental disorder caused by genetic and environmental alterations, especially during prenatal stages. On the other hand, cannabis consumption in adolescence has been also linked to an increased risk of developing SCZ. The combination of both hits has been proposed as the dual hit hypothesis of SCZ. We systematically reviewed prenatal environmental alterations and cannabis consumption during adolescence that are associated with an increased risk of SCZ, following the PRISMA model. The analysis focused on dual animal models where the first hit is prenatal environmental exposure and the second hit consists of postnatal cannabis exposure. The articles were evaluated by three independent reviewers based on inclusion criteria. We extracted the first author´s name, year, model species, sex and analysis. The articles reported on dual murine models and their effects on weight, behavior, genetics, electrophysiology and brain structure and function. We conclude that the defects caused by the dual hits depend on the sex of the model, as well as type of hits.
Published: 2023

15. Effect of the Cannabinoid Agonist WIN 55,212-2 on Neuropathic and Visceral Pain Induced by a Non-Diarrheagenic Dose of the Antitumoral Drug 5-Fluorouracil in the Rat

Author: Ministerio de Ciencia, Innovación y Universidades (España), Vera, G., López-Gómez, L., Girón, R., Martín-Fontelles, M. I., Nurgali, K., Abalo, R., Uranga, J. A., Ministerio de Ciencia, Innovación y Universidades (España), Vera, G., López-Gómez, L., Girón, R., Martín-Fontelles, M. I., Nurgali, K., Abalo, R., and Uranga, J. A.
Abstract: 5-fluorouracil (5-FU) is an antineoplastic drug used to treat colorectal cancer, but it causes, among other adverse effects, diarrhea and mucositis, as well as enteric neuropathy, as shown in experimental animals. It might also cause neuropathic pain and alterations in visceral sensitivity, but this has not been studied in either patients or experimental animals. Cannabinoids have antimotility and analgesic effects and may alleviate 5-FU-induced adverse effects. Our aim was to evaluate the effects of the cannabinoid agonist WIN 55,212-2 on neuropathic and visceral pain induced by a non-diarrheagenic dose of 5-FU. Male Wistar rats received a dose of 5-FU (150 mg/kg, ip) and gastrointestinal motility, colonic sensitivity, gut wall structure and tactile sensitivity were evaluated. WIN 55,212-2 (WIN) was administered to evaluate its effect on somatic (50–100 µg ipl; 1 mg/kg, ip) and visceral (1 mg/kg, ip) sensitivity. The cannabinoid tetrad was used to assess the central effects of WIN (1 mg/kg, ip). 5-FU decreased food intake and body weight gain, produced mucositis and thermal hyperalgesia, but these effects were reduced afterwards, and were not accompanied by diarrhea. Tactile mechanical allodynia was also evident and persisted for 15 days. Interestingly, it was alleviated by WIN. 5-FU tended to increase colonic sensitivity whereas WIN reduced the abdominal contractions induced by increasing intracolonic pressure in both control and 5-FU-treated animals. Importantly, the alleviating effects of WIN against those induced by 5-FU were not accompanied by any effect in the cannabinoid tetrad. The activation of the peripheral cannabinoid system may be useful to alleviate neuropathic and visceral pain associated with antitumoral treatment.
Published: 2023

16. Pharmacokinetics of Cannabidiol Following Intranasal, Intrarectal, and Oral Administration in Healthy Dogs

Author: Polidoro, Dakir, Temmerman, Robin, Devreese, Mathias, Charalambous, Marios, Ham, Luc Van, Cornelis, Ine, Broeckx, Bart J G, Mandigers, Paul J J, Fischer, Andrea, Storch, Jan, Bhatti, Sofie F M, Polidoro, Dakir, Temmerman, Robin, Devreese, Mathias, Charalambous, Marios, Ham, Luc Van, Cornelis, Ine, Broeckx, Bart J G, Mandigers, Paul J J, Fischer, Andrea, Storch, Jan, and Bhatti, Sofie F M
Abstract: The therapeutic potential of cannabidiol (CBD), a non-psychtropic component of the Cannabis sativa plant, is substantiated more and more. We aimed to determine the pharmacokinetic behavior of CBD after a single dose via intranasal (IN) and intrarectal (IR) administration in six healthy Beagle dogs age 3-8 years old, and compare to the oral administration route (PO). Standardized dosages applied for IN, IR and PO were 20, 100, and 100 mg, respectively. Each dog underwent the same protocol but received CBD through a different administration route. CBD plasma concentrations were determined by ultra-high performance liquid chromatography-tandem mass spectrometry before and at fixed time points after administration. Non-compartmental analysis was performed on the plasma concentration-time profiles. Plasma CBD concentrations after IR administration were below the limit of quantification. The mean area under the curve (AUC) after IN and PO CBD administration was 61 and 1,376 ng/mL*h, respectively. The maximal plasma CBD concentration (C max) after IN and PO CBD administration was 28 and 217 ng/mL reached after 0.5 and 3.5 h (T max), respectively. Significant differences between IN and PO administration were found in the T max ( p = 0.04). Higher AUC and C max were achieved with 100 mg PO compared to 20 mg IN, but no significant differences were found when AUC ( p = 0.09) and C max ( p = 0.44) were normalized to 1 mg dosages. IN administration of CBD resulted in faster absorption when compared to PO administration. However, PO remains the most favorable route for CBD delivery due to its more feasible administration. The IR administration route is not advised for clinical application.
Published: 2022

17. Endocannabinoid signaling in glioma

Author: Costas Insua, Carlos, Guzmán, Manuel, Costas Insua, Carlos, and Guzmán, Manuel
Abstract: CRUE-CSIC (Acuerdos Transformativos 2022), High-grade gliomas constitute the most frequent and aggressive form of primarybrain cancer in adults. These tumors express cannabinoid CB1and CB2receptors, aswell as other elements of the endocannabinoid system. Accruing preclinical evidencesupports that pharmacological activation of cannabinoid receptors located on gliomacells exerts overt anti-tumoral effects by modulating key intracellular signaling path-ways. The mechanism of this cannabinoid receptor-evoked anti-tumoral activity inexperimental models of glioma is intricate and may involve an inhibition not only ofcancer cell survival/proliferation, but also of invasiveness, angiogenesis, and the stemcell-like properties of cancer cells, thereby affecting the complex tumor microenvi-ronment. However, the precise biological role of the endocannabinoid system in thegeneration and progression of glioma seems very context-dependent and remainslargely unknown. Increasing our basic knowledge on how (endo)cannabinoids act onglioma cells could help to optimize experimental cannabinoid-based anti-tumoraltherapies, as well as the preliminary clinical testing that is currently underway., Ministerio de Ciencia e Innovación (MICINN)/FEDER, Instituto de Salud Carlos III (ISCIII), Ministerio de Universidades, Depto. de Bioquímica y Biología Molecular, Fac. de Ciencias Químicas, TRUE, pub
Published: 2022

18. Epidemiology of ∆8THC-related carcinogenesis in USA: A panel regression and causal inferential study

Author: Reece, Albert Stuart, Hulse, Gary Kenneth, Reece, Albert Stuart, and Hulse, Gary Kenneth
Abstract: The use of ∆8THC is increasing at present across the USA in association with widespread cannabis legalization and the common notion that it is “legal weed”. As genotoxic actions have been described for many cannabinoids, we studied the cancer epidemiology of ∆8THC. Data on 34 cancer types was from the Centers for Disease Control Atlanta Georgia, substance abuse data from the Substance Abuse and Mental Health Services Administration, ethnicity and income data from the U.S. Census Bureau, and cannabinoid concentration data from the Drug Enforcement Agency, were combined and processed in R. Eight cancers (corpus uteri, liver, gastric cardia, breast and post-menopausal breast, anorectum, pancreas, and thyroid) were related to ∆8THC exposure on bivariate testing, and 18 (additionally, stomach, Hodgkins, and Non-Hodgkins lymphomas, ovary, cervix uteri, gall bladder, oropharynx, bladder, lung, esophagus, colorectal cancer, and all cancers (excluding non-melanoma skin cancer)) demonstrated positive average marginal effects on fully adjusted inverse probability weighted interactive panel regression. Many minimum E-Values (mEVs) were infinite. p-values rose from 8.04 × 10−78. Marginal effect calculations revealed that 18 ∆8THCrelated cancers are predicted to lead to a further 8.58 cases/100,000 compared to 7.93 for alcoholism and −8.48 for tobacco. Results indicate that between 8 and 20/34 cancer types were associated with ∆8THC exposure, with very high effect sizes (mEVs) and marginal effects after adjustment exceeding tobacco and alcohol, fulfilling the epidemiological criteria of causality and suggesting a cannabinoid class effect. The inclusion of pediatric leukemias and testicular cancer herein demonstrates heritable malignant teratogenesis.
Published: 2022

19. Drug Addiction - the Research & the Researchers: The Lasting Impact of Adolescent Nicotine and Cannabinoid Exposure and The Importance of Effectively Supporting Historically Marginalized Scientists

Author: Dukes, Angeline, Fowler, Christie D1, Dukes, Angeline, Dukes, Angeline, Fowler, Christie D1, and Dukes, Angeline
Abstract: In the past decade overall, there have been increases in adolescent nicotine and cannabinoid use. Yet the long-term implications of this drug exposure, in particular the co-exposure of both of these drugs, on cognition, reward-related behaviors, later drug intake, and relapse-related behaviors is largely understudied. This dissertation explores the novel studies conducted to assess the long-term implications of adolescent nicotine and cannabinoid exposure. Using various behavioral paradigms and intravenous nicotine self-administration in a mouse model, we have shown that adolescent exposure to a cannabinoid or co-exposure to both nicotine and a cannabinoid alters anxiety-related behaviors, cognitive flexibility, natural reward consumption, and nicotine intake in a sex-dependent manner (Pushkin et al. 2019 and Dukes et al. 2020). Moreover, we have shown that adolescent drug exposure can alter the responsivity to cue-induced drug seeking later in life (Dukes et al. 2022 in prep). The final chapter of this dissertation branches off into a more global perspective focusing on the importance of proper mentorship and support for people from historically marginalized backgrounds in the field of neuroscience (Dukes 2020, Singleton et al. 2020, and Singleton et al. 2021).
Published: 2022

20. Epidemiology of ∆8THC-related carcinogenesis in USA: A panel regression and causal inferential study

Author: Reece, Albert Stuart, Hulse, Gary Kenneth, Reece, Albert Stuart, and Hulse, Gary Kenneth
Abstract: The use of ∆8THC is increasing at present across the USA in association with widespread cannabis legalization and the common notion that it is “legal weed”. As genotoxic actions have been described for many cannabinoids, we studied the cancer epidemiology of ∆8THC. Data on 34 cancer types was from the Centers for Disease Control Atlanta Georgia, substance abuse data from the Substance Abuse and Mental Health Services Administration, ethnicity and income data from the U.S. Census Bureau, and cannabinoid concentration data from the Drug Enforcement Agency, were combined and processed in R. Eight cancers (corpus uteri, liver, gastric cardia, breast and post-menopausal breast, anorectum, pancreas, and thyroid) were related to ∆8THC exposure on bivariate testing, and 18 (additionally, stomach, Hodgkins, and Non-Hodgkins lymphomas, ovary, cervix uteri, gall bladder, oropharynx, bladder, lung, esophagus, colorectal cancer, and all cancers (excluding non-melanoma skin cancer)) demonstrated positive average marginal effects on fully adjusted inverse probability weighted interactive panel regression. Many minimum E-Values (mEVs) were infinite. p-values rose from 8.04 × 10−78. Marginal effect calculations revealed that 18 ∆8THCrelated cancers are predicted to lead to a further 8.58 cases/100,000 compared to 7.93 for alcoholism and −8.48 for tobacco. Results indicate that between 8 and 20/34 cancer types were associated with ∆8THC exposure, with very high effect sizes (mEVs) and marginal effects after adjustment exceeding tobacco and alcohol, fulfilling the epidemiological criteria of causality and suggesting a cannabinoid class effect. The inclusion of pediatric leukemias and testicular cancer herein demonstrates heritable malignant teratogenesis.
Published: 2022

21. Synthetic Cannabinoids in Prisons: Content Analysis of TikToks.

Author: McMann, Tiana J, McMann, Tiana J, Calac, Alec, Nali, Matthew, Cuomo, Raphael, Maroulis, James, Mackey, Tim K, McMann, Tiana J, McMann, Tiana J, Calac, Alec, Nali, Matthew, Cuomo, Raphael, Maroulis, James, and Mackey, Tim K
Abstract: BackgroundSynthetic cannabinoids are a significant public health concern, especially among incarcerated populations due to increased reports of abuse. Recent news reports have highlighted the severe consequences of K2/Spice, a synthetic cannabinoid, among the prison population in the United States. Despite regulations against cell phone use, inmates use TikTok to post K2/Spice-related content.ObjectiveThis study aimed to examine TikTok posts for use and illicit distribution of psychoactive substances (eg, K2/Spice) among incarcerated populations.MethodsThe study collected TikTok videos associated with the #k2spice hashtag and used a data collection approach similar to snowball sampling. Inductive coding was used to conduct content analysis of video characteristics. Videos were manually annotated to generate binary classifications related to the use of K2/Spice as well as selling and buying activities associated with it. Statistical analysis was used to determine associations between a video's user engagement and an intent to buy or sell K2/Spice.ResultsA total of 89 TikTok videos with the hashtag #k2spice were manually coded, with 40% (n=36) identified as displaying the use, solicitation, or adverse effects of K2/Spice among the prison population. Of them, 44.44% (n=16) were in a prison-based setting documenting adverse effects including possible overdose. Videos with higher user engagement were positively correlated with comments indicating an intent to buy or sell K2/Spice.ConclusionsK2/Spice is a drug subject to abuse among prison inmates in the United States, including depictions of its harmful effects being recorded and shared on TikTok. Lack of policy enforcement on TikTok and the need for better access to treatment services within the prison system may be exacerbating substance use among this highly vulnerable population. Minimizing the potential individual harm of this content on the incarcerated population should be a priority for social media platforms and
Published: 2022

22. Cannabinol inhibits oxytosis/ferroptosis by directly targeting mitochondria independently of cannabinoid receptors.

Author: Liang, Zhibin, Liang, Zhibin, Soriano-Castell, David, Kepchia, Devin, Duggan, Brendan M, Currais, Antonio, Schubert, David, Maher, Pamela, Liang, Zhibin, Liang, Zhibin, Soriano-Castell, David, Kepchia, Devin, Duggan, Brendan M, Currais, Antonio, Schubert, David, and Maher, Pamela
Abstract: The oxytosis/ferroptosis regulated cell death pathway recapitulates many features of mitochondrial dysfunction associated with the aging brain and has emerged as a potential key mediator of neurodegeneration. It has thus been proposed that the oxytosis/ferroptosis pathway can be used to identify novel drug candidates for the treatment of age-associated neurodegenerative diseases that act by preserving mitochondrial function. Previously, we identified cannabinol (CBN) as a potent neuroprotector. Here, we demonstrate that not only does CBN protect nerve cells from oxytosis/ferroptosis in a manner that is dependent on mitochondria and it does so independently of cannabinoid receptors. Specifically, CBN directly targets mitochondria and preserves key mitochondrial functions including redox regulation, calcium uptake, membrane potential, bioenergetics, biogenesis, and modulation of fusion/fission dynamics that are disrupted following induction of oxytosis/ferroptosis. These protective effects of CBN are at least partly mediated by the promotion of endogenous antioxidant defenses and the activation of AMP-activated protein kinase (AMPK) signaling. Together, our data highlight the potential of mitochondrially-targeted compounds such as CBN as novel oxytotic/ferroptotic inhibitors to rescue mitochondrial dysfunction as well as opportunities for the discovery and development of future neurotherapeutics.
Published: 2022

23. Epidemiology of ∆8THC-related carcinogenesis in USA: A panel regression and causal inferential study

Author: Reece, Albert Stuart, Hulse, Gary Kenneth, Reece, Albert Stuart, and Hulse, Gary Kenneth
Abstract: The use of ∆8THC is increasing at present across the USA in association with widespread cannabis legalization and the common notion that it is “legal weed”. As genotoxic actions have been described for many cannabinoids, we studied the cancer epidemiology of ∆8THC. Data on 34 cancer types was from the Centers for Disease Control Atlanta Georgia, substance abuse data from the Substance Abuse and Mental Health Services Administration, ethnicity and income data from the U.S. Census Bureau, and cannabinoid concentration data from the Drug Enforcement Agency, were combined and processed in R. Eight cancers (corpus uteri, liver, gastric cardia, breast and post-menopausal breast, anorectum, pancreas, and thyroid) were related to ∆8THC exposure on bivariate testing, and 18 (additionally, stomach, Hodgkins, and Non-Hodgkins lymphomas, ovary, cervix uteri, gall bladder, oropharynx, bladder, lung, esophagus, colorectal cancer, and all cancers (excluding non-melanoma skin cancer)) demonstrated positive average marginal effects on fully adjusted inverse probability weighted interactive panel regression. Many minimum E-Values (mEVs) were infinite. p-values rose from 8.04 × 10−78. Marginal effect calculations revealed that 18 ∆8THCrelated cancers are predicted to lead to a further 8.58 cases/100,000 compared to 7.93 for alcoholism and −8.48 for tobacco. Results indicate that between 8 and 20/34 cancer types were associated with ∆8THC exposure, with very high effect sizes (mEVs) and marginal effects after adjustment exceeding tobacco and alcohol, fulfilling the epidemiological criteria of causality and suggesting a cannabinoid class effect. The inclusion of pediatric leukemias and testicular cancer herein demonstrates heritable malignant teratogenesis.
Published: 2022

24. Data to accompany: European epidemiological patterns of cannabis- and substance- related uronephrological congenital anomalies: Space-time and causal inferential study

Author: Reece, Albert and Reece, Albert
Abstract: Data to accompany paper of same title
Published: 2022

25. Data for: Epidemiological patterns of cannabis- and substance- related general congenital anomalies across Europe 2010-2019: Space-time and causal inference study

Author: Reece, Albert and Reece, Albert
Abstract: Data accompany paper of the same title.
Published: 2022

26. Data to accompany : European epidemiological patterns of cannabis- and substance- related body wall congenital anomalies: Space-time and causal inferential study

Author: Reece, Albert and Reece, Albert
Abstract: Data accompany paper of same title.
Published: 2022

27. Data to accompany: Epigenomic and other evidence for cannabis-induced aging contextualized in a synthetic epidemiologic overview of cannabinoid-related teratogenesis and cannabinoid-related carcinogenesis

Author: Reece, Albert and Reece, Albert
Abstract: Data accompany the paper of the same title.
Published: 2022

28. Data to accompany: Epidemiological patterns of cannabis- and substance- related congenital orofacial anomalies across Europe 2010-2019: Space-time and causal inference study

Author: Reece, Albert and Reece, Albert
Abstract: Data accompany paper of the same title.
Published: 2022

29. Data to accompany: European epidemiological patterns of cannabis- and substance- related chromosomal congenital anomalies: Space-time and causal inferential study

Author: Reece, Albert and Reece, Albert
Abstract: Data to accompany paper of the same title.
Published: 2022

30. Editorial: Cannabinoids as potential treatment for neurological diseases

Author: Gómez-Cañas, María, Morales, Paula, Satta, V., Rodríguez-Cueto, Carmen, García, Concepción, Sagredo, Onintza, Gómez-Cañas, María, Morales, Paula, Satta, V., Rodríguez-Cueto, Carmen, García, Concepción, and Sagredo, Onintza
Abstract: descripción no proporcionada por scopus
Published: 2022

31. Cannabis- and substance-related epidemiological patterns of chromosomal congenital anomalies in Europe: Geospatiotemporal and causal inferential study

Author: Reece, Albert Stuart, Hulse, Gary Kenneth, Reece, Albert Stuart, and Hulse, Gary Kenneth
Abstract: Introduction: Laboratory data link cannabinoid exposure to chromosomal mis-segregation errors. Recent epidemiological reports confirm this link and raise concern that elevated chromosomal congenital anomaly rates (CCAR) may be occurring in Europe which is experiencing increased cannabis use, daily intensity of use and cannabinoid potency. Methods: CCAR data from Eurocat. Drug use data from the European Monitoring Centre for Drugs and Drug Addiction. Income from World Bank. Bivariate, multivariate, panel and geotemporospatial regressions analyzed. Inverse probability weighting of panel models and E-values used as major quantitative causal inferential methodologies. Results: In countries where daily cannabis use was rising the trend for CCA’s was upwards whereas in those where daily use was declining it was usually downwards (p = 0.0002). In inverse probability weighted panel models terms for cannabis metrics were significant for chromosomal disorders, trisomies 21 and 13 and Klinefelters syndrome from p < 2.2 × 10−16. In spatiotemporal models cannabis terms were positive and significant for chromosomal disorders, genetic disorders, trisomies 21, 18 and 13, Turners and Klinefelters syndromes from 4.28 × 10−6, 5.79 × 10−12, 1.26 × 10−11, 1.12 × 10−7, 7.52 × 10−9, 7.19 × 10−7 and 7.27 × 10−7. 83.7% of E-value estimates and 74.4% of minimum E-values (mEV) > 9 including four values each at infinity. Considering E-values: the sensitivity of the individual disorders was trisomy 13 > trisomy 21 > Klinefelters > chromosomal disorders > Turners > genetic syndromes > trisomy 18 with mEV’s 1.91 × 1025 to 59.31; and daily cannabis use was the most powerful covariate (median mEV = 1.91 × 1025). Conclusions: Data indicate that, consistent with reports from Hawaii, Canada, Colorado, Australia and USA, CCARs are causally and spatiotemporally related to metrics and intensity of cannabis exposure, directly impact 645 MB (21.5%) of the human genome and may implicate epigenomic-centrosom
Published: 2022

32. Epidemiological patterns of cannabis- and substance- related congenital uronephrological anomalies in Europe: Geospatiotemporal and causal inferential study

Author: Reece, Albert Stuart, Hulse, Gary Kenneth, Reece, Albert Stuart, and Hulse, Gary Kenneth
Abstract: Introduction: Recent reports linking prenatal and community cannabis exposure to elevated uronephrological congenital anomaly (UCA) rates (UCAR’s) raise the question of its European epidemiology given recent increases in community cannabinoid penetration there. Methods: UCAR data from Eurocat. Drug use data from European Monitoring Centre for Drugs and Drug Addiction. Income from World bank. Results: UCAR increased across Spain, Netherlands, Poland and France. UCAR’s and cannabis resin THC increased simultaneously in France, Spain, Netherlands and Bulgaria. At bivariate analysis all UCA’s were related to cannabis herb and resin THC concentrations. All UCAR’s were bivariately related to cannabis metrics ordered by median minimum E-value (mEV) as hypospadias > multicystic renal disease > bilateral renal agenesis > UCA’s > hydronephrosis > posterior urethral valve > bladder exstrophy/epispadias. At inverse probability weighted multivariable analysis terms including cannabis were significant for the following series of anomalies: UCA’s, multicystic renal disease, bilateral renal agenesis, hydronephrosis, congenital posterior urethral valves from P = 1.91 × 10−5, 2.61 × 10−8, 4.60 × 10−15, 4.60 × 10−15 and 2.66 × 10−10. At geospatial analysis the same series of UCA’s were significantly related to cannabis from P = 7.84 × 10−15, 7.72 × 10−5, 0.0023, 6.95 × 10−5, and 8.82 × 10−5. 45/51 (88.2%) of E-value estimates and 31/51 (60.8%) of mEV’s >9. Conclusion: Analysis confirms a close relationship between cannabis metrics and all seven UCA’s and fulfill formal criteria for quantitative causal inference. Given the exponential cannabinoid genotoxicity dose–response relationship results provide a powerful stimulus to constrain community cannabinoid exposure including protection of the food chain to preserve the genome and epigenome of coming generations.
Published: 2022

33. Oral cannabidiol for prevention of acute and transient chemotherapy-induced peripheral neuropathy

Author: Nielsen, Sebastian W., Hasselsteen, Simone Dyring, Dominiak, Helena Sylow Heilmann, Labudovic, Dejan, Reiter, Lars, Dalton, Susanne Oksbjerg, Herrstedt, Jørn, Nielsen, Sebastian W., Hasselsteen, Simone Dyring, Dominiak, Helena Sylow Heilmann, Labudovic, Dejan, Reiter, Lars, Dalton, Susanne Oksbjerg, and Herrstedt, Jørn
Abstract: Purpose: To assess the safety, dosing, and preventive effects of cannabidiol (CBD) on chemotherapy-induced peripheral neuropathy (CIPN) in patients receiving oxaliplatin- or paclitaxel-based chemotherapy. Methods: Patients with cancer scheduled to undergo treatment with carboplatin and paclitaxel (Carbo-Tax) or capecitabine and oxaliplatin (CAPOX) received 150 mg CBD oil twice daily (300 mg/daily) for 8 days beginning 1 day before initiation of chemotherapy. Ten CIPN-specific patient-reported outcome (PRO) measures were captured at baseline and each day after the first cycle of chemotherapy for 8 days. Multi-frequency vibrometry (MF-V) was captured at baseline and day 4 ± 1 after initiation of chemotherapy. Controls were obtained from a similar patient cohort that did not receive CBD. Adverse events were captured using the CTCAE ver. 4.03. Results: From March to December 2021, 54 patients were recruited. CBD-treated patients were significantly older (p = 0.013/0.037, CAPOX/Carbo-Tax) compared to controls. Patients receiving CBD and CAPOX or Carbo-Tax showed significantly lower (better) change in Z-scores in high-frequency MF-V (125 and 250 Hz) compared to controls. This difference was most pronounced for patients receiving Carbo-Tax (− 1.76, CI-95 = [− 2.52; − 1.02] at 250 Hz). CAPOX patients treated with CBD had significantly lower peak baseline-adjusted difference in three PRO items on cold sensitivity to touch, discomfort swallowing cold liquids, and throat discomfort (− 2.08, − 2.06, and − 1.81, CI-95 = [− 3.89; − 0.12], NRS 0–10). No significant differences in PRO items were found for patients receiving Carbo-Tax. Possible side effects included stomach pain (grades 1–2) for patients receiving CAPOX. Conclusion: CBD attenuated early symptoms of CIPN with no major safety concerns. Long-term follow-up is ongoing. Results should be confirmed in a larger, randomized study. Trial registration number: NCT 04,167,319 (U.S National Library of Medicine; ClinicalTrials
Published: 2022

34. A geospatiotemporal and causal inference epidemiological exploration of substance and cannabinoid exposure as drivers of rising US pediatric cancer rates

Author: Reece, Albert S., Hulse, Gary K., Reece, Albert S., and Hulse, Gary K.
Abstract: Background: Age-adjusted US total pediatric cancer incidence rates (TPCIR) rose 49% 1975–2015 for unknown reasons. Prenatal cannabis exposure has been linked with several pediatric cancers which together comprise the majority of pediatric cancer types. We investigated whether cannabis use was related spatiotemporally and causally to TPCIR. Methods: State-based age-adjusted TPCIR data was taken from the CDC Surveillance, Epidemiology and End Results cancer database 2003–2017. Drug exposure was taken from the nationally-representative National Survey of Drug Use and Health, response rate 74.1%. Drugs included were: tobacco, alcohol, cannabis, opioid analgesics and cocaine. This was supplemented by cannabinoid concentration data from the Drug Enforcement Agency and ethnicity and median household income data from US Census. Results: TPCIR rose while all drug use nationally fell, except for cannabis which rose. TPCIR in the highest cannabis use quintile was greater than in the lowest (β-estimate = 1.31 (95%C.I. 0.82, 1.80), P = 1.80 × 10− 7) and the time:highest two quintiles interaction was significant (β-estimate = 0.1395 (0.82, 1.80), P = 1.00 × 10− 14). In robust inverse probability weighted additive regression models cannabis was independently associated with TPCIR (β-estimate = 9.55 (3.95, 15.15), P = 0.0016). In interactive geospatiotemporal models including all drug, ethnic and income variables cannabis use was independently significant (β-estimate = 45.67 (18.77, 72.56), P = 0.0009). In geospatial models temporally lagged to 1,2,4 and 6 years interactive terms including cannabis were significant. Cannabis interactive terms at one and two degrees of spatial lagging were significant (from β-estimate = 3954.04 (1565.01, 6343.09), P = 0.0012). The interaction between the cannabinoids THC and cannabigerol was significant at zero, 2 and 6 years lag (from β-estimate = 46.22 (30.06, 62.38), P = 2.10 × 10− 8). Cannabis legalization was associated with higher TPCIR (β-est
Published: 2021

35. Effects of systemic endocannabinoid manipulation on social and exploratory behavior in prairie voles (Microtus ochrogaster).

Author: Simmons, Trenton C, Simmons, Trenton C, Singh, Alexis LK, Bales, Karen L, Simmons, Trenton C, Simmons, Trenton C, Singh, Alexis LK, and Bales, Karen L
Abstract: RationaleAnandamide is an endocannabinoid that contributes to certain aspects of social behavior, like play and reward, by binding to cannabinoid receptor type 1 (CB1). Most interesting is the recent discovery that anandamide may be mobilized by oxytocin receptor activation under certain contexts, particularly in the nucleus accumbens.ObjectivesGiven the established role of oxytocin and the nucleus accumbens in the neurobiology of pair-bonding, we investigated whether systemic administration of brain-permeable modulators of the endocannabinoid system could alter preferential partner contact in both male and female prairie voles.MethodsSpecifically, we tested whether intraperitoneal administration of the neutral CB1 antagonist AM4113 (4.0-16.0 mg/kg) or the anandamide hydrolysis inhibitor URB597 (5.0-20.0 mg/kg) could prevent or facilitate partner preference formation, respectively. To further investigate the specificity of effects on partner preference, we repeated our URB597 dosing regimen on an additional group of females and tested their anxiety-related behavior in both an elevated-plus maze and a light/dark test.ResultsAM4113 administration had no effect on partner preference. But while URB597 also had no effect on partner preference, low-dose females did increase absolute preferential contact with either the partner or the stranger; individual females spent significant contact time with either the partner or the stranger. None of our outcome measures in either anxiety test showed significant effects of treatment.ConclusionsOur results reveal that experimentally increasing anandamide levels in female prairie voles can increase social contact with both a familiar and novel male via unknown mechanisms that are likely separate from anxiety reduction.
Published: 2021

36. Identification of BiP as a CB1 receptor- interacting protein that fine-tunes cannabinoid signaling in the mouse brain

Author: Farmacología, Farmakologia, Costas-Insua, Carlos, Moreno, Estefanía, Maroto, Irene B., Ruiz-Calvo, Andrea, Bajo-Grañeras, Raquel, Martín-Gutiérrez, David, Díez Alarcia, Rebeca, Vilaró, M. Teresa, Cortés, Roser, García-Font, Nuria, Martín, Ricardo, Espina, Marc, Botta, Joaquín, Ginés, Silvia, McCormick, Peter J., Sánchez-Prieto, José, Galve-Roperh, Ismael, Mengod, Guadalupe, Urigüen Echeverría, Leyre, Marsicano, Giovanni, Bellocchio, Luigi, Canela, Enric I., Casadó, Vicent, Rodríguez-Crespo, Ignacio, Guzmán, Manuel, Farmacología, Farmakologia, Costas-Insua, Carlos, Moreno, Estefanía, Maroto, Irene B., Ruiz-Calvo, Andrea, Bajo-Grañeras, Raquel, Martín-Gutiérrez, David, Díez Alarcia, Rebeca, Vilaró, M. Teresa, Cortés, Roser, García-Font, Nuria, Martín, Ricardo, Espina, Marc, Botta, Joaquín, Ginés, Silvia, McCormick, Peter J., Sánchez-Prieto, José, Galve-Roperh, Ismael, Mengod, Guadalupe, Urigüen Echeverría, Leyre, Marsicano, Giovanni, Bellocchio, Luigi, Canela, Enric I., Casadó, Vicent, Rodríguez-Crespo, Ignacio, and Guzmán, Manuel
Abstract: Cannabinoids, the bioactive constituents of cannabis, exert a wide array of effects on the brain by engaging Type 1 cannabinoid receptor (CB1R). Accruing evidence supports that cannabinoid action relies on context-dependent factors, such as the biological characteristics of the target cell, suggesting that cell population-intrinsic molecular cues modulate CB1R-dependent signaling. Here, by using a yeast two-hybrid-based high-throughput screening, we identified BiP as a potential CB1R-interacting protein. We next found that CB1R and BiP interact specifically in vitro, and mapped the interaction site within the CB1R C-terminal (intracellular) domain and the BiP C-terminal (substrate-binding) domain-alpha. BiP selectively shaped agonist-evoked CB1R signaling by blocking an "alternative" Gq/11 protein-dependent signaling module while leaving the "classical" Gi/o protein-dependent inhibition of the cAMP pathway unaffected. In situ proximity ligation assays conducted on brain samples from various genetic mouse models of conditional loss or gain of CB1R expression allowed to map CB1R-BiP complexes selectively on terminals of GABAergic neurons. Behavioral studies using cannabinoid-treated male BiP+/- mice supported that CB1R-BiP complexes modulate cannabinoid-evoked anxiety, one of the most frequent undesired effects of cannabis. Together, by identifying BiP as a CB1R-interacting protein that controls receptor function in a signaling pathway- and neuron population-selective manner, our findings may help to understand the striking context-dependent actions of cannabis in the brain.SIGNIFICANCE STATEMENT Cannabis use is increasing worldwide, so innovative studies aimed to understand its complex mechanism of neurobiological action are warranted. Here, we found that cannabinoid CB1 receptor (CB1R), the primary molecular target of the bioactive constituents of cannabis, interacts specifically with an intracellular protein called BiP. The interaction between CB1R and BiP occurs s
Published: 2021

37. Dopaminergic Denervation Impairs Cortical Motor and Associative/Limbic Information Processing Through the Basal Ganglia and its Modulation by the CB1 Receptor

Author: Farmacología, Neurociencias, Farmakologia, Neurozientziak, Antonazzo Soler, Mario, Gómez Urquijo, Sonia María, Ugedo Urruela, Luisa, Morera Herreras, Teresa, Farmacología, Neurociencias, Farmakologia, Neurozientziak, Antonazzo Soler, Mario, Gómez Urquijo, Sonia María, Ugedo Urruela, Luisa, and Morera Herreras, Teresa
Abstract: The basal ganglia (BG) are involved in cognitive/motivational functions in addition to movement control. Thus, BG segregated circuits, the sensorimotor (SM) and medial prefrontal (mPF) circuits, process different functional domains, such as motor and cognitive/motivational behaviours, respectively. With a high presence in the BG, the CB1 cannabinoid receptor modulates BG circuits. Furthermore, dopamine (DA), one of the principal neurotransmitters in the BG, also plays a key role in circuit functionality. Taking into account the interaction between DA and the endocannabinoid system at the BG level, we investigated the functioning of BG circuits and their modulation by the CB1 receptor under DA-depleted conditions. We performed single-unit extracellular recordings of substantia nigra pars reticulata (SNr) neurons with simultaneous cortical stimulation in sham and 6-hydroxydopamine (6-OHDA)-lesioned rats, together with immunohistochemical assays. We showed that DA loss alters cortico-nigral information processing in both circuits, with a predominant transmission through the hyperdirect pathway in the SM circuit and an increased transmission through the direct pathway in the mPF circuit. Moreover, although DA denervation does not change CB1 receptor density, it impairs its functionality, leading to a lack of modulation. These data highlight an abnormal transfer of information through the associative/limbic domains after DA denervation that may be related to the non-motor symptoms manifested by Parkinson's disease patients.
Published: 2021

38. Cannabidiol and Neurodevelopmental Disorders in Children

Author: Kwan Cheung, Keith A., Mitchell, Murray D., Heussler, Helen S., Kwan Cheung, Keith A., Mitchell, Murray D., and Heussler, Helen S.
Abstract: Neurodevelopmental and neuropsychiatric disorders (such as autism spectrum disorder) have broad health implications for children, with no definitive cure for the vast majority of them. However, recently medicinal cannabis has been successfully trialled as a treatment to manage many of the patients' symptoms and improve quality of life. The cannabinoid cannabidiol, in particular, has been reported to be safe and well-tolerated with a plethora of anticonvulsant, anxiolytic and anti-inflammatory properties. Lately, the current consensus is that the endocannabinoid system is a crucial factor in neural development and health; research has found evidence that there are a multitude of signalling pathways involving neurotransmitters and the endocannabinoid system by which cannabinoids could potentially exert their therapeutic effects. A better understanding of the cannabinoids' mechanisms of action should lead to improved treatments for neurodevelopmental disorders.
Published: 2021

39. Identification of BiP as a CB1 receptor- interacting protein that fine-tunes cannabinoid signaling in the mouse brain

Author: Farmacología, Farmakologia, Costas-Insua, Carlos, Moreno, Estefanía, Maroto, Irene B., Ruiz-Calvo, Andrea, Bajo-Grañeras, Raquel, Martín-Gutiérrez, David, Díez Alarcia, Rebeca, Vilaró, M. Teresa, Cortés, Roser, García-Font, Nuria, Martín, Ricardo, Espina, Marc, Botta, Joaquín, Ginés, Silvia, McCormick, Peter J., Sánchez-Prieto, José, Galve-Roperh, Ismael, Mengod, Guadalupe, Urigüen Echeverría, Leyre, Marsicano, Giovanni, Bellocchio, Luigi, Canela, Enric I., Casadó, Vicent, Rodríguez-Crespo, Ignacio, Guzmán, Manuel, Farmacología, Farmakologia, Costas-Insua, Carlos, Moreno, Estefanía, Maroto, Irene B., Ruiz-Calvo, Andrea, Bajo-Grañeras, Raquel, Martín-Gutiérrez, David, Díez Alarcia, Rebeca, Vilaró, M. Teresa, Cortés, Roser, García-Font, Nuria, Martín, Ricardo, Espina, Marc, Botta, Joaquín, Ginés, Silvia, McCormick, Peter J., Sánchez-Prieto, José, Galve-Roperh, Ismael, Mengod, Guadalupe, Urigüen Echeverría, Leyre, Marsicano, Giovanni, Bellocchio, Luigi, Canela, Enric I., Casadó, Vicent, Rodríguez-Crespo, Ignacio, and Guzmán, Manuel
Abstract: Cannabinoids, the bioactive constituents of cannabis, exert a wide array of effects on the brain by engaging Type 1 cannabinoid receptor (CB1R). Accruing evidence supports that cannabinoid action relies on context-dependent factors, such as the biological characteristics of the target cell, suggesting that cell population-intrinsic molecular cues modulate CB1R-dependent signaling. Here, by using a yeast two-hybrid-based high-throughput screening, we identified BiP as a potential CB1R-interacting protein. We next found that CB1R and BiP interact specifically in vitro, and mapped the interaction site within the CB1R C-terminal (intracellular) domain and the BiP C-terminal (substrate-binding) domain-alpha. BiP selectively shaped agonist-evoked CB1R signaling by blocking an "alternative" Gq/11 protein-dependent signaling module while leaving the "classical" Gi/o protein-dependent inhibition of the cAMP pathway unaffected. In situ proximity ligation assays conducted on brain samples from various genetic mouse models of conditional loss or gain of CB1R expression allowed to map CB1R-BiP complexes selectively on terminals of GABAergic neurons. Behavioral studies using cannabinoid-treated male BiP+/- mice supported that CB1R-BiP complexes modulate cannabinoid-evoked anxiety, one of the most frequent undesired effects of cannabis. Together, by identifying BiP as a CB1R-interacting protein that controls receptor function in a signaling pathway- and neuron population-selective manner, our findings may help to understand the striking context-dependent actions of cannabis in the brain.SIGNIFICANCE STATEMENT Cannabis use is increasing worldwide, so innovative studies aimed to understand its complex mechanism of neurobiological action are warranted. Here, we found that cannabinoid CB1 receptor (CB1R), the primary molecular target of the bioactive constituents of cannabis, interacts specifically with an intracellular protein called BiP. The interaction between CB1R and BiP occurs s
Published: 2021

40. Dopaminergic Denervation Impairs Cortical Motor and Associative/Limbic Information Processing Through the Basal Ganglia and its Modulation by the CB1 Receptor

Author: Farmacología, Neurociencias, Farmakologia, Neurozientziak, Antonazzo Soler, Mario, Gómez Urquijo, Sonia María, Ugedo Urruela, Luisa, Morera Herreras, Teresa, Farmacología, Neurociencias, Farmakologia, Neurozientziak, Antonazzo Soler, Mario, Gómez Urquijo, Sonia María, Ugedo Urruela, Luisa, and Morera Herreras, Teresa
Abstract: The basal ganglia (BG) are involved in cognitive/motivational functions in addition to movement control. Thus, BG segregated circuits, the sensorimotor (SM) and medial prefrontal (mPF) circuits, process different functional domains, such as motor and cognitive/motivational behaviours, respectively. With a high presence in the BG, the CB1 cannabinoid receptor modulates BG circuits. Furthermore, dopamine (DA), one of the principal neurotransmitters in the BG, also plays a key role in circuit functionality. Taking into account the interaction between DA and the endocannabinoid system at the BG level, we investigated the functioning of BG circuits and their modulation by the CB1 receptor under DA-depleted conditions. We performed single-unit extracellular recordings of substantia nigra pars reticulata (SNr) neurons with simultaneous cortical stimulation in sham and 6-hydroxydopamine (6-OHDA)-lesioned rats, together with immunohistochemical assays. We showed that DA loss alters cortico-nigral information processing in both circuits, with a predominant transmission through the hyperdirect pathway in the SM circuit and an increased transmission through the direct pathway in the mPF circuit. Moreover, although DA denervation does not change CB1 receptor density, it impairs its functionality, leading to a lack of modulation. These data highlight an abnormal transfer of information through the associative/limbic domains after DA denervation that may be related to the non-motor symptoms manifested by Parkinson's disease patients.
Published: 2021

41. Effects of inflammatory pain on CB1 receptor in the midbrain periaqueductal gray.

Author: Wilson-Poe, Adrianne R, Wilson-Poe, Adrianne R, Wiese, Beth, Kibaly, Cherkaouia, Lueptow, Lindsay, Garcia, Jeniffer, Anand, Preeti, Cahill, Catherine, Morón, Jose A, Wilson-Poe, Adrianne R, Wilson-Poe, Adrianne R, Wiese, Beth, Kibaly, Cherkaouia, Lueptow, Lindsay, Garcia, Jeniffer, Anand, Preeti, Cahill, Catherine, and Morón, Jose A
Abstract: IntroductionThe periaqueductal gray (PAG) mediates the antinociceptive properties of analgesics, including opioids and cannabinoids. Administration of either opioids or cannabinoids into the PAG induces antinociception. However, most studies characterizing the antinociceptive properties of cannabinoids in the PAG have been conducted in naive animals. Few studies have reported on the role of CB1 receptors in the PAG during conditions which would prompt the administration of analgesics, namely, during pain states.ObjectivesTo examine inflammatory pain-induced changes in CB1 receptor expression and function in the midbrain periaqueductal gray.MethodsIn this study, we used the Complete Freund Adjuvant model to characterize CB1 receptor expression and G-protein coupling during persistent inflammatory pain.ResultsInflammatory pain induced an upregulation in the expression of synaptic CB1 receptors in the PAG. Despite this pain-induced change in CB1 expression, there was no corresponding upregulation of CB1 mRNA after the induction of inflammatory pain, suggesting a pain-induced recruitment of CB1 receptors to the synaptic sites within PAG neurons or increased coupling efficiency between the receptor and effector systems. Inflammatory pain also enhanced ventrolateral PAG CB1 receptor activity, as there was an increase in CP55,940-stimulated G-protein activation compared with pain-naïve control animals.ConclusionThese findings complement a growing body of evidence which demonstrate pain-induced changes in brain regions that are responsible for both the analgesic and rewarding properties of analgesic pharmacotherapies. Because much of our understanding of the pharmacology of cannabinoids is based on studies which use largely pain-naïve male animals, this work fills in important gaps in the knowledge base by incorporating pain-induced adaptations and cannabinoid pharmacology in females.
Published: 2021

42. Effects of systemic endocannabinoid manipulation on social and exploratory behavior in prairie voles (Microtus ochrogaster).

Author: Simmons, Trenton C, Simmons, Trenton C, Singh, Alexis LK, Bales, Karen L, Simmons, Trenton C, Simmons, Trenton C, Singh, Alexis LK, and Bales, Karen L
Abstract: RationaleAnandamide is an endocannabinoid that contributes to certain aspects of social behavior, like play and reward, by binding to cannabinoid receptor type 1 (CB1). Most interesting is the recent discovery that anandamide may be mobilized by oxytocin receptor activation under certain contexts, particularly in the nucleus accumbens.ObjectivesGiven the established role of oxytocin and the nucleus accumbens in the neurobiology of pair-bonding, we investigated whether systemic administration of brain-permeable modulators of the endocannabinoid system could alter preferential partner contact in both male and female prairie voles.MethodsSpecifically, we tested whether intraperitoneal administration of the neutral CB1 antagonist AM4113 (4.0-16.0 mg/kg) or the anandamide hydrolysis inhibitor URB597 (5.0-20.0 mg/kg) could prevent or facilitate partner preference formation, respectively. To further investigate the specificity of effects on partner preference, we repeated our URB597 dosing regimen on an additional group of females and tested their anxiety-related behavior in both an elevated-plus maze and a light/dark test.ResultsAM4113 administration had no effect on partner preference. But while URB597 also had no effect on partner preference, low-dose females did increase absolute preferential contact with either the partner or the stranger; individual females spent significant contact time with either the partner or the stranger. None of our outcome measures in either anxiety test showed significant effects of treatment.ConclusionsOur results reveal that experimentally increasing anandamide levels in female prairie voles can increase social contact with both a familiar and novel male via unknown mechanisms that are likely separate from anxiety reduction.
Published: 2021

43. Cannabinoid receptor Type 1 densities reflect social organization in Microtus.

Author: Simmons, Trenton C, Simmons, Trenton C, Freeman, Sara M, Lackey, Nicholas S, Dreyer, Brooke K, Manoli, Devanand S, Bales, Karen L, Simmons, Trenton C, Simmons, Trenton C, Freeman, Sara M, Lackey, Nicholas S, Dreyer, Brooke K, Manoli, Devanand S, and Bales, Karen L
Abstract: Across many species, endocannabinoids play an important role in regulating social play, reward, and anxiety. These processes are mediated through at least two distinct cannabinoid receptors (CB), CB1 and CB2. CB1 expression is found in appreciable densities across regions of the brain that integrate memory with socio-spatial information; many of these regions have been directly linked to the neurobiology of pair bonding in monogamous species. Using receptor autoradiography, we provide the first distributional map of CB1 within the brains of closely related monogamous prairie voles and promiscuous meadow voles, and compare receptor densities across sexes and species in limbic regions. We observe CB1-specific signal using [3H] CP-55,940 and [3H] SR141716A, though the latter exhibited a lower signal to noise ratio. We confirmed the presence of CB2 in prairie vole spleen tissue using [3H] CP-55,940. However, we found no evidence of CB2 in the brain using either [3H] CP-55,940 or [3H] A-836,339. The overall distribution of putative CB1 in the brain was similar across vole species and followed the pattern of CB1 expression observed in other species-high intensity binding within the telencephalon, moderate binding within the diencephalon, and mild binding within the mesencephalon and metencephalon (aside from the cerebellar cortex). However, we found profound differences in CB1 densities across species, with prairie voles having higher CB1 binding in regions implicated in social attachment and spatial memory (e.g., periaqueductal gray, hippocampus). These findings suggest that CB1 densities, but not distribution, correlate with the social systems of vole species.
Published: 2021

44. Cannabinoid Receptor Subtype-1 Regulates Allergic Airway Eosinophilia During Lung Helminth Infection.

Author: Wiley, Mark B, Wiley, Mark B, Bobardt, Sarah D, Nordgren, Tara M, Nair, Meera G, DiPatrizio, Nicholas V, Wiley, Mark B, Wiley, Mark B, Bobardt, Sarah D, Nordgren, Tara M, Nair, Meera G, and DiPatrizio, Nicholas V
Abstract: Introduction: Over 1 billion humans carry infectious helminth parasites that can lead to chronic comorbidities such as anemia and growth retardation in children. Helminths induce a T-helper type 2 (Th2) immune response in the host and can cause severe tissue damage and fibrosis if chronic. We recently reported that mice infected with the soil-transmitted helminth, Nippostrongylus brasiliensis, displayed elevated levels of endocannabinoids (eCBs) in the lung and intestine. eCBs are lipid-signaling molecules that control inflammation; however, their function in infection is not well defined. Materials and Methods: A combination of pharmacological approaches and genetic mouse models was used to investigate roles for the eCB system in inflammatory responses and lung injury in mice during parasitic infection with N. brasiliensis. Results: Hemorrhaging of lung tissue in mice infected with N. brasiliensis was exacerbated by inhibiting peripheral cannabinoid receptor subtype-1 (CB1Rs) with the peripherally restricted CB1R antagonist, AM6545. In addition, these mice exhibited an increase in nonfunctional alveolar space and prolonged airway eosinophilia compared to vehicle-treated infected mice. In contrast to mice treated with AM6545, infected cannabinoid receptor subtype-2-null mice (Cnr2-/-) did not display any changes in these parameters compared to wild-type mice. Conclusions: Roles for the eCB system in Th2 immune responses are not well understood; however, increases in its activity in response to infection suggest an immunomodulatory role. Moreover, these findings suggest a role for eCB signaling at CB1Rs but not cannabinoid receptor subtypes-2 in the resolution of Th2 inflammatory responses, which become host destructive over time.
Published: 2021

45. Control of exploration, motor coordination and amphetamine sensitization by cannabinoid CB1 receptors expressed in medium spiny neurons.

Author: Bonm, Alipi V, Bonm, Alipi V, Elezgarai, Izaskun, Gremel, Christina M, Viray, Katie, Bamford, Nigel S, Palmiter, Richard D, Grandes, Pedro, Lovinger, David M, Stella, Nephi, Bonm, Alipi V, Bonm, Alipi V, Elezgarai, Izaskun, Gremel, Christina M, Viray, Katie, Bamford, Nigel S, Palmiter, Richard D, Grandes, Pedro, Lovinger, David M, and Stella, Nephi
Abstract: Activation of cannabinoid 1 receptors (CB1 R) modulates multiple behaviours, including exploration, motor coordination and response to psychostimulants. It is known that CB1 R expressed by either excitatory or inhibitory neurons mediates different behavioural responses to CB1 R activation, yet the involvement of CB1 R expressed by medium spiny neurons (MSNs), the neuronal subpopulation that expresses the highest level of CB1 R in the CNS, remains unknown. We report a new genetically modified mouse line that expresses functional CB1 R in MSN on a CB1 R knockout (KO) background (CB1 R(MSN) mice). The absence of cannabimimetic responses measured in CB1 R KO mice was not rescued in CB1 R(MSN) mice, nor was decreased spontaneous locomotion, impaired instrumental behaviour or reduced amphetamine-triggered hyperlocomotion measured in CB1 R KO mice. Significantly, reduced novel environment exploration of an open field and absence of amphetamine sensitization (AS) measured in CB1 R KO mice were fully rescued in CB1 R(MSN) mice. Impaired motor coordination in CB1 R KO mice measured on the Rotarod was partially rescued in CB1 R(MSN) mice. Thus, CB1 R expressed by MSN control exploration, motor coordination, and AS. Our study demonstrates a new functional roles for cell specific CB1 R expression and their causal link in the control of specific behaviors.
Published: 2021

46. Data to accompany: Cannabinoid- and substance- relationships of European congenital anomaly patterns: A space-time panel regression and causal inferential study

Author: Reece, Albert and Reece, Albert
Abstract: Data accompanies paper of the same name.
Published: 2021

47. Dataset to accompany: Geotemporospatial and causal inferential epidemiological analysis of US survey and overview of cannabis, cannabidiol and cannabinoid genotoxicity expressed in cancer incidence 2003–2017

Author: Reece, Albert and Reece, Albert
Abstract: Data accompanies article of the same title.
Published: 2021

48. Dopaminergic Denervation Impairs Cortical Motor and Associative/Limbic Information Processing Through the Basal Ganglia and its Modulation by the CB1 Receptor

Author: Farmacología, Neurociencias, Farmakologia, Neurozientziak, Antonazzo Soler, Mario, Gómez Urquijo, Sonia María, Ugedo Urruela, Luisa, Morera Herreras, Teresa, Farmacología, Neurociencias, Farmakologia, Neurozientziak, Antonazzo Soler, Mario, Gómez Urquijo, Sonia María, Ugedo Urruela, Luisa, and Morera Herreras, Teresa
Abstract: The basal ganglia (BG) are involved in cognitive/motivational functions in addition to movement control. Thus, BG segregated circuits, the sensorimotor (SM) and medial prefrontal (mPF) circuits, process different functional domains, such as motor and cognitive/motivational behaviours, respectively. With a high presence in the BG, the CB1 cannabinoid receptor modulates BG circuits. Furthermore, dopamine (DA), one of the principal neurotransmitters in the BG, also plays a key role in circuit functionality. Taking into account the interaction between DA and the endocannabinoid system at the BG level, we investigated the functioning of BG circuits and their modulation by the CB1 receptor under DA-depleted conditions. We performed single-unit extracellular recordings of substantia nigra pars reticulata (SNr) neurons with simultaneous cortical stimulation in sham and 6-hydroxydopamine (6-OHDA)-lesioned rats, together with immunohistochemical assays. We showed that DA loss alters cortico-nigral information processing in both circuits, with a predominant transmission through the hyperdirect pathway in the SM circuit and an increased transmission through the direct pathway in the mPF circuit. Moreover, although DA denervation does not change CB1 receptor density, it impairs its functionality, leading to a lack of modulation. These data highlight an abnormal transfer of information through the associative/limbic domains after DA denervation that may be related to the non-motor symptoms manifested by Parkinson's disease patients.
Published: 2021

49. Identification of BiP as a CB1 receptor- interacting protein that fine-tunes cannabinoid signaling in the mouse brain

Author: Farmacología, Farmakologia, Costas-Insua, Carlos, Moreno, Estefanía, Maroto, Irene B., Ruiz-Calvo, Andrea, Bajo-Grañeras, Raquel, Martín-Gutiérrez, David, Díez Alarcia, Rebeca, Vilaró, M. Teresa, Cortés, Roser, García-Font, Nuria, Martín, Ricardo, Espina, Marc, Botta, Joaquín, Ginés, Silvia, McCormick, Peter J., Sánchez-Prieto, José, Galve-Roperh, Ismael, Mengod, Guadalupe, Urigüen Echeverría, Leyre, Marsicano, Giovanni, Bellocchio, Luigi, Canela, Enric I., Casadó, Vicent, Rodríguez-Crespo, Ignacio, Guzmán, Manuel, Farmacología, Farmakologia, Costas-Insua, Carlos, Moreno, Estefanía, Maroto, Irene B., Ruiz-Calvo, Andrea, Bajo-Grañeras, Raquel, Martín-Gutiérrez, David, Díez Alarcia, Rebeca, Vilaró, M. Teresa, Cortés, Roser, García-Font, Nuria, Martín, Ricardo, Espina, Marc, Botta, Joaquín, Ginés, Silvia, McCormick, Peter J., Sánchez-Prieto, José, Galve-Roperh, Ismael, Mengod, Guadalupe, Urigüen Echeverría, Leyre, Marsicano, Giovanni, Bellocchio, Luigi, Canela, Enric I., Casadó, Vicent, Rodríguez-Crespo, Ignacio, and Guzmán, Manuel
Abstract: Cannabinoids, the bioactive constituents of cannabis, exert a wide array of effects on the brain by engaging Type 1 cannabinoid receptor (CB1R). Accruing evidence supports that cannabinoid action relies on context-dependent factors, such as the biological characteristics of the target cell, suggesting that cell population-intrinsic molecular cues modulate CB1R-dependent signaling. Here, by using a yeast two-hybrid-based high-throughput screening, we identified BiP as a potential CB1R-interacting protein. We next found that CB1R and BiP interact specifically in vitro, and mapped the interaction site within the CB1R C-terminal (intracellular) domain and the BiP C-terminal (substrate-binding) domain-alpha. BiP selectively shaped agonist-evoked CB1R signaling by blocking an "alternative" Gq/11 protein-dependent signaling module while leaving the "classical" Gi/o protein-dependent inhibition of the cAMP pathway unaffected. In situ proximity ligation assays conducted on brain samples from various genetic mouse models of conditional loss or gain of CB1R expression allowed to map CB1R-BiP complexes selectively on terminals of GABAergic neurons. Behavioral studies using cannabinoid-treated male BiP+/- mice supported that CB1R-BiP complexes modulate cannabinoid-evoked anxiety, one of the most frequent undesired effects of cannabis. Together, by identifying BiP as a CB1R-interacting protein that controls receptor function in a signaling pathway- and neuron population-selective manner, our findings may help to understand the striking context-dependent actions of cannabis in the brain.SIGNIFICANCE STATEMENT Cannabis use is increasing worldwide, so innovative studies aimed to understand its complex mechanism of neurobiological action are warranted. Here, we found that cannabinoid CB1 receptor (CB1R), the primary molecular target of the bioactive constituents of cannabis, interacts specifically with an intracellular protein called BiP. The interaction between CB1R and BiP occurs s
Published: 2021

50. Inflammatory biomarkers in addictive disorders

Author: Instituto de Salud Carlos III, European Commission, Plan Nacional sobre Drogas (España), Agencia Estatal de Investigación (España), Ministerio de Ciencia, Innovación y Universidades (España), Morcuende, Álvaro, Navarrete, Francisco, Nieto, Elena, Manzanares, Jorge, Nieto, M. Ángela, Instituto de Salud Carlos III, European Commission, Plan Nacional sobre Drogas (España), Agencia Estatal de Investigación (España), Ministerio de Ciencia, Innovación y Universidades (España), Morcuende, Álvaro, Navarrete, Francisco, Nieto, Elena, Manzanares, Jorge, and Nieto, M. Ángela
Abstract: Substance use disorders are a group of diseases that are associated with social, professional, and family impairment and that represent a high socio-economic impact on the health systems of countries around the world. These disorders present a very complex diagnosis and treatment regimen due to the lack of suitable biomarkers supporting the correct diagnosis and classification and the difficulty of selecting effective therapies. Over the last few years, several studies have pointed out that these addictive disorders are associated with systemic and central nervous system inflammation, which could play a relevant role in the onset and progression of these diseases. Therefore, identifying different immune system components as biomarkers of such addictive disorders could be a crucial step to promote appropriate diagnosis and treatment. Thus, this work aims to provide an overview of the immune system alterations that may be biomarkers of various addictive disorders.
Published: 2021

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