358 results on '"Sanna, L"'
Search Results
2. Pre-planned Study Design Adaptations in UNISUS: A Phase 3, Randomized Superiority Study Comparing the Efficacy, Safety, and Tolerability of Macitentan 75 Mg Versus 10 Mg in Patients With Pulmonary Arterial Hypertension (PAH)
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Mclaughlin, V.V., primary, Tamura, Y., additional, Humbert, M.J.C., additional, Backer, A., additional, Boyanova, N., additional, Kracker, H., additional, Larbalestier, A., additional, Sanna, L., additional, and Hoeper, M., additional
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- 2024
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3. The immunological architecture of granulomatous inflammation in central nervous system tuberculosis
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Zaharie, Stefan-Dan, Franken, Daniel J., van der Kuip, Martijn, van Elsland, Sabine, de Bakker, Bernadette S., Hagoort, Jaco, Roest, Sanna L., van Dam, Carmen S., Timmers, Carlie, Solomons, Regan, van Toorn, Ronald, Kruger, Mariana, and Marceline van Furth, A.
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- 2020
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4. Locked nucleic acid: modality, diversity, and drug discovery
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Hagedorn, Peter H., Persson, Robert, Funder, Erik D., Albæk, Nanna, Diemer, Sanna L., Hansen, Dennis J., Møller, Marianne R., Papargyri, Natalia, Christiansen, Helle, Hansen, Bo R., Hansen, Henrik F., Jensen, Mads A., and Koch, Troels
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- 2018
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5. Three-dimensional visualizations from a dataset of immunohistochemical stained serial sections of human brain tissue containing tuberculosis related granulomas
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Stefan-Dan Zaharie, Daniel J. Franken, Martijn van der Kuip, Sabine van Elsland, Bernadette S. de Bakker, Jaco Hagoort, Sanna L. Roest, Carmen S. van Dam, Carlie Timmers, Regan Solomons, Ronald van Toorn, Mariana Kruger, and A. Marceline van Furth
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Central nervous system tuberculosis ,Tuberculous meningitis ,Granuloma ,Rich-focus ,3D-reconstruction ,Computer applications to medicine. Medical informatics ,R858-859.7 ,Science (General) ,Q1-390 - Abstract
This data article presents datasets associated with the research article entitled “The immunological architecture of granulomatous inflammation in central nervous system tuberculosis’’ (Zaharie et al., 2020). The morphology of tuberculosis related granulomas within the central nervous system of human patients was visualized in six different three-dimensional (3D) models. Post-mortem, formalin fixed and paraffin embedded specimens from deceased tuberculous meningitis patients were immunohistochemically stained and 800 serial histologically stained sections were acquired. Images from all sections were obtained with an Olympus BX43 light microscope and structures were identified, labeled and made three-dimensional. The interactive 3D-models allows the user to directly visualize the morphology of the granulomas and to understand the localization of the granulomas. The 3D-models can be used for multiple purposes and provide both an educational source as a gold standard for further animal studies, human research and the development of in silico models on the topic of central nervous system tuberculosis.
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- 2020
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6. Humulone Modulation of GABAA Receptors and Its Role in Hops Sleep-Promoting Activity
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Ali Y. Benkherouf, Kim Eerola, Sanna L. Soini, and Mikko Uusi-Oukari
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GABAA receptors ,humulone ,ethanol ,allosteric modulation ,radioligand binding ,electrophysiology ,Neurosciences. Biological psychiatry. Neuropsychiatry ,RC321-571 - Abstract
Humulus lupulus L. (hops) is a major constituent of beer. It exhibits neuroactive properties that make it useful as a sleeping aid. These effects are hypothesized to be mediated by an increase in GABAA receptor function. In the quest to uncover the constituents responsible for the sedative and hypnotic properties of hops, recent evidence revealed that humulone, a prenylated phloroglucinol derivative comprising 35–70% of hops alpha acids, may act as a positive modulator of GABAA receptors at low micromolar concentrations. This raises the question whether humulone plays a key role in hops pharmacological activity and potentially interacts with other modulators such as ethanol, bringing further enhancement in GABAA receptor-mediated effects of beer. Here we assessed electrophysiologically the positive modulatory activity of humulone on recombinant GABAA receptors expressed in HEK293 cells. We then examined humulone interactions with other active hops compounds and ethanol on GABA-induced displacement of [3H]EBOB binding to native GABAA receptors in rat brain membranes. Using BALB/c mice, we assessed humulone’s hypnotic behavior with pentobarbital- and ethanol-induced sleep as well as sedation in spontaneous locomotion with open field test. We demonstrated for the first time that humulone potentiates GABA-induced currents in α1β3γ2 receptors. In radioligand binding to native GABAA receptors, the inclusion of ethanol enhanced humulone modulation of GABA-induced displacement of [3H]EBOB binding in rat forebrain and cerebellum as it produced a leftward shift in [3H]EBOB displacement curves. Moreover, the additive modulatory effects between humulone, isoxanthohumol and 6-prenylnaringenin were evident and corresponded to the sum of [3H]EBOB displacement by each compound individually. In behavioral tests, humulone shortened sleep onset and increased the duration of sleep induced by pentobarbital and decreased the spontaneous locomotion in open field at 20 mg/kg (i.p.). Despite the absence of humulone effects on ethanol-induced sleep onset, sleep duration was increased dose-dependently down to 10 mg/kg (i.p.). Our findings confirmed humulone’s positive allosteric modulation of GABAA receptor function and displayed its sedative and hypnotic behavior. Humulone modulation can be potentially enhanced by ethanol and hops modulators suggesting a probable enhancement in the intoxicating effects of ethanol in hops-enriched beer.
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- 2020
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7. Post-IR IRSL290 dating of K-rich feldspar sand grains in a wind-dominated system on Sardinia
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Andreucci, S., Sechi, D., Buylaert, J.-P., Sanna, L., and Pascucci, V.
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- 2017
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8. The Influence of AA29504 on GABAA Receptor Ligand Binding Properties and Its Implications on Subtype Selectivity
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Sanna L. Soini, Sylvia Sikstus, Mikko Uusi-Oukari, and Ali Y. Benkherouf
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Agonist ,Allosteric modulator ,Chemistry ,GABAA receptor ,medicine.drug_class ,Ligand binding assay ,Allosteric regulation ,Stimulation ,General Medicine ,Biochemistry ,Cellular and Molecular Neuroscience ,chemistry.chemical_compound ,Muscimol ,medicine ,Biophysics ,Receptor - Abstract
The unique pharmacological properties of δ-containing γ-aminobutyric acid type A receptors (δ-GABAARs) make them an attractive target for selective and persistent modulation of neuronal excitability. However, the availability of selective modulators targeting δ-GABAARs remains limited. AA29504 ([2-amino-4-(2,4,6-trimethylbenzylamino)-phenyl]-carbamic acid ethyl ester), an analog of K+ channel opener retigabine, acts as an agonist and a positive allosteric modulator (Ago-PAM) of δ-GABAARs. Based on electrophysiological studies using recombinant receptors, AA29504 was found to be a more potent and effective agonist in δ-GABAARs than in γ2-GABAARs. In comparison, AA29504 positively modulated the activity of recombinant δ-GABAARs more effectively than γ2-GABAARs, with no significant differences in potency. The impact of AA29504's efficacy- and potency-associated GABAAR subtype selectivity on radioligand binding properties remain unexplored. Using [3H]4'-ethynyl-4-n-propylbicycloorthobenzoate ([3H]EBOB) binding assay, we found no difference in the modulatory potency of AA29504 on GABA- and THIP (4,5,6,7-tetrahydroisoxazolo[5,4-c]pyridin-3-ol)-induced responses between native forebrain GABAARs of wild type and δ knock-out mice. In recombinant receptors expressed in HEK293 cells, AA29504 showed higher efficacy on δ- than γ2-GABAARs in the GABA-independent displacement of [3H]EBOB binding. Interestingly, AA29504 showed a concentration-dependent stimulation of [3H]muscimol binding to γ2-GABAARs, which was absent in δ-GABAARs. This was explained by AA29504 shifting the low-affinity γ2-GABAAR towards a higher affinity desensitized state, thereby rising new sites capable of binding GABAAR agonists with low nanomolar affinity. Hence, the potential of AA29504 to act as a desensitization-modifying allosteric modulator of γ2-GABAARs deserves further investigation for its promising influence on shaping efficacy, duration and plasticity of GABAAR synaptic responses.
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- 2021
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9. UNISUS study design: a phase 3 superiority study comparing the efficacy, safety, and tolerability of macitentan 75 mg vs macitentan 10 mg in patients with pulmonary arterial hypertension (PAH)
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McLaughlin, V, primary, Hoeper, M, additional, Tamura, Y, additional, Backer, A, additional, Boyanova, N, additional, Kracker, H, additional, Larbalestier, A, additional, Lassen, C, additional, Sanna, L, additional, and Humbert, M, additional
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- 2022
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10. Comparing Treatment Outcomes in Children and Adolescents With ADHD to Other Disorders Within an Australian and Dutch Outpatient Cohort
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Leanne Payne, Sanna L. Roest, Zhen Qi Lu, Nardia Zendarski, Matthew Bisset, Emma Sciberras, Stephen Stathis, Bart M. Siebelink, Robert R. J. M. Vermeiren, Mark A. Bellgrove, David Coghill, and Christel M. Middeldorp
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Adolescent ,Autism Spectrum Disorder ,Australia ,treatment outcomes ,service evaluation ,community mental health service ,child and adolescent mental disorders ,Clinical Psychology ,Treatment Outcome ,Attention Deficit Disorder with Hyperactivity ,Outpatients ,emotional disorders ,Developmental and Educational Psychology ,ADHD ,Humans ,Child - Abstract
Objective: Previous studies at child and youth mental health services (CYMHS) suggest that children with ADHD have poorer outcomes compared to those with other diagnoses. This study investigates this in more detail. Methods: Children with ADHD were compared to those with ASD and those with emotional disorders, on routinely collected outcomes at CYMHS in Australia ( N = 2,513) and the Netherlands ( N = 844). Results: Where the emotional disorders group reached a similar level of emotional symptoms at the end-of-treatment as the ADHD and ASD groups, the latter two groups still had higher scores on ADHD and ASD symptoms (attention and peer problems). The poorer outcomes were mainly explained by higher severity at baseline. In Australia, an ADHD and/or ASD diagnosis also independently contributed to worse outcomes. Conclusion: Those with neurodevelopmental disorders within both countries had poorer outcomes than those with emotional disorders. Services should aim to optimize treatment to ensure best possible outcomes.
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- 2022
11. Alexithymia in eating disorders: therapeutic implications
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Pinna F, Sanna L, and Carpiniello B
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Psychology ,BF1-990 ,Industrial psychology ,HF5548.7-5548.85 - Abstract
Federica Pinna, Lucia Sanna, Bernardo Carpiniello Department of Public Health, Clinical and Molecular Medicine - Unit of Psychiatry, University of Cagliari, Cagliari, Italy Abstract: A high percentage of individuals affected by eating disorders (ED) achieve incomplete recovery following treatment. In an attempt to improve treatment outcome, it is crucial that predictors of outcome are identified, and personalized care approaches established in line with new treatment targets, thus facilitating patient access to evidence-based treatments. Among the psychological factors proposed as predictors of outcome in ED, alexithymia is of outstanding interest. The objective of this paper is to undertake a systematic review of the literature relating to alexithymia, specifically in terms of the implications for treatment of ED. In particular, issues concerning the role of alexithymia as a predictor of outcome and as a factor to be taken into account in the choice of treatment will be addressed. The effect of treatments on alexithymia will also be considered. A search of all relevant literature published in English using PubMed, PsycINFO, and Scopus databases was carried out on the basis of the following keywords: alexithymia, anorexia nervosa, bulimia nervosa, eating disorders, and treatment; no time limits were imposed. Despite the clinical relevance of alexithymia, the number of studies published on the above cited aspects is somewhat limited, and these studies are largely heterogeneous and feature significant methodological weaknesses. Overall, data currently available mostly correlate higher levels of alexithymia with a less favorable outcome in ED. Accordingly, alexithymia is seen as a relevant treatment target with the aim of achieving recovery of these patients. Treatments focusing on improving alexithymic traits, and specifically those targeting emotions, seem to show greater efficacy, although alexithymia levels often remain high even after specific treatment. Further investigations are needed to overcome the methodological limitations of previous studies, to understand the actual impact of alexithymia on ED outcome, and to allow more precise implications for treatment to be drawn. Additional research should also be undertaken to specify which of the alexithymic dimensions are specifically relevant to the course and outcome of ED, and to identify treatment protocols producing a significantly greater efficacy in ED patients with relevant alexithymic traits. Keywords: anorexia nervosa, bulimia nervosa, treatment
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- 2014
12. CARE PAH study design: an international, prospective real-world cohort of PAH patients
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Humbert, M, primary, Dreyer, N, additional, Mclaughlin, V, additional, Pulido, T, additional, Boyanova, N, additional, Frauchiger, B, additional, Kiefer, F, additional, Lassen, C, additional, Ong, R, additional, Sanna, L, additional, Sauter, A, additional, and Kiely, D, additional
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- 2022
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13. Comparing Treatment Outcomes in Children and Adolescents With ADHD to Other Disorders Within an Australian and Dutch Outpatient Cohort
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Payne, Leanne, primary, Roest, Sanna L., additional, Lu, Zhen Qi, additional, Zendarski, Nardia, additional, Bisset, Matthew, additional, Sciberras, Emma, additional, Stathis, Stephen, additional, Siebelink, Bart M., additional, Vermeiren, Robert R. J. M., additional, Bellgrove, Mark A., additional, Coghill, David, additional, and Middeldorp, Christel M., additional
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- 2022
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14. Fertility History and Cognition in Later Life
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Read, Sanna L and Grundy, Emily M D
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- 2017
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15. Target identification of a novel unsymmetrical 1,3,4‐oxadiazole derivative with antiproliferative properties
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Sanna L, Zeng Tiansheng, David J. Kelvin, Valentina Bordoni, Luigi Bagella, Lyu Weidong, Li Chengxun, Gérard Aimé Pinna, and Gabriele Murineddu
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0301 basic medicine ,Physiology ,Clinical Biochemistry ,Gene regulatory network ,RNA-Seq ,Computational biology ,03 medical and health sciences ,0302 clinical medicine ,Humans ,Gene Regulatory Networks ,Protein Interaction Maps ,KEGG ,Cell Proliferation ,Oxadiazoles ,Binding Sites ,biology ,Chemistry ,Gene Expression Profiling ,Cell Cycle ,Reproducibility of Results ,Cell Biology ,Cell cycle ,Small molecule ,Molecular Docking Simulation ,Gene Ontology ,030104 developmental biology ,Tubulin ,Gene Expression Regulation ,030220 oncology & carcinogenesis ,biology.protein ,Signal transduction ,Function (biology) ,HeLa Cells - Abstract
1,3,4-Oxadiazole derivatives are widely used in research on antineoplastic drugs. Recently, we discovered a novel unsymmetrical 1,3,4-oxadiazole compound with antiproliferative properties called 2j. To further investigate its possible targets and molecular mechanisms, RNA-seq was performed and the differentially expressed genes (DEGs) were obtained after treatment. Data were analyzed using functional (Gene Ontology term) and pathway (Kyoto Encyclopedia of Genes and Genomes) enrichment of the DEGs. The hub genes were determined by the analysis of protein-protein interaction networks. The connectivity map (CMap) information provided insight into the model action of antitumor small molecule drugs. Hub genes have been identified through function gene networks using STRING analysis. The small molecular targets obtained by CMap comparison showed that 2j is a tubulin inhibitor and it acts mainly affecting tumor cells through the cell cycle, FoxO signaling pathway, apoptotic, and p53 signaling pathways. The possible targets of 2j could be TUBA1A and TUBA4A. Molecular docking results indicated that 2j interacts at the colchicine-binding site on tubulin.
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- 2020
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16. sj-docx-2-jad-10.1177_10870547221112941 – Supplemental material for Comparing Treatment Outcomes in Children and Adolescents With ADHD to Other Disorders Within an Australian and Dutch Outpatient Cohort
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Payne, Leanne, Roest, Sanna L., Lu, Zhen Qi, Zendarski, Nardia, Bisset, Matthew, Sciberras, Emma, Stathis, Stephen, Siebelink, Bart M., Vermeiren, Robert R. J. M., Bellgrove, Mark A., Coghill, David, and Middeldorp, Christel M.
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FOS: Psychology ,170199 Psychology not elsewhere classified ,Education - Abstract
Supplemental material, sj-docx-2-jad-10.1177_10870547221112941 for Comparing Treatment Outcomes in Children and Adolescents With ADHD to Other Disorders Within an Australian and Dutch Outpatient Cohort by Leanne Payne, Sanna L. Roest, Zhen Qi Lu, Nardia Zendarski, Matthew Bisset, Emma Sciberras, Stephen Stathis, Bart M. Siebelink, Robert R. J. M. Vermeiren, Mark A. Bellgrove, David Coghill and Christel M. Middeldorp in Journal of Attention Disorders
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- 2022
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17. sj-docx-1-jad-10.1177_10870547221112941 – Supplemental material for Comparing Treatment Outcomes in Children and Adolescents With ADHD to Other Disorders Within an Australian and Dutch Outpatient Cohort
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Payne, Leanne, Roest, Sanna L., Lu, Zhen Qi, Zendarski, Nardia, Bisset, Matthew, Sciberras, Emma, Stathis, Stephen, Siebelink, Bart M., Vermeiren, Robert R. J. M., Bellgrove, Mark A., Coghill, David, and Middeldorp, Christel M.
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FOS: Psychology ,170199 Psychology not elsewhere classified ,Education - Abstract
Supplemental material, sj-docx-1-jad-10.1177_10870547221112941 for Comparing Treatment Outcomes in Children and Adolescents With ADHD to Other Disorders Within an Australian and Dutch Outpatient Cohort by Leanne Payne, Sanna L. Roest, Zhen Qi Lu, Nardia Zendarski, Matthew Bisset, Emma Sciberras, Stephen Stathis, Bart M. Siebelink, Robert R. J. M. Vermeiren, Mark A. Bellgrove, David Coghill and Christel M. Middeldorp in Journal of Attention Disorders
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- 2022
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18. Tomentosin a Sesquiterpene Lactone Induces Antiproliferative and Proapoptotic Effects in Human Burkitt Lymphoma by Deregulation of Anti- and Pro-Apoptotic Genes
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Francesco Fiorentino, Luigi Bagella, Maria Rosaria Muroni, Claudio Fozza, Maria Rosaria De Miglio, Valentina Bordoni, Patrizia Virdis, Sanna L, Rossana Migheli, Luigi Podda, Giorgio Antonio Mario Pintore, Grazia Galleri, and Irene Marchesi
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chemistry.chemical_classification ,Cell cycle checkpoint ,Science ,Paleontology ,Burkitt lymphoma ,BCL2A1 ,Biology ,Sesquiterpene lactone ,General Biochemistry, Genetics and Molecular Biology ,Article ,CDKN1A ,chemistry ,Downregulation and upregulation ,Space and Planetary Science ,Apoptosis ,Cell culture ,Cancer research ,PMAIP1 ,Viability assay ,tomentosin ,Protein kinase B ,Ecology, Evolution, Behavior and Systematics ,PI3K/AKT/mTOR pathway - Abstract
(1) Tomentosin is the most representative sesquiterpene lactone extracted by I. viscosa. Recently, it has gained particular attention in therapeutic oncologic fields due to its anti-tumor properties. (2) In this study, the potential anticancer features of tomentosin were evaluated on human Burkitt’s lymphoma (BL) cell line, treated with increasing tomentosin concentration for cytotoxicity screening. (3) Our data showed that both cell cycle arrest and cell apoptosis induction are responsible of the antiproliferative effects of tomentosin and may end in the inhibition of BL cell viability. Moreover, a microarray gene expression profile was performed to assess differentially expressed genes contributing to tomentosin activity. Seventy-five genes deregulated by tomentosin have been identified. Downregulated genes are enriched in immune-system pathways, and PI3K/AKT and JAK/STAT pathways which favor proliferation and growth processes. Importantly, different deregulated genes identified in tomentosin-treated BL cells are prevalent in molecular pathways known to lead to cellular death, specifically by apoptosis. Tomentosin-treatment in BL cells induces the downregulation of antiapoptotic genes such as BCL2A1 and CDKN1A and upregulation of the proapoptotic PMAIP1 gene. (4) Overall, our results suggest that tomentosin could be taken into consideration as a potential natural product with limited toxicity and relevant anti-tumoral activity in the therapeutic options available to BL patients.
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- 2021
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19. Clarifying the molecular mechanism of tomentosin-induced antiproliferative and proapoptotic effects in human multiple myeloma via gene expression profile and genetic interaction network analysis
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Maria Rosaria De Miglio, Claudio Fozza, Maria Rosaria Muroni, Giorgio Antonio Mario Pintore, Rossana Migheli, Francesco Fiorentino, Patrizia Virdis, Grazia Galleri, Valentina Bordoni, Sanna L, Irene Marchesi, Luigi Bagella, and Luigi Podda
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Cell ,Biology ,cyclic AMP-dependent transcription factor ATF-4 ,Lactones ,Downregulation and upregulation ,Protein-Protein Interaction network ,Cell Line, Tumor ,Gene expression ,Genetics ,medicine ,Humans ,Protein Interaction Maps ,tomentosin ,Transcription factor ,DNA damage-inducible transcript 3 protein ,Gene Expression Profiling ,Cell Cycle ,apoptosis ,General Medicine ,Articles ,Cell cycle ,Antineoplastic Agents, Phytogenic ,Cell biology ,Gene expression profiling ,multiple myeloma ,Gene Expression Regulation, Neoplastic ,medicine.anatomical_structure ,Unfolded protein response ,cytotoxicity ,Signal transduction ,Drug Screening Assays, Antitumor ,Sesquiterpenes - Abstract
Multiple myeloma (MM) is an aggressive B cell malignancy. Substantial progress has been made in the therapeutic context for patients with MM, however it still represents an incurable disease due to drug resistance and recurrence. Development of more effective or synergistic therapeutic approaches undoubtedly represents an unmet clinical need. Tomentosin is a bioactive natural sesquiterpene lactone extracted by various plants with therapeutic properties, including anti‑neoplastic effects. In the present study, the potential antitumor activity of tomentosin was evaluated on the human RPMI‑8226 cell line, treated with increasing tomentosin concentration for cytotoxicity screening. The data suggested that both cell cycle arrest and cell apoptosis could explain the antiproliferative effects of tomentosin and may result in the inhibition of RPMI‑8226 cell viability. To assess differentially expressed genes contributing to tomentosin activity and identify its mechanism of action, a microarray gene expression profile was performed, identifying 126 genes deregulated by tomentosin. To address the systems biology and identify how tomentosin deregulates gene expression in MM from a systems perspective, all deregulated genes were submitted to enrichment and molecular network analysis. The Protein‑Protein Interaction (PPI) network analysis showed that tomentosin in human MM induced the downregulation of genes involved in several pathways known to lead immune‑system processes, such as cytokine‑cytokine receptor interaction, chemokine or NF‑κB signaling pathway, as well as genes involved in pathways playing a central role in cellular neoplastic processes, such as growth, proliferation, migration, invasion and apoptosis. Tomentosin also induced endoplasmic reticulum stress via upregulation of cyclic AMP‑dependent transcription factor ATF‑4 and DNA damage‑inducible transcript 3 protein genes, suggesting that in the presence of tomentosin the protective unfolded protein response signaling may induce cell apoptosis. The functional connections analysis executed using the Connectivity Map tool, suggested that the effects of tomentosin on RPMI‑8226 cells might be similar to those exerted by heat shock proteins inhibitors. Taken together, these data suggested that tomentosin may be a potential drug candidate for the treatment of MM.
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- 2021
20. Silver Nanoparticles Derived by Artemisia arborescens Reveal Anticancer and Apoptosis-Inducing Effects
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Stefano Zoroddu, Sanna L, Valentina Bordoni, Weidong Lyu, Serenella Medici, Elisabetta Avitabile, David J. Kelvin, and Luigi Bagella
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silver nanoparticles ,Silver ,Artemisia arborescens ,Cell Survival ,QH301-705.5 ,Metal Nanoparticles ,Context (language use) ,Antineoplastic Agents ,Apoptosis ,Catalysis ,Silver nanoparticle ,Article ,Inorganic Chemistry ,HeLa ,chemistry.chemical_compound ,medicine ,Humans ,Physical and Theoretical Chemistry ,Biology (General) ,Clonogenic assay ,Molecular Biology ,QD1-999 ,Spectroscopy ,biology ,nanotechnology ,Plant Extracts ,Organic Chemistry ,Cancer ,food and beverages ,Green Chemistry Technology ,General Medicine ,Cell cycle ,biology.organism_classification ,medicine.disease ,Computer Science Applications ,Gene Expression Regulation, Neoplastic ,Chemistry ,chemistry ,Artemisia ,Cancer cell ,PC-3 Cells ,Cancer research ,MCF-7 Cells ,cancer research ,Growth inhibition ,Drug Screening Assays, Antitumor ,RNA-seq ,HeLa Cells - Abstract
The fight against cancer is one of the main challenges for medical research. Recently, nanotechnology has made significant progress, providing possibilities for developing innovative nanomaterials to overcome the common limitations of current therapies. In this context, silver nanoparticles (AgNPs) represent a promising nano-tool able to offer interesting applications for cancer research. Following this path, we combined the silver proprieties with Artemisia , arborescens characteristics, producing novel nanoparticles called Artemisia–AgNPs. A “green” synthesis method was performed to produce Artemisia–AgNPs, using Artemisia , arborescens extracts. This kind of photosynthesis is an eco-friendly, inexpensive, and fast approach. Moreover, the bioorganic molecules of plant extracts improved the biocompatibility and efficacy of Artemisia–AgNPs. The Artemisia–AgNPs were fully characterized and tested to compare their effects on various cancer cell lines, in particular HeLa and MCF-7. Artemisia–AgNPs treatment showed dose-dependent growth inhibition of cancer cells. Moreover, we evaluated their impact on the cell cycle, observing a G1 arrest mediated by Artemisia–AgNPs treatment. Using a clonogenic assay after treatment, we observed a complete lack of cell colonies, which demonstrated cell reproducibility death. To have a broader overview on gene expression impact, we performed RNA-sequencing, which demonstrated the potential of Artemisia–AgNPs as a suitable candidate tool in cancer research.
- Published
- 2021
21. The Influence of AA29504 on GABAA Receptor Ligand Binding Properties and Its Implications on Subtype Selectivity
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Sikstus, Sylvia, primary, Benkherouf, Ali Y., additional, Soini, Sanna L., additional, and Uusi-Oukari, Mikko, additional
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- 2021
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22. What Flavor Is Your Soda?
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Garcia, Sanna L., Hake, John M., Heaton, Michael I., Harris, Richard W., and Gabb, Donald M.
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- 2000
23. Positive allosteric modulation of native and recombinant GABAA receptors by hops prenylflavonoids
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Monika Stompor, Sanna L. Soini, Mikko Uusi-Oukari, and Ali Y. Benkherouf
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0301 basic medicine ,Pharmacology ,Isoxanthohumol ,Chemistry ,GABAA receptor ,Ligand binding assay ,Allosteric regulation ,ta1182 ,ta3111 ,ta3112 ,Prenylflavonoid ,03 medical and health sciences ,chemistry.chemical_compound ,030104 developmental biology ,0302 clinical medicine ,Flumazenil ,Xanthohumol ,medicine ,Receptor ,030217 neurology & neurosurgery ,medicine.drug - Abstract
Hops are a major component of beer that is added during brewing. In addition to its wide range of bioactivity, it exhibits neuroactive properties as a sedative and sleeping aid. The compounds responsible for this activity are yet to be revealed and understood in terms of their pharmacological properties. Here we evaluated the potential of several hops flavonoids in modulating the GABAergic activity and assessed their selectivity to GABAA receptors subtypes. GABA-potentiating effects were measured using [3H]ethynylbicycloorthobenzoate (EBOB) radioligand binding assay in native and recombinant α1β3γ2, α2β3γ2 and α6β3δ receptors expressed in HEK293 cells. Flumazenil sensitivity of GABA-potentiating effects and [3H]Ro 15-4513 binding assay were used to examine the flavonoids binding to benzodiazepine site. The prenylflavonoids xanthohumol (XN), isoxanthohumol (IXN) and 8-prenylnaringenin (8PN) potentiated GABA-induced displacement of [3H]EBOB binding in a concentration-dependent manner. The IC50 for this potentiation in native GABAA receptors were 29.7 µM, 11.6 µM, 7.3 µM, respectively. In recombinant receptors, the sensitivity to prenylflavonoid potentiation of GABA-induced displacement of [3H]EBOB binding followed the order α6β3δ > α2β3γ2 > α1β3γ2 with the strongest inhibition observed by 8PN in α6β3δ (IC50 = 3.6 μM). Flumazenil had no significant effect on the prenylflavonoid-induced displacement of [3H]EBOB binding and [3H]Ro 15-4513 displacement from native GABAA receptors was only detected at high micromolar concentrations (100 µM). We identified potent prenylflavonoids in hops that positively modulate GABA-induced responses in native and αβγ/δ recombinant GABAA receptors at low micromolar concentrations. These GABAergic modulatory effects were not mediated via the high-affinity benzodiazepine binding site.
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- 2019
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24. Extrasynaptic δ‐GABAA receptors are high affinity muscimol receptors
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Ali Y. Benkherouf, Pratap Meera, Sanna L. Soini, Mikko Uusi-Oukari, Kaisa‐Riitta Taina, Xiang-Guo Li, Martin Wallner, and Asko J. Aalto
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0301 basic medicine ,Agonist ,biology ,GABAA receptor ,medicine.drug_class ,Protein subunit ,Wild type ,biology.organism_classification ,ta3111 ,Biochemistry ,ta3112 ,03 medical and health sciences ,Cellular and Molecular Neuroscience ,chemistry.chemical_compound ,030104 developmental biology ,0302 clinical medicine ,nervous system ,Muscimol ,chemistry ,Forebrain ,medicine ,Biophysics ,Receptor ,030217 neurology & neurosurgery ,Amanita muscaria - Abstract
Muscimol, the major psychoactive ingredient in the mushroom Amanita muscaria, has been regarded as a universal non-selective GABA-site agonist. Deletion of the GABAA receptor (GABAA R) δ subunit in mice (δKO) leads to a drastic reduction in high-affinity muscimol binding in brain sections and to a lower behavioral sensitivity to muscimol than their wild type counterparts. Here, we use forebrain and cerebellar brain homogenates from WT and δKO mice to show that deletion of the δ subunit leads to a > 50% loss of high-affinity 5 nM [3 H]muscimol-binding sites despite the relatively low abundance of δ-containing GABAA Rs (δ-GABAA R) in the brain. By subtracting residual high-affinity binding in δKO mice and measuring the slow association and dissociation rates we show that native δ-GABAA Rs in WT mice exhibit high-affinity [3 H]muscimol-binding sites (KD ~1.6 nM on α4βδ receptors in the forebrain and ~1 nM on α6βδ receptors in the cerebellum at 22°C). Co-expression of the δ subunit with α6 and β2 or β3 in recombinant (HEK 293) expression leads to the appearance of a slowly dissociating [3 H]muscimol component. In addition, we compared muscimol currents in recombinant α4β3δ and α4β3 receptors and show that δ subunit co-expression leads to highly muscimol-sensitive currents with an estimated EC50 of around 1-2 nM and slow deactivation kinetics. These data indicate that δ subunit incorporation leads to a dramatic increase in GABAA R muscimol sensitivity. We conclude that biochemical and behavioral low-dose muscimol selectivity for δ-subunit-containing receptors is a result of low nanomolar-binding affinity on δ-GABAA Rs.
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- 2019
25. The Influence of AA29504 on GABA
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Sylvia, Sikstus, Ali Y, Benkherouf, Sanna L, Soini, and Mikko, Uusi-Oukari
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Mice ,HEK293 Cells ,Muscimol ,Animals ,Humans ,GABA-A Receptor Agonists ,Ligands ,Receptors, GABA-A - Abstract
The unique pharmacological properties of δ-containing γ-aminobutyric acid type A receptors (δ-GABA
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- 2021
26. 322 Adipokines in psoriasis and obesity: emerging role of visfatin, leptin and adiponectin
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Mercurio, L., Belli, R., Mubarak, M., Eyerich, S., Lolli, M., Sanna, L., Scarponi, C., Scala, E., Albanesi, C., and Madonna, S.
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- 2024
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27. Zoledronic acid efficacy and safety over five years in postmenopausal osteoporosis
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Devogelaer, J. P., Brown, J. P., Burckhardt, P., Meunier, P. J., Goemaere, S., Lippuner, K., Body, J. J., Samsioe, G., Felsenberg, D., Fashola, T., Sanna, L., Ortmann, C. E., Trechsel, U., Krasnow, J., Eriksen, E. F., and Garnero, P.
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- 2007
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28. A comprehensive assessment of a new series of 5',6'-difluorobenzotriazole-acrylonitrile derivatives as microtubule targeting agents (MTAs)
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Roberta Ibba, Valentina Bordoni, Luigi Bagella, Simona Sestito, Michele Lai, Sanna L, M. Andrea Scorciapino, Federico Riu, Antonio Carta, and Sandra Piras
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Cell growth inhibition ,Benzotriazoles ,Extrusion pump inhibition ,Microtubule targeting agents ,Molecular docking ,Tubulin ,Acrylonitrile ,Antineoplastic Agents ,Cell Proliferation ,Dose-Response Relationship, Drug ,Drug Screening Assays, Antitumor ,HeLa Cells ,Humans ,Microtubules ,Mitosis ,Molecular Docking Simulation ,Molecular Structure ,Structure-Activity Relationship ,Triazoles ,Drug Screening Assays ,01 natural sciences ,Dose-Response Relationship ,HeLa ,03 medical and health sciences ,chemistry.chemical_compound ,Microtubule ,Drug Discovery ,Binding site ,030304 developmental biology ,Pharmacology ,0303 health sciences ,biology ,010405 organic chemistry ,Chemistry ,Organic Chemistry ,Antitumor ,General Medicine ,biology.organism_classification ,0104 chemical sciences ,Biochemistry ,Docking (molecular) ,Cancer cell ,biology.protein ,Drug ,Lead compound - Abstract
Microtubules (MTs) are the principal target for drugs acting against mitosis. These compounds, called microtubule targeting agents (MTAs), cause a mitotic arrest during G2/M phase, subsequently inducing cell apoptosis. MTAs could be classified in two groups: microtubule stabilising agents (MSAs) and microtubule destabilising agents (MDAs). In this paper we present a new series of (E) (Z)-2-(5,6-difluoro-(1H)2H-benzo[d] [1,2,3]triazol-1(2)-yl)-3-(R)acrylonitrile (9a-j, 10e, 11a,b) and (E)-2-(1H-benzo[d] [1,2,3]triazol-1-yl)-3-(R)acrylonitrile derivatives (13d,j), which were recognised to act as MTAs agents. They were rationally designed, synthesised, characterised and subjected to different biological assessments. Computational docking was carried out in order to investigate the potential binding to the colchicine-binding site on tubulin. From this first prediction, the di-fluoro substitution seemed to be beneficial for the binding affinity with tubulin. The new fluorine derivatives, here presented, showed an improved antiproliferative activity when compared to the previously reported compounds. The biological evaluation included a preliminary antiproliferative screening on NCI60 cancer cells panel (1–10 μM). Compound 9a was selected as lead compound of the new series of derivatives. The in vitro XTT assay, flow cytometry analysis and immunostaining performed on HeLa cells treated with 9a showed a considerable antiproliferative effect, (IC50 = 3.2 μM), an increased number of cells in G2/M-phase, followed by an enhancement in cell division defects. Moreover, β-tubulin staining confirmed 9a as a MDA triggering tubulin disassembly, whereas colchicine-9a competition assay suggested that compound 9a compete with colchicine for the binding site on tubulin. Then, the co-administration of compound 9a and an extrusion pump inhibitor (EPI) was investigated: the association resulted beneficial for the antiproliferative activity and compound 9a showed to be client of extrusion pumps. Finally, structural superimposition of different colchicine binding site inhibitors (CBIs) in clinical trial and our MDA, provided an additional confirmation of the targeting to the predicted binding site. Physicochemical, pharmacokinetic and druglikeness predictions were also conducted and all the newly synthesised derivatives showed to be drug-like molecules.
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- 2020
29. The immunological architecture of granulomatous inflammation in central nervous system tuberculosis
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A. Marceline van Furth, Mariana Kruger, Sabine L van Elsland, Ronald van Toorn, Carmen S. van Dam, Sanna L. Roest, Jaco Hagoort, Daniel J. Franken, Regan Solomons, Bernadette S. de Bakker, Carlie Timmers, Martijn van der Kuip, Stefan-Dan Zaharie, Pediatric surgery, AII - Infectious diseases, Internal medicine, Amsterdam Reproduction & Development (AR&D), Medical Biology, Amsterdam Cardiovascular Sciences, and ACS - Heart failure & arrhythmias
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0301 basic medicine ,Microbiology (medical) ,Adult ,Male ,Pathology ,medicine.medical_specialty ,Tuberculosis ,Adolescent ,030106 microbiology ,Immunology ,Central nervous system ,Microbiology ,Tuberculous meningitis ,03 medical and health sciences ,Young Adult ,Cerebrospinal fluid ,medicine ,Humans ,Child ,Neuroinflammation ,Central nervous system tuberculosis ,Aged ,Retrospective Studies ,Inflammation ,Immunity, Cellular ,Rich focus ,Granuloma ,3D-reconstruction ,business.industry ,Leptomeninges ,Infant ,Mycobacterium tuberculosis ,Middle Aged ,Tuberculosis, Central Nervous System ,medicine.disease ,Immunohistochemistry ,030104 developmental biology ,Infectious Diseases ,medicine.anatomical_structure ,Child, Preschool ,Female ,business - Abstract
Of all tuberculosis (TB) cases, 1% affects the central nervous system (CNS), with a mortality rate of up to 60%. Our aim is to fill the 'key gap' in TBM research by analyzing brain specimens in a unique historical cohort of 84 patients, focusing on granuloma formation. We describe three different types: non-necrotizing, necrotizing gummatous, and necrotizing abscess type granuloma. Our hypothesis is that these different types of granuloma are developmental stages of the same pathological process. All types were present in each patient and were mainly localized in the leptomeninges. Intra-parenchymal granulomas were less abundant than the leptomeningeal ones and mainly located close to the cerebrospinal fluid (subpial and subependymal). We found that most of the intraparenchymal granulomas are an extension of leptomeningeal lesions which is the opposite of the classical Rich focus theory. We present a 3D-model to facilitate further understanding of the topographic relation of granulomas with leptomeninges, brain parenchyma and blood vessels. We describe innate and adaptive immune responses during granuloma formation including the cytokine profiles. We emphasize the presence of leptomeningeal B-cell aggregates as tertiary lymphoid structures. Our study forms a basis for further research in neuroinflammation and infectious diseases of the CNS, especially TB.
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- 2020
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30. Three-dimensional visualizations from a dataset of immunohistochemical stained serial sections of human brain tissue containing tuberculosis related granulomas
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Jaco Hagoort, Carlie Timmers, Regan Solomons, Ronald van Toorn, Mariana Kruger, A. Marceline van Furth, Carmen S. van Dam, Stefan Dan Zaharie, Daniel J. Franken, Sanna L. Roest, Martijn van der Kuip, Bernadette S. de Bakker, Sabine L van Elsland, Graduate School, Amsterdam Reproduction & Development (AR&D), Amsterdam Cardiovascular Sciences, Medical Biology, ACS - Heart failure & arrhythmias, Pediatric surgery, and AII - Infectious diseases
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Pathology ,medicine.medical_specialty ,Tuberculosis ,Biology ,lcsh:Computer applications to medicine. Medical informatics ,Tuberculous meningitis ,03 medical and health sciences ,0302 clinical medicine ,medicine ,Research article ,Rich-focus ,lcsh:Science (General) ,Central nervous system tuberculosis ,Data Article ,030304 developmental biology ,0303 health sciences ,Multidisciplinary ,Granuloma ,3D-reconstruction ,Formalin fixed ,Human brain ,medicine.disease ,medicine.anatomical_structure ,Immunohistochemistry ,lcsh:R858-859.7 ,Human research ,030217 neurology & neurosurgery ,lcsh:Q1-390 - Abstract
This data article presents datasets associated with the research article entitled “The immunological architecture of granulomatous inflammation in central nervous system tuberculosis’’ (Zaharie et al., 2020). The morphology of tuberculosis related granulomas within the central nervous system of human patients was visualized in six different three-dimensional (3D) models. Post-mortem, formalin fixed and paraffin embedded specimens from deceased tuberculous meningitis patients were immunohistochemically stained and 800 serial histologically stained sections were acquired. Images from all sections were obtained with an Olympus BX43 light microscope and structures were identified, labeled and made three-dimensional. The interactive 3D-models allows the user to directly visualize the morphology of the granulomas and to understand the localization of the granulomas. The 3D-models can be used for multiple purposes and provide both an educational source as a gold standard for further animal studies, human research and the development of in silico models on the topic of central nervous system tuberculosis.
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- 2020
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31. Increased ROS generation and p53 activation in α-lipoic acid-induced apoptosis of hepatoma cells
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Simbula, G., Columbano, A., Ledda-Columbano, G. M., Sanna, L., Deidda, M., Diana, A., and Pibiri, M.
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- 2007
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32. Non-specific binding of [18F]FDG to calcifications in atherosclerotic plaques: experimental study of mouse and human arteries
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Laitinen, Iina, Marjamäki, Päivi, Haaparanta, Merja, Savisto, Nina, Laine, V. Jukka O., Soini, Sanna L., Wilson, Ian, Leppänen, Pia, Ylä-Herttuala, Seppo, Roivainen, Anne, and Knuuti, Juhani
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- 2006
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33. MDR1, cholesterol esterification and cell growth: a comparative study in normal and multidrug-resistant KB cell lines
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Pani*, A., Batetta, B., Putzolu, M., Sanna, F., Spano, O., Piras, S., Mulas, M. F., Bonatesta, R. R., Amat di S. Filippo, C., Vargiu, L., Marceddu, T., Sanna, L., La Colla, P., and Dessi, S.
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- 2000
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34. Experience Informs: Spanning Three Decades with the Neuman Systems Model
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Beckman, Sarah J., Boxley-Harges, Sanna L., and Kaskel, Beth L.
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- 2012
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35. Three-dimensional visualizations from a dataset of immunohistochemical stained serial sections of human brain tissue containing tuberculosis related granulomas
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Zaharie, Stefan-Dan, primary, Franken, Daniel J., additional, van der Kuip, Martijn, additional, van Elsland, Sabine, additional, de Bakker, Bernadette S., additional, Hagoort, Jaco, additional, Roest, Sanna L., additional, van Dam, Carmen S., additional, Timmers, Carlie, additional, Solomons, Regan, additional, van Toorn, Ronald, additional, Kruger, Mariana, additional, and van Furth, A. Marceline, additional
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- 2020
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36. Humulone Modulation of GABAA Receptors and Its Role in Hops Sleep-Promoting Activity
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Benkherouf, Ali Y., primary, Eerola, Kim, additional, Soini, Sanna L., additional, and Uusi-Oukari, Mikko, additional
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- 2020
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37. Hops compounds modulatory effects and 6-prenylnaringenin dual mode of action on GABAA receptors
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Benkherouf, Ali Y., primary, Logrén, Nora, additional, Somborac, Tamara, additional, Kortesniemi, Maaria, additional, Soini, Sanna L., additional, Yang, Baoru, additional, Salo-Ahen, Outi M.H., additional, Laaksonen, Oskar, additional, and Uusi-Oukari, Mikko, additional
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- 2020
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38. Familial aggregation of MATRICS Consensus Cognitive Battery scores in a large sample o outpatients with schizophrenia and their unaffected relatives
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Mucci A., Galderisi S., Green M. F., Nuechterlein K., Rucci P., Gibertoni D., Rossi A., Rocca P., Bertolino A., Bucci P., Hellemann G., Spisto M., Palumbo D., Aguglia E., Amodeo G., Amore M., Bellomo A., Brugnoli R., Carpiniello B., Dell'osso L., Di Fabio F., Di Giannantonio M., Di Lorenzo G., Marchesi C., Monteleone P., Montemagni C., Oldani L., Romano R., Roncone R., Stratta P., Tenconi E., Vita A., Zeppegno P., Maj M., Piegari G., Vignapiano A., Caputo F., Plescia G., Montefusco V., Mancini M., Attrotto M. T., Paladini V., Atti A. R., Barlati S., Galluzzo A., Mussoni C., Pinna F., Sanna L., Primavera D., Signorelli M. S., Minutolo G., Cannavo D., Acciavatti T., Santacroce R., Corbo M., Altamura M., La Montagna M., Carnevale R., Pizziconi G., Rossi R., Santarelli V., Giusti L., Malavolta M., Salza A., Murri M. B., Calcagno P., Bugliani M., Serati M., Orsenigo G., Gramaglia C., Gattoni E., Cattaneo C., Campagnola N., Ferronato L., Piovan C., Tonna M., Bettini E., Ossola P., Gesi C., Landi P., Rutigliano G., Biondi M., Girardi P., Buzzanca A., Zocconali M., Comparelli A., Mancinelli I., Niolu C., Ribolsi M., Siracusano A., Corrivetti G., Bartoli L., Diasco F., Bolognesi S., Goracci A., Fagiolini A., Bellino S., Cardillo S., Bracale N., Mucci, A., Galderisi, S., Green, M. F., Nuechterlein, K., Rucci, P., Gibertoni, D., Rossi, A., Rocca, P., Bertolino, A., Bucci, P., Hellemann, G., Spisto, M., Palumbo, D., Aguglia, E., Amodeo, G., Amore, M., Bellomo, A., Brugnoli, R., Carpiniello, B., Dell'Osso, L., Di Fabio, F., Di Giannantonio, M., Di Lorenzo, G., Marchesi, C., Monteleone, P., Montemagni, C., Oldani, L., Romano, R., Roncone, R., Stratta, P., Tenconi, E., Vita, A., Zeppegno, P., Maj, M., Piegari, G., Vignapiano, A., Caputo, F., Plescia, G., Montefusco, V., Mancini, M., Attrotto, M. T., Paladini, V., Atti, A. R., Barlati, S., Galluzzo, A., Mussoni, C., Pinna, F., Sanna, L., Primavera, D., Signorelli, M. S., Minutolo, G., Cannavo, D., Acciavatti, T., Santacroce, R., Corbo, M., Altamura, M., La Montagna, M., Carnevale, R., Pizziconi, G., Rossi, R., Santarelli, V., Giusti, L., Malavolta, M., Salza, A., Murri, M. B., Calcagno, P., Bugliani, M., Serati, M., Orsenigo, G., Gramaglia, C., Gattoni, E., Cattaneo, C., Campagnola, N., Ferronato, L., Piovan, C., Tonna, M., Bettini, E., Ossola, P., Gesi, C., Landi, P., Rutigliano, G., Biondi, M., Girardi, P., Buzzanca, A., Zocconali, M., Comparelli, A., Mancinelli, I., Niolu, C., Ribolsi, M., Siracusano, A., Corrivetti, G., Bartoli, L., Diasco, F., Bolognesi, S., Goracci, A., Fagiolini, A., Bellino, S., Cardillo, S., Bracale, N., and di Giannantonio, M.
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Attention, MCCB Italian standardization, reasoning and problem solving, social cognition, verbal learning, working memory ,Proband ,Adult ,Male ,Consensus ,Psychometrics ,Context (language use) ,social cognition ,Verbal learning ,working memory ,03 medical and health sciences ,Attention ,MCCB Italian standardization ,reasoning and problem solving ,verbal learning ,Aged ,Cognition ,Cognitive Dysfunction ,Family ,Female ,Humans ,Middle Aged ,Outpatients ,Psychiatric Status Rating Scales ,Schizophrenia ,Schizophrenic Psychology ,0302 clinical medicine ,Social cognition ,medicine ,Applied Psychology ,Psychiatry and Mental Health ,Family aggregation ,medicine.disease ,030227 psychiatry ,Settore MED/25 ,Psychology ,MATRICS ,Neurocognitive ,030217 neurology & neurosurgery ,Clinical psychology - Abstract
BackgroundThe increased use of the MATRICS Consensus Cognitive Battery (MCCB) to investigate cognitive dysfunctions in schizophrenia fostered interest in its sensitivity in the context of family studies. As various measures of the same cognitive domains may have different power to distinguish between unaffected relatives of patients and controls, the relative sensitivity of MCCB tests for relative–control differences has to be established. We compared MCCB scores of 852 outpatients with schizophrenia (SCZ) with those of 342 unaffected relatives (REL) and a normative Italian sample of 774 healthy subjects (HCS). We examined familial aggregation of cognitive impairment by investigating within-family prediction of MCCB scores based on probands’ scores.MethodsMultivariate analysis of variance was used to analyze group differences in adjusted MCCB scores. Weighted least-squares analysis was used to investigate whether probands’ MCCB scores predicted REL neurocognitive performance.ResultsSCZ were significantly impaired on all MCCB domains. REL had intermediate scores between SCZ and HCS, showing a similar pattern of impairment, except for social cognition. Proband's scores significantly predicted REL MCCB scores on all domains except for visual learning.ConclusionsIn a large sample of stable patients with schizophrenia, living in the community, and in their unaffected relatives, MCCB demonstrated sensitivity to cognitive deficits in both groups. Our findings of significant within-family prediction of MCCB scores might reflect disease-related genetic or environmental factors.
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- 2018
39. The complex relationship between self-reported 'personal recovery' and clinical recovery in schizophrenia
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Rossi, A, Amore, M, Galderisi, S, Rocca, P, Bertolino, A, Aguglia, E, Amodeo, G, Bellomo, A, Bucci, P, Buzzanca, A, Carpiniello, B, Comparelli, A, Dell'Osso, L, Giannantonio, M, Mancini, M, Marchesi, C, Monteleone, P, Montemagni, C, Oldani, L, Roncone, R, Siracusano, A, Stratta, P, Tenconi, E, Vignapiano, A, Vita, A, Zeppegno, P, Maj, M, Rossetti, M, Rossi, R, Santarelli, V, Giusti, L, Malavolta, M, Salza, A, Palumbo, D, Patriarca, S, Chieffi, M, Attrotto, M, Colagiorgio, L, Andriola, I, Atti, A, Barlati, S, Deste, G, Galluzzo, A, Pinna, F, Deriu, L., Sanna, L, Signorelli, M., Minutolo, G, Cannavò, D, Martinotti, G, Acciavatti, T, Corbo, M, Altamura, M, Carnevale, R, Malerba, S, Murri, M, Calcagno, P, Bugliani, M, Serati, M, Bartolomeis, A, Gramaglia, C, Gattoni, E, Gambaro, E, Collantoni, E, Cremonese, C, Rossi, E, Ossola, P, Tonna, M, Panfilis, C, Rutigliano, G, Gesi, C, Carmassi, C, Biondi, M, Girardi, P, Brugnoli, R, Fabio, F, Pietro, S, Girardi, N, Niolu, C, Lorenzo, G, Ribolsi, M, Corrivetti, G, Pinto, G, Longobardi, N, Fagiolini, A, Goracci, A, Bolognesi, S, Bellino, S, Villari, V, Bracale, N, Rossi, A., Amore, M., Galderisi, S., Rocca, P., Bertolino, A., Aguglia, E., Amodeo, G., Bellomo, A., Bucci, P., Buzzanca, A., Carpiniello, B., Comparelli, A., Dell'Osso, L., Giannantonio, M. D., Mancini, M., Marchesi, C., Monteleone, P., Montemagni, C., Oldani, L., Roncone, R., Siracusano, A., Stratta, P., Tenconi, E., Vignapiano, A., Vita, A., Zeppegno, P., Maj, M., Rossetti, M. C., Rossi, R., Santarelli, V., Giusti, L., Malavolta, M., Salza, A., Palumbo, D., Patriarca, S., Chieffi, M., Attrotto, M. T., Colagiorgio, L., Andriola, I., Atti, A. R., Barlati, S., Deste, G., Galluzzo, A., Pinna, F., Deriu, L., Sanna, L., Signorelli, M. S., Minutolo, G., Cannavo, D., Martinotti, G., Acciavatti, T., Corbo, M., Altamura, M., Carnevale, R., Malerba, S., Murri, M. B., Calcagno, P., Bugliani, M., Serati, M., Bartolomeis, A., Gramaglia, C., Gattoni, E., Gambaro, E., Collantoni, E., Cremonese, C., Rossi, E., Ossola, P., Tonna, M., Panfilis, C. D., Rutigliano, G., Gesi, C., Carmassi, C., Biondi, M., Girardi, P., Brugnoli, R., Fabio, F. D., Pietro, S. D., Girardi, N., Niolu, C., Lorenzo, G. D., Ribolsi, M., Corrivetti, G., Pinto, G., Longobardi, N., Fagiolini, A., Goracci, A., Bolognesi, S., Bellino, S., Villari, V., and Bracale, N.
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Adult ,Male ,Schizophrenia, Personal recovery, Clinical recovery, Insight, Recovery styles, Cluster analysis ,Clinical recovery ,Coping (psychology) ,Cross-sectional study ,Recovery style ,03 medical and health sciences ,Diagnostic Self Evaluation ,0302 clinical medicine ,Cluster analysis ,Recovery styles ,Insight ,Personal recovery ,Schizophrenia ,Cluster Analysis ,Cross-Sectional Studies ,Female ,Humans ,Psychiatric Status Rating Scales ,Self Report ,Recovery of Function ,Schizophrenic Psychology ,Cluster analysi ,Self report ,Settore MED/25 - Psichiatria ,Biological Psychiatry ,030227 psychiatry ,Psychiatry and Mental Health ,Psychiatric status rating scales ,Biological psychiatry ,Psychology ,030217 neurology & neurosurgery ,Clinical psychology - Abstract
Self-reported 'personal recovery' and clinical recovery in schizophrenia (SRPR and CR. respectively) reflect different perspectives in schizophrenia outcome, not necessarily concordant with each other and usually representing the consumer's or the therapist's point of view. By means of a cluster analysis on SRPR related variables, we identified three dusters. The first and third cluster included subjects with the best and the poorest clinical outcome respectively. The second cluster was characterized by better insight, higher levels of depression and stigma, lowest self-esteem and personal strength, and highest emotional coping. The first duster showed positive features of recovery, while the third duster showed negative features. The second cluster, with the most positive insight, showed a more complex pattern, a some-what 'paradoxical' mixture of positive and negative personal and clinical features of recovery. The present results suggest the need for a characterization of persons with schizophrenia along SRPR and CR dimensions to design individualized and integrated treatment programs aimed to improve insight and coping strategies, reduce stigma and shape recovery styles. (C) 2017 Elsevier B.V. All rights reserved.
- Published
- 2018
40. 12-O-tetradecanoylphorbol-13-acetate and EZH2 inhibition: A novel approach for promoting myogenic differentiation in embryonal rhabdomyosarcoma cells
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Francesco Fiorentino, Sanna L, Luigi Bagella, Irene Marchesi, Antonio Giordano, and Milena Fais
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0301 basic medicine ,Indoles ,Time Factors ,Pyridones ,Physiology ,Cellular differentiation ,Clinical Biochemistry ,macromolecular substances ,Biology ,GSK126 ,Muscle Development ,12-O-Tetradecanoylphorbol-13-acetate ,Methylation ,Cell Line ,Embryonal ,Histones ,03 medical and health sciences ,chemistry.chemical_compound ,0302 clinical medicine ,Cell Line, Tumor ,Antineoplastic Combined Chemotherapy Protocols ,Rhabdomyosarcoma ,medicine ,Humans ,Rhabdomyosarcoma, Embryonal ,Enhancer of Zeste Homolog 2 Protein ,EZH2 ,Enzyme Inhibitors ,Protein kinase C ,Tumor ,Myogenesis ,myogenesis ,rhabdomyosarcoma ,TPA ,Cell Cycle Checkpoints ,Cell Differentiation ,Drug Synergism ,Signal Transduction ,Tetradecanoylphorbol Acetate ,Cell Biology ,medicine.disease ,030104 developmental biology ,chemistry ,030220 oncology & carcinogenesis ,Cancer research ,Embryonal rhabdomyosarcoma ,Signal transduction - Abstract
Rhabdomyosarcoma (RMS) is a soft tissue sarcoma that arises from muscle precursors affecting predominately children and young adults. It can be divided into two main classes: embryonal (eRMS) and alveolar rhabodomyosarcomas (aRMS). Despite the expression of early muscle specific genes, RMS cells fail to complete myogenesis even in differentiation conditions. We previously demonstrated that Enhancer Zeste of Homolog 2 (EZH2), the catalytic subunits of PRC2 complex, contributes to inhibit muscle differentiation in eRMS and its down-regulation causes a partial recovery of myogenesis. 12-O-tetradecanoylphorbol-13-acetate (TPA) is a molecule able to induce differentiation in eRMS with a mechanism that involves the protein kinase C (PKC). In this paper we report that treatment with TPA reduces the expression of EZH2 without affecting levels of H3K27me3. The combination of TPA with GSK126, an inhibitor of the catalytic activity of EZH2, has a synergic effect on the induction of muscle differentiation in RD rhabdomyosarcoma cells, suggesting a new therapeutic combinatory approach for RMS treatment.
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- 2017
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41. Fluorescent Immunohistochemistry: An Important Tool to Reveal Proteins From Tissues in Ancient Mummified Remains
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Daniela Chessa, Salvatore Rubino, Vittorio Mazzarello, Paola Delaconi, Franco Campus, Sanna L, Maria Antonietta Demurtas, Nikki Kelvin, and David J. Kelvin
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Male ,0301 basic medicine ,Pathology ,medicine.medical_specialty ,Histology ,Crypt ,Fluorescent Antibody Technique ,Biology ,Pathology and Forensic Medicine ,03 medical and health sciences ,0302 clinical medicine ,Skin tissue ,medicine ,Humans ,030216 legal & forensic medicine ,Skin ,Muscles ,Proteins ,Mummies ,Immunohistochemistry ,General state ,Medical Laboratory Technology ,030104 developmental biology ,Italy ,Ultrastructure - Abstract
During the restoration of the Saint Antonio Abate Cathedral in Castelsardo, Sardinia, Italy, numerous human remains were found in a crypt. The burial site contained upwards of 120 individuals organized in successive layers from the bottom of the crypt; of these, 18 partially mummified individuals have been identified, including the last 2 individuals buried in the crypt. In the present study, we focused on these 2 individuals by initially adopting a morphologic and anthropological approach. The anthropological analysis of the remains showed that the 2 bodies were partially mummified and that most of the organs were not available; for this reason, the sex was determined by secondary sexual characteristics of the skulls and the long bones. The aim of this research was to describe the general state of the mummified bodies and tissues by morphologic and ultrastructural analysis using light and electron microscopy techniques. To ensure the preservation of specific tissue proteins, immunohistochemical fluorescence analysis was used. Limited information is available regarding the preservation of mummified tissues. Thus, this study demonstrated the presence of muscle and skin tissue markers in a good state of preservation, even though the tissues had undergone a slow mummification process. Our results demonstrate that several types of tissues and cell proteins may survive over a prolonged period and that these materials survive the postmortem processes.
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- 2017
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42. The Influence of AA29504 on GABAA Receptor Ligand Binding Properties and Its Implications on Subtype Selectivity.
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Sikstus, Sylvia, Benkherouf, Ali Y., Soini, Sanna L., and Uusi-Oukari, Mikko
- Subjects
LIGAND binding (Biochemistry) ,KNOCKOUT mice ,BINDING site assay ,ETHYL esters ,BINDING sites ,POTASSIUM channels ,BOTULINUM A toxins - Abstract
The unique pharmacological properties of δ-containing γ-aminobutyric acid type A receptors (δ-GABA
A Rs) make them an attractive target for selective and persistent modulation of neuronal excitability. However, the availability of selective modulators targeting δ-GABAA Rs remains limited. AA29504 ([2-amino-4-(2,4,6-trimethylbenzylamino)-phenyl]-carbamic acid ethyl ester), an analog of K+ channel opener retigabine, acts as an agonist and a positive allosteric modulator (Ago-PAM) of δ-GABAA Rs. Based on electrophysiological studies using recombinant receptors, AA29504 was found to be a more potent and effective agonist in δ-GABAA Rs than in γ2-GABAA Rs. In comparison, AA29504 positively modulated the activity of recombinant δ-GABAA Rs more effectively than γ2-GABAA Rs, with no significant differences in potency. The impact of AA29504's efficacy- and potency-associated GABAA R subtype selectivity on radioligand binding properties remain unexplored. Using [3 H]4'-ethynyl-4-n-propylbicycloorthobenzoate ([3 H]EBOB) binding assay, we found no difference in the modulatory potency of AA29504 on GABA- and THIP (4,5,6,7-tetrahydroisoxazolo[5,4-c]pyridin-3-ol)-induced responses between native forebrain GABAA Rs of wild type and δ knock-out mice. In recombinant receptors expressed in HEK293 cells, AA29504 showed higher efficacy on δ- than γ2 -GABAA Rs in the GABA-independent displacement of [3 H]EBOB binding. Interestingly, AA29504 showed a concentration-dependent stimulation of [3 H]muscimol binding to γ2 -GABAA Rs, which was absent in δ-GABAA Rs. This was explained by AA29504 shifting the low-affinity γ2 -GABAA R towards a higher affinity desensitized state, thereby rising new sites capable of binding GABAA R agonists with low nanomolar affinity. Hence, the potential of AA29504 to act as a desensitization-modifying allosteric modulator of γ2-GABAA Rs deserves further investigation for its promising influence on shaping efficacy, duration and plasticity of GABAA R synaptic responses. [ABSTRACT FROM AUTHOR]- Published
- 2022
- Full Text
- View/download PDF
43. A Multicenter, Randomized, Double-Blind Trial of Everolimus Versus Azathioprine and Placebo to Maintain Steroid-Induced Remission in Patients With Moderate-to-Severe Active Crohnʼs Disease
- Author
-
Reinisch, Walter, Panés, Julian, Lémann, Marc, Schreiber, Stefan, Feagan, B., Schmidt, Steven, Sturniolo, Giacomo C., Mikhailova, T., Alexeeva, Olga, Sanna, L., Haas, T., Korom, S., and Mayer, H.
- Published
- 2008
44. 'Verteporfin exhibits anti-proliferative activity in embryonal and alveolar rhabdomyosarcoma cell lines'
- Author
-
Sonia Vanina Forcales, Irene Marchesi, Sanna L, Luigi Bagella, Diego Francesco Calvisi, Valentina Bordoni, and Roberta Piredda
- Subjects
0301 basic medicine ,Poly (ADP-Ribose) Polymerase-1 ,Cell Cycle Proteins ,Toxicology ,medicine.disease_cause ,Proto-Oncogene Proteins c-myc ,03 medical and health sciences ,0302 clinical medicine ,Downregulation and upregulation ,Cell Line, Tumor ,medicine ,Humans ,Rhabdomyosarcoma, Embryonal ,Rhabdomyosarcoma ,Rhabdomyosarcoma, Alveolar ,Cell Proliferation ,Hippo signaling pathway ,Chemistry ,Cell growth ,Nuclear Proteins ,Verteporfin ,General Medicine ,Cell cycle ,medicine.disease ,G1 Phase Cell Cycle Checkpoints ,Cell biology ,030104 developmental biology ,030220 oncology & carcinogenesis ,Alveolar rhabdomyosarcoma ,Embryonal rhabdomyosarcoma ,Carcinogenesis ,Acyltransferases ,Transcription Factors - Abstract
Rhabdomyosarcoma (RMS) is a pediatric tumor, which arises from muscle precursor cells. Recently, it has been demonstrated that Hippo Pathway (Hpo), a pathway that regulates several physiological and biological features, is involved in RMS tumorigenesis. For instance, an upregulation of the Hpo downstream effector Yes-Associated Protein 1 (YAP) leads to the development of embryonal rhabdomyosarcoma (eRMS) in murine activated muscle satellite cells. On the other hand, the YAP paralog transcriptional co-activator with PDZ-binding motif (TAZ) is overexpressed in alveolar rhabdomyosarcoma (aRMS) patients with poor survival. YAP and TAZ exhibit both cytoplasmic and nuclear functions. In the nucleus, YAP binds TEADs (TEA domain family members) factors and together they constitute a complex that is able either to activate the transcription of several genes such as MYC, Tbx5 and PAX8 or to maintain the stability of others like p73. Due to the key role of YAP and TAZ in cancer, the identification and/or development of new compounds able to block their activity might be an effective antineoplastic strategy. Verteporfin (VP) is a molecule able to stop the formation of YAP/TEAD complex in the nucleus. The aim of this study is to evaluate the action of VP on RMS cell lines. This work shows that VP has an anti-proliferative activity on all RMS cell lines analyzed. Depending on RMS cell lines, VP affects cell cycle differently. Moreover, VP is able to decrease YAP protein levels, and to induce the activation of apoptosis mechanism through the cleavage of PARP-1. In addition, Annexin V assay showed the activation of apoptosis and necrosis after VP treatment. In summary, the ability of VP to disrupt RMS cell proliferation could be a novel and valuable strategy to improve the therapeutic approaches in treating rhabdomyosarcoma.
- Published
- 2019
45. Alcohol enhances hops modulation of GABA(A) receptors
- Author
-
Benkherouf, Ali, Soini, Sanna L., and Uusi-Oukari, Mikko
- Published
- 2019
- Full Text
- View/download PDF
46. 'Verteporfin exhibits anti-proliferative activity in embryonal and alveolar rhabdomyosarcoma cell lines'
- Author
-
Sanna, L, Piredda, R, Marchesi, I, Bordoni, V, Forcales, SV, Calvisi, DF, and Bagella, L
- Subjects
TAZ ,Anti-proliferation ,Rhabdomyosarcoma ,Verteporfin ,YAP ,Cancer - Abstract
Rhabdomyosarcoma (RMS) is a pediatric tumor, which arises from muscle precursor cells. Recently, it has been demonstrated that Hippo Pathway (Hpo), a pathway that regulates several physiological and biological features, is involved in RMS tumorigenesis. For instance, an upregulation of the Hpo downstream effector Yes-Associated Protein 1 (YAP) leads to the development of embryonal rhabdomyosarcoma (eRMS) in murine activated muscle satellite cells. On the other hand, the YAP paralog transcriptional co-activator with PDZ-binding motif (TAZ) is overexpressed in alveolar rhabdomyosarcoma (aRMS) patients with poor survival. YAP and TAZ exhibit both cytoplasmic and nuclear functions. In the nucleus, YAP binds TEADs (TEA domain family members) factors and together they constitute a complex that is able either to activate the transcription of several genes such as MYC, Tbx5 and PAX8 or to maintain the stability of others like p73. Due to the key role of YAP and TAZ in cancer, the identification and/or development of new compounds able to block their activity might be an effective antineoplastic strategy. Verteporfin (VP) is a molecule able to stop the formation of YAP/TEAD complex in the nucleus. The aim of this study is to evaluate the action of VP on RMS cell lines. This work shows that VP has an anti-proliferative activity on all RMS cell lines analyzed. Depending on RMS cell lines, VP affects cell cycle differently. Moreover, VP is able to decrease YAP protein levels, and to induce the activation of apoptosis mechanism through the cleavage of PARP-1. In addition, Annexin V assay showed the activation of apoptosis and necrosis after VP treatment. In summary, the ability of VP to disrupt RMS cell proliferation could be a novel and valuable strategy to improve the therapeutic approaches in treating rhabdomyosarcoma.
- Published
- 2019
47. Induction of hepatocyte proliferation by retinoic acid
- Author
-
Ledda-Columbano, G.M., Pibiri, M., Molotzu, F., Cossu, C., Sanna, L., Simbula, G., Perra, A., and Columbano, A.
- Published
- 2004
48. Flank Margin Caves In Telogenetic Limestones In Italy
- Author
-
Arriolabengoa, M, D’Angeli, I M, De Waele, J, Parise, M, Ruggieri, R, Sanna, L, Madonia, G, Vattano, M, Moore Kevin, White Susan, Arriolabengoa, Martin, D’Angeli, Ilenia Maria, De Waele, Jo, Parise, Mario, Ruggieri, Rosario, Sanna, Laura, Madonia, Giuliana, Vattano, Marco, Arriolabengoa, M, D’Angeli, I M, De Waele, J, Parise, M, Ruggieri, R, Sanna, L, Madonia, G, and Vattano, M
- Subjects
Settore GEO/04 - Geografia Fisica E Geomorfologia ,Karst ,salt-fresh water mixing, coastal karst, cave geomorphology, coastal uplift, speleogenesis - Abstract
Almost 20% of Italy is characterized by the outcropping of carbonate massifs ranging in age from Cambrian to Quaternary. Coastal karst is present in many Italian regions: from North-East to South and West: the Gulf of Trieste, the Conero (South of Ancona, Marche), the Adriatic coast of Apulia including Gargano, Murge and Salento, Maratea in Basilicata, Cilento in Campania, Circeo and Gaeta in Latium, Argentario and Giannutri Island in Tuscany, the southernmost part of the Ligurian Alps, Palermo Mts., San Vito Lo Capo, Syracuse coast and Marettimo Island in Sicily, and, especially, in Sardinia, which has carbonate rocks touching the sea along the coast of Balai near Porto Torres, Capo Caccia-Punta Giglio (Alghero), Sinis and Buggerru along the western litoral, Capo Teulada and Capo Sant’Elia at Cagliari, Capo Figari, Tavolara Island and the Gulf of Orosei along the eastern mountainside. Recent researches have revealed several coastal cave systems that have a clear origin by mixing corrosion, in which the aggressive solution derives from the mixing between saline and fresh water at the watertable interface (the so-called flank margin caves). Glacioeustasy and tectonic movements can control the position of sea level with respect to coastal carbonate outcrops. For this reason these coastal caves represent useful records of sea-level stillstands. These caves are normally organized in sub-horizontal levels, and are characterized by the lack of high flow velocity markers (scallops) and alluvial sediments. Instead, they show rounded cave passage morphologies, often with horizontal wall notches, a characteristic swiss-cheese or sponge morphology, and passages that narrow going away from the coastline (due to the decreasing of sea water influence and mixing-corrosion effect). This paper describes some flank margin cave systems found in Apulia, Sicily, and Sardinia. In particular, five cave systems are illustrated: Sant’Angelo caves (Apulia), Pellegrino and Rumena caves (Sicily), and Giuanniccu Mene cave and Fico cave (Sardinia), explaining their relationship with past sea levels and local uplift rate.
- Published
- 2017
49. Äiti, mitä nää oikein on? Monilapsisten perheiden ruokataloudenhoidosta selviytyminen
- Author
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Åman, Sanna L P, Soveltavan kasvatustieteen ja opettajankoulutuksen osasto, School of Applied Educational Science and Teacher Education, Filosofinen tiedekunta, Soveltavan kasvatustieteen ja opettajankoulutuksen osasto, Philosophical faculty, School of Applied Educational Science and Teacher Education, Filosofinen tiedekunta, and Philosophical faculty
- Subjects
home economics ,kotitaloustiede - Published
- 2018
50. Positive allosteric modulation of native and recombinant GABA
- Author
-
Ali Y, Benkherouf, Sanna L, Soini, Monika, Stompor, and Mikko, Uusi-Oukari
- Subjects
Flavonoids ,Male ,Prenylation ,Rats, Sprague-Dawley ,Binding Sites ,HEK293 Cells ,Allosteric Regulation ,Animals ,Humans ,Humulus ,Receptors, GABA-A ,Recombinant Proteins ,Rats - Abstract
Hops are a major component of beer that is added during brewing. In addition to its wide range of bioactivity, it exhibits neuroactive properties as a sedative and sleeping aid. The compounds responsible for this activity are yet to be revealed and understood in terms of their pharmacological properties. Here we evaluated the potential of several hops flavonoids in modulating the GABAergic activity and assessed their selectivity to GABA
- Published
- 2018
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