Your search keyword '"*BIOLOGY experiments"' showing total 22 results

1. Flavocoxid, a dual inhibitor of cyclooxygenase-2 and 5-lipoxygenase, reduces pancreatic damage in an experimental model of acute pancreatitis.

Author

Polito, F, Bitto, A, Irrera, N, Squadrito, F, Fazzari, C, Minutoli, L, and Altavilla, D

Subjects

*CYCLOOXYGENASE 2 inhibitors, *ENZYME inhibitors, *LIPOXYGENASES, *PANCREATIC injuries, *BIOLOGY experiments, *PANCREATITIS, *AUTOLYSIS

Abstract

Background and Purpose: Acute pancreatitis is an autodigestive process resulting in acute inflammation of the pancreas. Accumulating evidence indicates the essential contribution of cyclooxygenase (COX)-2 and 5-lipoxygenase (5-LOX) to acute pancreatitis. We studied the effects of flavocoxid, a plant-derived dual inhibitor of COX-2 and 5-LOX, in a model of caerulein (CER)-induced acute pancreatitis.Experimental Approach: Rats were given CER (80 µg·kg⁻¹ for each of four injections at hourly intervals) or vehicle (Sham-CER). Animals were then randomized to receive flavocoxid (20 mg·kg⁻¹ i.p.) or vehicle, 30 min after the first CER injection. Two hours after the last CER injection, we evaluated damage to the pancreas by histological methods; serum levels of amylase, lipase, leukotriene (LT)B₄ and prostaglandin (PG)E₂ ; pancreatic expression of COX-2 and 5-LOX and tumour necrosis factor-α (TNF-α) gene expression by real-time polymerase chain reaction.Key Results: Caerulein induced inflammatory changes in the pancreas and raised values of the other variables measured. In CER-treated animals, but not in those given saline, flavocoxid inhibited COX-2 and 5-LOX expression, reduced serum levels of lipase and amylase and the degree of pancreatic oedema. Treatment with flavocoxid blunted the increased pancreatic TNF-α mRNA expression, serum leukotriene B₄ and prostaglandin E₂ levels, and protected against histological damage in terms of vacuolization and leukocyte infiltration.Conclusions and Implications: Our results confirm the key role of both COX-2 and 5-LOX in the inflammatory response to acute pancreatitis. Flavocoxid may provide a potential therapeutic approach to the treatment of patients at high risk of developing this life-threatening condition. [ABSTRACT FROM AUTHOR]

Published

2010

2. Dapsone hydroxylamine induces premature removal of human erythrocytes by membrane reorganization and antibody binding.

Author

Bordin, Luciana, Fiore, Cristina, Zen, Francesco, Coleman, Michael D, Ragazzi, Eugenio, and Clari, Giulio

Subjects

*DAPSONE, *HYDROXYLAMINE, *ERYTHROCYTES, *IMMUNOGLOBULINS, *BINDING sites, *HYDROXYLATION, *BIOLOGY experiments, *IMMUNOGLOBULIN G

Abstract

Background and Purpose: N-hydroxylation of dapsone leads to the formation of the toxic hydroxylamines responsible for the clinical methaemoglobinaemia associated with dapsone therapy. Dapsone has been associated with decreased lifespan of erythrocytes, with consequences such as anaemia and morbidity in patients treated with dapsone for malaria. Here, we investigated how dapsone and/or its hydroxylamine derivative (DDS-NHOH) induced erythrocyte membrane alterations that could lead to premature cell removal.Experimental Approach: Erythrocytes from healthy donors were subjected to incubation with dapsone and DDS-NHOH for varying times and the band 3 protein tyrosine-phosphorylation process, band 3 aggregation, membrane alteration and IgG binding were all examined and compared with erythrocytes from two patients receiving dapsone therapy.Key Results: The hydroxylamine derivative, but not dapsone (the parent sulphone) altered membrane protein interactions, leading both to aggregation of band 3 protein and to circulating autologous antibody binding, shown in erythrocytes from patients receiving dapsone therapy. The band 3 tyrosine-phosphorylation process can be used as a diagnostic system to monitor membrane alterations both in vitro, assessing concentration and time-dependent effects of DDS-NHOH treatment, and in vivo, evaluating erythrocytes from dapsone-treated patients, in resting or oxidatively stimulated conditions.Conclusions and Implications: DDS-NHOH-induced alterations of human erythrocytes can be directly monitored in vitro by tyrosine-phosphorylation level and formation of band 3 protein aggregates. The latter, together with antibody-mediated labelling of erythrocytes, also observed after clinical use of dapsone, may lead to shortening of erythrocyte lifespan. [ABSTRACT FROM AUTHOR]

Published

2010

3. Agonists at the δ-opioid receptor modify the binding of µ-receptor agonists to the µ-δ receptor hetero-oligomer.

Author

Kabli, N, Martin, N, Fan, T, Nguyen, T, Hasbi, A, Balboni, G, O'Dowd, BF, George, SR, O'Dowd, B F, and George, S R

Subjects

*OPIOID receptors, *DOPAMINE agonists, *OLIGOMERS, *HETEROMETRY, *LIGAND binding (Biochemistry), *BIOLOGY experiments, *RADIOLIGAND assay, *IMMUNOFLUORESCENCE

Abstract

Background and Purpose: µ- and δ-opioid receptors form heteromeric complexes with unique ligand binding and G protein-coupling profiles linked to G protein α z-subunit (Gα(z) ) activation. However, the mechanism of action of agonists and their regulation of the µ-δ receptor heteromer are not well understood.Experimental Approach: Competition radioligand binding, cell surface receptor internalization in intact cells, confocal microscopy and receptor immunofluorescence techniques were employed to study the regulation of the µ-δ receptor heteromer in heterologous cells with and without agonist exposure.Key Results: Gα(z) enhanced affinity of some agonists at µ-δ receptor heteromers, independent of agonist chemical structure. δ-Opioid agonists displaced µ-agonist binding with high affinity from µ-δ heteromers, but not µ receptor homomers, suggestive of δ-agonists occupying a novel µ-receptor ligand binding pocket within the heteromers. Also, δ-agonists induced internalization of µ-opioid receptors in cells co-expressing µ- and δ-receptors, but not those expressing µ-receptors alone, indicative of µ-δ heteromer internalization. This dose-dependent, Pertussis toxin-resistant and clathrin- and dynamin-dependent effect required agonist occupancy of both µ- and δ-opioid receptors. In contrast to µ-receptor homomers, agonist-induced internalization of µ-δ heteromers persisted following chronic morphine exposure.Conclusions and Implications: The µ-δ receptor heteromer may contain a novel δ-agonist-detected, high-affinity, µ-receptor ligand binding pocket and is regulated differently from the µ-receptor homomer following chronic morphine exposure. Occupancy of both µ- and δ-receptor binding pockets is required for δ-agonist-induced endocytosis of µ-δ receptor heteromers. δ-Opioid agonists target µ-δ receptor heteromers, and thus have a broader pharmacological specificity than previously identified. [ABSTRACT FROM AUTHOR]

Published

2010

4. The anti-aggregating effect of BAY 41-2272, a stimulator of soluble guanylyl cyclase, requires the presence of nitric oxide.

Author

Roger, Séverine, Badier-Commander, Cécile, Paysant, Jérôme, Cordi, Alex, Verbeuren, Tony J, Félétou, Michel, Roger, Séverine, Badier-Commander, Cécile, Paysant, Jérôme, and Félétou, Michel

Subjects

*PLATELET aggregation inhibitors, *GUANYLATE cyclase, *NITRIC oxide, *BIOLOGY experiments, *ADENOSINES, *NITROGLYCERIN, *SODIUM nitroferricyanide, *VITAMIN B12, *NUCLEOTIDE metabolism, *ENZYME metabolism, *ANIMAL experimentation, *BLOOD platelet aggregation, *CARDIOVASCULAR agents, *CELL receptors, *CYCLIC adenylic acid, *DRUG interactions, *DRUG synergism, *HETEROCYCLIC compounds, *PROSTACYCLIN, *PYRIDINE, *RATS, *PHARMACODYNAMICS

Abstract

Background and Purpose: The purpose of the present study was to determine whether a stimulator of soluble guanylyl cyclase, BAY 41-2272, inhibits platelet aggregation and to clarify its interaction with nitric oxide (NO).Experimental Approach: Blood was collected from anaesthetized Wistar Kyoto rats. The aggregation of washed platelets was measured and the production of cAMP and cGMP was determined.Key Results: In adenosine 5'-diphosphate (ADP)-induced platelet aggregation, the anti-aggregating effects of BAY 41-2272, nitroglycerin, sodium nitroprusside and DEA-NONOate were associated with increased levels of cGMP while that of beraprost, a prostacyclin analogue, was correlated with an increase in cAMP. 1H-[1,2,4]oxadiazolo[4,3-a]quinoxalin-1-one (ODQ) prevented the effects of BAY 41-2272 and that of nitroglycerin and sodium nitroprusside, but only inhibited the increase in cGMP produced by of DEA-NONOate. Hydroxocobalamin, an NO scavenger, inhibited the effects of the three NO donors and BAY 41-2272 but did not affect those of beraprost. ADP-induced aggregation and the effects of BAY 41-2272 were not affected by L-nitroarginine. A positive interaction was observed between BAY 41-2272 and the three NO donors. BAY 41-2272 potentiated also the anti-aggregating effects of beraprost, and again this potentiation was inhibited by hydroxocobalamin.Conclusions and Implications: Inhibition of platelet aggregation by BAY 41-2272 requires the reduced form of soluble guanylyl cyclase and the presence of NO. The positive interaction observed between BAY 41-2272 and various NO donors is qualitatively similar whatever the mechanism involved in NO release. Furthermore, a potent synergism is observed between BAY 41-2272 and a prostacyclin analogue, but only in the presence of NO. [ABSTRACT FROM AUTHOR]

Published

2010

5. Biological actions of green tea catechins on cardiac troponin C.

Author

Tadano, Naoto, Du, Cheng-Kun, Yumoto, Fumiaki, Morimoto, Sachio, Ohta, Mika, Xie, Ming-Fang, Nagata, Koji, Zhan, Dong-Yun, Lu, Qun-Wei, Miwa, Yoshikazu, Takahashi-Yanaga, Fumi, Tanokura, Masaru, Ohtsuki, Iwao, and Sasaguri, Toshiyuki

Subjects

*GREEN tea, *CATECHIN, *POLYPHENOLS, *CARDIOVASCULAR disease prevention, *BIOLOGY experiments, *CYTOPLASMIC filaments, *MYOCARDIUM, *EPIGALLOCATECHIN gallate

Abstract

Background and Purpose: Catechins, biologically active polyphenols in green tea, are known to have a protective effect against cardiovascular diseases. In this study, we investigated direct actions of green tea catechins on cardiac muscle function to explore their uses as potential drugs for cardiac muscle disease.Experimental Approach: The effects of catechins were systematically investigated on the force-pCa relationship in skinned cardiac muscle fibres to determine their direct effects on cardiac myofilament contractility. The mechanisms of action of effective catechins were investigated using troponin exchange techniques, quartz crystal microbalance, nuclear magnetic resonance and a transgenic mouse model.Key Results: (-)-Epicatechin-3-gallate (ECg) and (-)-epigallocatechin-3-gallate (EGCg), but not their stereoismers (-)-catechin-3-gallate and (-)-gallocatechin-3-gallate, decreased cardiac myofilament Ca(2+) sensitivity probably through its interaction with cardiac troponin C. EGCg restored cardiac output in isolated working hearts by improving diastolic dysfunction caused by increased myofilament Ca(2+) sensitivity in a mouse model of hypertrophic cardiomyopathy.Conclusions and Implications: The green tea catechins, ECg and EGCg, are Ca(2+) desensitizers acting through binding to cardiac troponin C. These compounds might be useful compounds for the development of therapeutic agents to treat the hypertrophic cardiomyopathy caused by increased Ca(2+) sensitivity of cardiac myofilaments. [ABSTRACT FROM AUTHOR]

Published

2010

6. Spasticity therapy reacts to astrocyte GluA1 receptor upregulation following spinal cord injury.

Author

Gómez-Soriano, Julio, Goiriena, Eider, Taylor, Julian, and Gómez-Soriano, Julio

Subjects

*SPASTICITY, *ASTROCYTES, *SPINAL cord injuries, *THERAPEUTICS, *DRUG side effects, *DRUG withdrawal symptoms, *STRETCH reflex, *BIOLOGY experiments

Abstract

For almost three decades intrathecal baclofen therapy has been the standard treatment for spinal cord injury spasticity when oral medication is ineffective or produces serious side effects. Although intrathecal baclofen therapy has a good clinical benefit-risk ratio for spinal spasticity, tolerance and the life-threatening withdrawal syndrome present serious problems for its management. Now, in an experimental model of spinal cord injury spasticity, AMPA receptor blockade with NGX424(Tezampanel) has been shown to reduce stretch reflex activity alone and during tolerance to intrathecal baclofen therapy.These results stem from the observation that GluA1 receptors are overexpressed on reactive astrocytes following experimental ischaemic spinal cord injury. Although further validation is required, the appropriate choice of AMPA receptor antagonists for treatment of stretch hyperreflexia based on our recent understanding of reactive astrocyte neurobiology following spinal cord injury may lead to the development of a better adjunct clinical therapy for spasticity without the side effects of intrathecal baclofen therapy. [ABSTRACT FROM AUTHOR]

Published

2010

7. Pharmacological modulation by celecoxib of cachexia associated with experimental arthritis and atherosclerosis in rabbits.

Author

Romero, FI, Martínez-Calatrava, MJ, Sánchez-Pernaute, O, Gualillo, O, Largo, R, Herrero-Beaumont, G, Romero, F I, Martínez-Calatrava, M J, and Sánchez-Pernaute, O

Subjects

*PHARMACOLOGY, *ALLOSTERIC regulation, *CELECOXIB, *CACHEXIA, *BIOLOGY experiments, *ARTHRITIS, *ATHEROSCLEROSIS, *LABORATORY rabbits

Abstract

Background and Purpose: Non-steroidal anti-inflammatory drugs improve inflammatory cachexia in several conditions. Thus, we have explored inhibition of cyclooxygenase-2 (COX-2) in an experimental model of rheumatoid cachexia in rabbits.Experimental Approach: Chronic arthritis was induced in immunized rabbits by repeated intra-articular injections of ovalbumin. To increase the degree of systemic inflammation and also to induce atherosclerotic lesions, the animals were fed a hyperlipidaemic diet (2% cholesterol and 6% peanut oil) and were given an endothelial injury of the femoral artery. Rabbits were randomized to receive the COX-2 inhibitor celecoxib (10 mg·kg⁻¹ ·day⁻¹) or no treatment. After 4 weeks, sera, peripheral mononuclear cells and vessel specimens were collected.Key Results: Inhibition of COX-2 by celecoxib modulated the systemic inflammatory response and increased total cholesterol and triglyceride levels. Celecoxib also minimized weight loss and prevented serum albumin fall. At a vascular level, celecoxib reduced COX-2 protein in the femoral arterial wall, but did not modify size or the macrophage infiltration of femoral lesions nor the percentage of rabbits with spontaneous aortic plaques.Conclusions and Implications: Our animal model induced a severe inflammatory cachexia, comparable to that of persistently active rheumatoid arthritis. The inhibition of COX-2 by celecoxib improves this state, suggesting that COX products play an important role in its development, without affecting the development or the progression of vascular lesions. Overall, these results suggest that celecoxib might be considered as a new therapeutic tool for the treatment of rheumatoid cachexia. [ABSTRACT FROM AUTHOR]

Published

2010

8. Curcumin prevents leptin raising glucose levels in hepatic stellate cells by blocking translocation of glucose transporter-4 and increasing glucokinase.

Author

Tang, Youcai and Chen, Anping

Subjects

*LEPTIN, *GLUCOSE, *KUPFFER cells, *CHROMOSOMAL translocation, *GLUCOKINASE, *FIBROSIS, *BIOLOGY experiments, *PROTEIN kinases, *CELL metabolism, *GLUCOSE metabolism, *ANIMAL experimentation, *BIOLOGICAL transport, *CARRIER proteins, *CELL culture, *CELLS, *EPITHELIAL cells, *PHOSPHORYLATION, *RATS, *RESEARCH funding, *TRANSFERASES, *WESTERN immunoblotting, *CURCUMIN

Abstract

Background and Purpose: Hyperleptinemia is commonly found in obese patients, associated with non-alcoholic steatohepatitis and hepatic fibrosis. Hepatic stellate cells (HSCs) are the most relevant effectors during hepatic fibrogenesis. We recently reported that leptin stimulated HSC activation, which was eliminated by curcumin, a phytochemical from turmeric. This study was designed to explore the underlying mechanisms, focusing on their effects on intracellular glucose in HSCs. We hypothesized that leptin stimulated HSC activation by elevating the level of intracellular glucose, which was eliminated by curcumin by inhibiting the membrane translocation of glucose transporter-4 (GLUT4) and inducing the conversion of glucose to glucose-6-phosphate (G-6-P).Experimental Approach: Levels of intracellular glucose were measured in rat HSCs and immortalized human hepatocytes. Contents of GLUT4 in cell fractions were analysed by Western blotting analyses. Activation of signalling pathways was assessed by comparing phosphorylation levels of protein kinases.Key Results: Leptin elevated the level of intracellular glucose in cultured HSCs, which was diminished by curcumin. Curcumin suppressed the leptin-induced membrane translocation of GLUT4 by interrupting the insulin receptor substrates/phosphatidyl inositol 3-kinase/AKT signalling pathway. Furthermore, curcumin stimulated glucokinase activity, increasing conversion of glucose to G-6-P.Conclusions and Implications: Curcumin prevented leptin from elevating levels of intracellular glucose in activated HSCs in vitro by inhibiting the membrane translocation of GLUT4 and stimulating glucose conversion, leading to the inhibition of HSC activation. Our results provide novel insights into mechanisms of curcumin in inhibiting leptin-induced HSC activation. [ABSTRACT FROM AUTHOR]

Published

2010

9. Inhibition of vascular ectonucleotidase activities by the pro-drugs ticlopidine and clopidogrel favours platelet aggregation.

Author

Lecka, Joanna, Rana, Manjit Singh, Sévigny, Jean, and Sévigny, Jean

Subjects

*ENZYME inhibitors, *PRODRUGS, *TICLOPIDINE, *CLOPIDOGREL, *PLATELET aggregation inhibitors, *BIOLOGY experiments, *NUCLEOTIDES

Abstract

Background and Purpose: After conversion to their active forms by the liver, ticlopidine and clopidogrel exert antiplatelet effects through irreversible inhibition of the P2Y₁₂ receptor. Concentrations of nucleotides such as ADP, the physiological agonist at platelet P2Y₁ and P2Y₁₂ receptors, are regulated by vascular ectonucleotidases, mainly nucleoside triphosphate diphosphohydrolase (NTPDase)1 and ecto-5'-nucleotidase. Here we evaluate the effect of these pro-drugs on vascular ectonucleotidase activity and on the natural function of these enzymes in regulating platelet aggregation.Experimental Approach: Nucleotidase assays were performed by HPLC and by P(i) determination, using human umbilical vein endothelial cells (HUVEC) and protein extracts from transfected COS-7 cells as sources of enzymes. Platelet aggregation was assayed using human platelet-rich plasma.Key Results: Each pro-drug inhibited endothelial ectonucleotidase activities and decreased their ability to block platelet aggregation in vitro. At their therapeutic concentrations, ticlopidine (60 µM) and clopidogrel (20 µM) inhibited ADP hydrolysis by HUVEC by about 80%, and AMP hydrolysis by one-third. Accordingly, these compounds showed a mixed-type inhibition of recombinant human NTPDase1 with an apparent K(i) (K(i,app) ) of 10 µM (clopidogrel) and 14 µM (ticlopidine). Recombinant rat ecto-5'-nucleotidase, but not its human orthologue, was inhibited by ticlopidine with a K(i,app) of 4.5 mM.Conclusions and Implications: These pro-drugs facilitated platelet aggregation via the inhibition of vascular NTPDase1 in vitro. Further studies should be performed to assess whether this effect also occurs in vivo, especially at the beginning of treatment, before sufficient levels of active metabolites are produced by the liver. [ABSTRACT FROM AUTHOR]

Published

2010

10. Control of enteric neuromuscular functions by purinergic A(3) receptors in normal rat distal colon and experimental bowel inflammation.

Author

Antonioli, L, Fornai, M, Colucci, R, Ghisu, N, Tuccori, M, Awwad, O, Bin, A, Zoppellaro, C, Castagliuolo, I, Gaion, RM, Giron, MC, Blandizzi, C, Gaion, R M, and Giron, M C

Subjects

*NEUROMUSCULAR system, *PURINERGIC receptors, *LABORATORY rats, *COLON (Anatomy), *INFLAMMATION, *BIOLOGY experiments, *ADENOSINES

Abstract

Background and Purpose: Adenosine A(3) receptors mediate beneficial effects in experimental colitis, but their involvement in enteric neuromuscular functions during bowel inflammation is undetermined. This study investigated the regulatory role of A(3) receptors on colonic motility in the presence of experimental colitis.Experimental Approach: Colitis was induced in rats by 2,4-dinitrobenzenesulfonic acid. A(3) receptors and adenosine deaminase (ADA, adenosine catabolic enzyme) mRNA were examined by RT-PCR. Tissue distribution of A(3) receptors was detected by confocal immunofluorescence. The effects of 2,3-ethyl-4,5-dipropyl-6-phenylpyridine-3-thiocarboxylate-5-carboxylate (MRS1523) (MRS, A(3) receptor antagonist), 2-chloro-N(6) -(3-iodobenzyl)-adenosine-5'-N-methyluronamide (2Cl-IB-MECA) (CIB, A(3) receptor agonist), dipyridamole (DIP, adenosine transport inhibitor) and ADA were assayed on contractile responses evoked by electrical stimulation (ES) or carbachol in colonic longitudinal muscle preparations (LMP).Key Results: RT-PCR showed A(3) receptors and ADA mRNA in normal colon and their increased level in inflamed tissues. Immunofluorescence showed a predominant distribution of A(3) receptors in normal myenteric ganglia and an increased density during colitis. MRS enhanced ES-induced cholinergic contractions in normal LMP, but was less effective in inflamed tissues. After pretreatment with dipyridamole plus ADA, to reduce extracellular adenosine, CIB decreased cholinergic motor responses of normal LMP to ES, with enhanced efficacy in inflamed LMP. A(3) receptor ligands did not affect carbachol-induced contractions in LMP from normal or inflamed colon.Conclusions and Implications: Normally, adenosine modulated colonic cholinergic motility via activation of A(3) receptors in the myenteric plexus. A(3) receptor-mediated tonic inhibitory control by adenosine was impaired in inflamed bowel, despite increased density of functioning and pharmacologically recruitable A(3) receptors. [ABSTRACT FROM AUTHOR]

Published

2010

11. Investigating the interaction of McN-A-343 with the M muscarinic receptor using its nitrogen mustard derivative and ACh mustard.

Author

Figueroa, KW, Suga, H, Ehlert, FJ, Figueroa, K W, and Ehlert, F J

Subjects

*MUSCARINIC receptors, *ENZYME inhibitors, *NITROGEN mustards, *ALKYLATION, *BIOLOGY experiments, *SCOPOLAMINE, *ALLOSTERIC regulation

Abstract

Background and Purpose: We investigated how McN-A-343 inhibited the alkylation of the M(1) muscarinic receptor by its nitrogen mustard derivative and that of ACh to identify whether it interacts allosterically or orthosterically.Experimental Approach: We incubated the M(1) muscarinic receptor expressed in Chinese hamster ovary cells with ACh mustard for various periods of time in the presence of McN-A-343 or known allosteric and orthosteric ligands. After stopping the reaction and removing unreacted ligands, unalkylated receptors were measured using [(3)H]N-methylscopolamine. Analogous experiments were done using a nitrogen mustard analog of McN-A-343. Affinity constants, cooperativity values for allosteric interactions and rate constants for receptor alkylation were estimated using a mathematical model.Key Results: The kinetics of receptor alkylation by the nitrogen mustard derivatives of ACh and McN-A-343 were consistent with a two-step model in which the aziridinium ion rapidly forms a reversible receptor complex, which converts to a covalent complex at a slower rate. The inhibition of receptor alkylation by acetycholine, N-methylscopolamine and McN-A-343 was consistent with competitive inhibition, whereas that caused by gallamine was consistent with allosterism. Affinity constants estimated from alkylation kinetics agreed with those measured by displacement of [(3)H]N-methylscopolamine binding.Conclusions and Implications: Our results suggest that McN-A-343 and its nitrogen mustard derivative interact competitively with ACh and N-methylscopolamine at the orthosteric site on the M(1) muscarinic receptor. Measuring how drugs modulate the kinetics of receptor alkylation by an irreversible ligand is a powerful approach for distinguishing between negative allosteric modulators and competitive inhibitors. [ABSTRACT FROM AUTHOR]

Published

2010

12. Co-administration of ibuprofen and nitric oxide is an effective experimental therapy for muscular dystrophy, with immediate applicability to humans.

Author

Sciorati, Clara, Buono, Roberta, Azzoni, Emanuele, Casati, Silvana, Ciuffreda, Pierangela, D'Angelo, Grazia, Cattaneo, Dario, Brunelli, Silvia, and Clementi, Emilio

Subjects

*IBUPROFEN, *NITRIC oxide, *BIOLOGY experiments, *MUSCULAR dystrophy treatment, *ADRENOCORTICAL hormones, *ANTI-inflammatory agents, *STEM cells, *ANIMAL experimentation, *ANIMAL diseases, *CARDIOVASCULAR agents, *COMPARATIVE studies, *CYTOSKELETAL proteins, *DRUG synergism, *RESEARCH methodology, *MEDICAL cooperation, *MICE, *NONSTEROIDAL anti-inflammatory agents, *RESEARCH, *RESEARCH funding, *EVALUATION research, *ISOSORBIDE dinitrate (Drug), *PHARMACODYNAMICS

Abstract

Background and Purpose: Current therapies for muscular dystrophy are based on corticosteroids. Significant side effects associated with these therapies have prompted several studies aimed at identifying possible alternative strategies. As inflammation and defects of nitric oxide (NO) generation are key pathogenic events in muscular dystrophies, we have studied the effects of combining the NO donor isosorbide dinitrate (ISDN) and the non-steroidal anti-inflammatory drug ibuprofen.Experimental Approach: alpha-Sarcoglycan-null mice were treated for up to 8 months with ISDN (30 mg.kg(-1)) plus ibuprofen (50 mg.kg(-1)) administered daily in the diet. Effects of ISDN and ibuprofen alone were assessed in parallel. Drug effects on animal motility and muscle function, muscle damage, inflammatory infiltrates and cytokine levels, as well as muscle regeneration including assessment of endogenous stem cell pool, were measured at selected time points.Key Results: Combination of ibuprofen and ISDN stimulated regeneration capacity, of myogenic precursor cells, reduced muscle necrotic damage and inflammation. Muscle function in terms of free voluntary movement and resistance to exercise was maintained throughout the time window analysed. The effects of ISDN and ibuprofen administered separately were transient and significantly lower than those induced by their combination.Conclusions and Implications: Co-administration of NO and ibuprofen provided synergistic beneficial effects in a mouse model of muscular dystrophy, leading to an effective therapy. Our results open the possibility of immediate clinical testing of a combination of ISDN and ibuprofen in dystrophic patients, as both components are approved for use in humans, with a good safety profile. [ABSTRACT FROM AUTHOR]

Published

2010

13. A series of structurally novel heterotricyclic alpha-amino-3-hydroxyl-5-methyl-4-isoxazole-propionate receptor-selective antagonists.

Author

Gill, MB, Frausto, S, Ikoma, M, Sasaki, M, Oikawa, M, Sakai, R, Swanson, GT, Gill, M B, and Swanson, G T

Subjects

*AMINO group, *GLUTAMIC acid, *MOLECULAR structure, *HYDROXYL group, *METHYL groups, *PROPIONATES, *ENZYME inhibitors, *BIOLOGY experiments, *DRUG antagonism, *ANIMAL experimentation, *BINDING sites, *CELL lines, *CELL receptors, *COMPARATIVE studies, *CYTOLOGICAL techniques, *HETEROCYCLIC compounds, *HIPPOCAMPUS (Brain), *KIDNEYS, *RESEARCH methodology, *MEDICAL cooperation, *MICE, *NEURAL transmission, *NEURONS, *RADIOISOTOPES in medical diagnosis, *RESEARCH, *EVALUATION research, *STATUS epilepticus

Abstract

Background and Purpose: A new class of heterotricyclic glutamate analogues recently was generated by incorporating structural elements of two excitotoxic marine compounds, kainic acid and neodysiherbaine A. Rather than acting as convulsants, several of these 'IKM' compounds markedly depressed CNS activity in mice. Here, we characterize the pharmacological profile of the series with a focus on the most potent of these molecules, IKM-159.Experimental Approach: The pharmacological activity and specificity of IKM compounds were characterized using whole-cell patch clamp recording from neurons and heterologous receptor expression systems, in combination with radioligand binding techniques.Key Results: The majority of the IKM compounds tested reduced excitatory synaptic transmission in neuronal cultures, and IKM-159 inhibited synaptic currents from CA1 pyramidal neurons in hippocampal slices. IKM-159 inhibited glutamate-evoked whole-cell currents from recombinant GluA2- and GluA4-containing alpha-amino-3-hydroxyl-5-methyl-4-isoxazole-propionate (AMPA) receptors most potently, whereas kainate and NMDA receptor currents were not reduced by IKM-159. Antagonism of steady-state currents was agonist concentration dependent, suggesting that its mechanism of action was competitive, although it paradoxically did not displace [(3)H]-AMPA from receptor binding sites. IKM-159 reduced spontaneous action potential firing in both cultured hippocampal neurons in control conditions and during hyperactive states in an in vitro model of status epilepticus.Conclusions and Implications: IKM-159 is an AMPA receptor-selective antagonist. IKM-159 and related nitrogen heterocycles represent structurally novel AMPA receptor antagonists with accessible synthetic pathways and potentially unique pharmacology, which could be of use in exploring the role of specific populations of receptors in neurophysiological and neuropathological processes. [ABSTRACT FROM AUTHOR]

Published

2010

14. Chemo-nociceptive signalling from the colon is enhanced by mild colitis and blocked by inhibition of transient receptor potential ankyrin 1 channels.

Author

Mitrovic, Martina, Shahbazian, Anaid, Bock, Elisabeth, Pabst, Maria A., and Holzer, Peter

Subjects

*CELLULAR signal transduction, *COLITIS, *TRP channels, *COLON (Anatomy), *BIOLOGY experiments, *DEXTRAN, *SODIUM sulfate, *CAPSAICIN, *AMIDES, *ANALYSIS of variance, *ANIMAL experimentation, *BIOLOGICAL models, *CARRIER proteins, *GENES, *HISTOLOGICAL techniques, *IMMUNOHISTOCHEMISTRY, *MICE, *MICROSCOPY, *MORPHINE, *PURINES, *RESEARCH funding, *SENSORY neurons, *SPINAL cord, *STATISTICS, *T-test (Statistics), *PHYTOCHEMICALS, *DATA analysis, *DATA analysis software, *DESCRIPTIVE statistics, *KRUSKAL-Wallis Test, *CHEMICAL inhibitors, *PHARMACODYNAMICS

Abstract

Background and Purpose: Transient receptor potential ankyrin 1 (TRPA1) channels are expressed by primary afferent neurones and activated by irritant chemicals including allyl isothiocyanate (AITC). Here we investigated whether intracolonic AITC causes afferent input to the spinal cord and whether this response is modified by mild colitis, morphine or a TRPA1 channel blocker.Experimental Approach: One hour after intracolonic administration of AITC to female mice, afferent signalling was visualized by expression of c-Fos in laminae I-II(o) of the spinal dorsal horn at sacral segment S1. Mild colitis was induced by dextran sulphate sodium (DSS) added to drinking water for 1 week.Key Results: Relative to vehicle, AITC (2%) increased expression of c-Fos in the spinal cord. Following induction of mild colitis by DSS (2%), spinal c-Fos responses to AITC, but not vehicle, were augmented by 41%. Colonic inflammation was present (increased myeloperoxidase content and disease activity score), whereas colonic histology, locomotion, feeding and drinking remained unchanged. Morphine (10 mg.kg(-1)) or the TRPA1 channel blocker HC-030031 (300 mg.kg(-1)) inhibited the spinal c-Fos response to AITC, in control and DSS-pretreated animals, whereas the response to intracolonic capsaicin (5%) was blocked by morphine but not HC-030031.Conclusions and Implications: Activation of colonic TRPA1 channels is signalled to the spinal cord. Mild colitis enhanced this afferent input that, as it is sensitive to morphine, is most likely of a chemonociceptive nature. As several irritant chemicals can be present in chyme, TRPA1 channels may mediate several gastrointestinal pain conditions. [ABSTRACT FROM AUTHOR]

Published

2010

15. Sublethal concentrations of the platinum(II) complex [Pt(O,O'-acac)(gamma-acac)(DMS)] alter the motility and induce anoikis in MCF-7 cells.

Author

Muscella, Antonella, Calabriso, Nadia, Vetrugno, Carla, Urso, Loredana, Fanizzi, Francesco Paolo, De Pascali, Sandra Angelica, and Marsigliante, Santo

Subjects

*LETHAL mutations, *PLATINUM compounds, *APOPTOSIS, *BIOLOGY experiments, *CELLULAR signal transduction, *GELATIN, *METASTASIS

Abstract

Background and Purpose: We showed previously that a new Pt(II) complex ([Pt(O,O'-acac)(gamma-acac)(DMS)]) exerted high and fast apoptotic processes in MCF-7 cells. The objective of this study was to investigate the hypothesis that [Pt(O,O'-acac)(gamma-acac)(DMS)] is also able to exert anoikis and alter the migration ability of MCF-7 cells, and to show some of the signalling events leading to these alterations.Experimental Approach: Cells were treated with sublethal doses of [Pt(O,O'-acac)(gamma-acac)(DMS)], and the efficiency of colony initiation and anchorage-independent growth was assayed; cell migration was examined by in vitro culture wounding assay. Gelatin zymography for MMP-2 and -9 activities, Western blottings of MMPs, MAPKs, Src, PKC-epsilon and FAK, after [Pt(O,O'-acac)(gamma-acac)(DMS)] treatment, were also performed.Key Results: Sub-cytotoxic drug concentrations decreased the: (i) anchorage-dependent and -independent growth; (ii) migration ability; and (iii) expression and activity of MMP-2 and MMP-9. [Pt(O,O'-acac)(gamma-acac)(DMS)] provoked the generation of reactive oxygen species (ROS), and the activation of p38MAPK, Src and PKC-epsilon. p38MAPK phosphorylation, cell anoikis and migration due to [Pt(O,O'-acac)(gamma-acac)(DMS)] were blocked by PKC-epsilon inhibition. Furthermore, Src inhibition blocked the [Pt(O,O'-acac)(gamma-acac)(DMS)]-provoked activation of PKC-epsilon, while ROS generation blockage inhibited the activation of Src, and also the decrement of phosphorylated FAK observed in detached [Pt(O,O'-acac)(gamma-acac)(DMS)]-treated cells.Conclusions and Implications: Sublethal concentrations of [Pt(O,O'-acac)(gamma-acac)(DMS)] induced anoikis and prevented events leading to metastasis via alterations in cell migration, anchorage independency, stromal interactions and MMP activity. Hence, [Pt(O,O'-acac)(gamma-acac)(DMS)] may be a promising therapeutic agent for preventing growth and metastasis of breast cancer. [ABSTRACT FROM AUTHOR]

Published

2010

16. Molecular determinants of state-dependent block of voltage-gated sodium channels by pilsicainide.

Author

Desaphy, J-F, Dipalma, A, Costanza, T, Bruno, C, Lentini, G, Franchini, C, George, AL, and Conte Camerino, D

Subjects

*EPITOPES, *SODIUM channels, *MYOCARDIAL depressants, *BIOLOGY experiments, *GENE expression, *MUSCLE protein metabolism, *BRAIN, *CELL lines, *COMPARATIVE studies, *CYTOLOGICAL techniques, *FLECAINIDE, *HEART, *LIDOCAINE, *RESEARCH methodology, *MEDICAL cooperation, *MEMBRANE proteins, *MEXILETINE, *MUSCLE proteins, *NERVE tissue proteins, *RESEARCH, *RESEARCH funding, *EVALUATION research, *SODIUM channel blockers, *SKELETAL muscle, *MEMBRANE transport proteins, *PHARMACODYNAMICS, BRAIN metabolism

Abstract

Background and Purpose: Pilsicainide, an anti-arrhythmic drug used in Japan, is described as a pure sodium channel blocker. We examined the mechanisms by which it is able to block open channels, because these properties may be especially useful to reduce hyperexcitability in pathologies characterized by abnormal sodium channel opening.Experimental Approach: The effects of pilsicainide on various heterologously expressed human sodium channel subtypes and mutants were investigated using the patch clamp technique.Key Results: Pilsicainide exhibited tonic and use-dependent effects comparable to those of mexiletine and flecainide on hNav1.4 channels. These use-dependent effects were abolished in the mutations F1586C and Y1593C within segment 6 of domain IV, suggesting that the interaction of pilsicainide with these residues is critical for its local anaesthetic action. Its affinity constants for closed channels (K(R)) and channels inactivated from the closed state (K(I)) were high, suggesting that its use-dependent block (UDB) requires the channel to be open for it to reach a high-affinity blocking site. Accordingly, basic pH, which slightly increased the proportion of neutral drug, dramatically decreased K(R) and K(I) values. Effects of pilsicainide were similar on skeletal muscle hNav1.4, brain hNav1.1 and heart hNav1.5 channels. The myotonic R1448C and G1306E hNav1.4 mutants were more and less sensitive to pilsicainide, respectively, due to mutation-induced gating modifications.Conclusions and Implications: Although therapeutic concentrations of pilsicainide may have little effect on resting and closed-state inactivated channels, it induces a strong UDB due to channel opening, rendering the drug ideally suited for inhibition of high-frequency action potential firing. [ABSTRACT FROM AUTHOR]

Published

2010

17. The transient receptor potential channel antagonist SKF96365 is a potent blocker of low-voltage-activated T-type calcium channels.

Author

Singh, A, Hildebrand, ME, Garcia, E, Snutch, TP, Hildebrand, M E, and Snutch, T P

Subjects

*TRP channels, *CALCIUM antagonists, *CALCIUM channels, *PURKINJE cells, *GENE expression, *BIOLOGY experiments, *MOLECULAR genetics, *CALCIUM metabolism, *ANIMAL experimentation, *CALCIUM, *CELL lines, *COMPARATIVE studies, *CYTOLOGICAL techniques, *IMIDAZOLES, *KIDNEYS, *RESEARCH methodology, *MEDICAL cooperation, *NEURONS, *RATS, *RESEARCH, *RESEARCH funding, *EVALUATION research, *PHARMACODYNAMICS

Abstract

Background and Purpose: SKF96365 (SKF), originally identified as a blocker of receptor-mediated calcium entry, is widely used diagnostically, as a blocker of transient receptor potential canonical type (TRPC) channels. While SKF has been used as a tool to define the functional roles of TRPC channels in various cell and tissue types, there are notable overlapping physiological and pathophysiological associations between TRPC channels and low-voltage-activated (LVA) T-type calcium channels. The activity of SKF against T-type Ca channels has not been previously explored, and here we systematically investigated the effects of SKF on recombinant and native voltage-gated Ca channel-mediated currents.Experimental Approach: Effects of SKF on recombinant Ca channels were studied under whole-cell patch clamp conditions after expression in HEK293 cells. The effect of SKF on cerebellar Purkinje cells (PCs) expressing native T-type Ca channels was also assessed.Key Results: SKF blocked recombinant Ca channels, representative of each of the three main molecular genetic classes (Ca(V)1, Ca(V)2 and Ca(V)3) at concentrations typically utilized to assay TRPC function (10 microM). Particularly, human Ca(V)3.1 T-type Ca channels were more potently inhibited by SKF (IC(50) approximately 560 nM) in our experiments than previously reported for similarly expressed TRPC channels. SKF also inhibited native Ca(V)3.1 T-type currents in a rat cerebellar PC slice preparation.Conclusions and Implications: SKF was a potent blocker of LVA T-type Ca channels. We suggest caution in the interpretation of results using SKF alone as a diagnostic agent for TRPC activity in native tissues. [ABSTRACT FROM AUTHOR]

Published

2010

18. Increased morphine analgesia and reduced side effects in mice lacking the tac1 gene.

Author

Bilkei-Gorzo, A, Berner, J, Zimmermann, J, Wickström, R, Racz, I, Zimmer, A, and Wickström, R

Subjects

*MORPHINE, *ANALGESIA, *DRUG side effects, *LABORATORY mice, *TACHYKININS, *OPIOIDS, *BIOLOGY experiments, *PHARMACOLOGY

Abstract

Background and Purpose: Although morphine is a very effective analgesic, its narrow therapeutic index and severe side effects limit its therapeutic use. Previous studies indicated that the pharmacological responses of opioids are modulated by genetic and pharmacological invalidation of tachykinin receptors. Here we address the role of substance P and neurokinin A, which are both encoded by the tachykinin 1 (tac1) gene, as modulators of opioid effects.Experimental Approach: The analgesic and side effect potential of morphine was compared between wild-type and tac1 null mutant mice.Key Results: Morphine was a more potent analgesic in tac1 null mutant mice, that is, in the absence of substance P/neurokinin A signalling. Interestingly, the most serious side effect of acute morphine, that is respiratory depression, was reduced in tac1(-/-) animals. Comparing the addictive potential of morphine in wild-type and knockout animals we found that morphine preference was similar between the genotypes. However, the aversive effect of withdrawal precipitated by naloxone in morphine-dependent animals was significantly reduced in tac1 knockout mice. Behavioural sensitization, the underlying mechanism of addiction, was also significantly lower in tac1(-/-) mice.Conclusion and Implications: The analgesic potential of morphine was increased in tac1 knockout mice. In contrast, both the ventilatory suppressing effect and the addictive potential of morphine were reduced. These results suggest that reducing activity of the tachykinin system may be a possible strategy to improve the pharmacological potential of morphine. [ABSTRACT FROM AUTHOR]

Published

2010

19. The selectivity of beta-adrenoceptor agonists at human beta1-, beta2- and beta3-adrenoceptors.

Author

Baker, Jillian G

Subjects

*ADRENERGIC receptors, *RECEPTOR-ligand complexes, *CELL lines, *BIOLOGY experiments, *RADIOLIGAND assay, *GENE transfection, *ADRENERGIC beta agonists, *ANIMAL experimentation, *CYCLIC adenylic acid, *HAMSTERS, *PROPANOLAMINES, *RADIOISOTOPES in medical diagnosis, *RODENTS, *PHARMACODYNAMICS

Abstract

Background and Purpose: There are two important properties of receptor-ligand interactions: affinity (the ability of the ligand to bind to the receptor) and efficacy (the ability of the receptor-ligand complex to induce a response). Ligands are classified as agonists or antagonists depending on whether or not they have efficacy. In theory, it is possible to develop selective agonists based on selective affinity, selective intrinsic efficacy or both. This study examined the affinity and intrinsic efficacy of 31 beta-adrenoceptor agonists at the three human beta-adrenoceptors to determine whether the current agonists are subtype selective because of affinity or intrinsic efficacy.Experimental Approach: Stable clonal CHO-K1 cell lines, transfected with either the human beta(1), beta(2) or beta(3)-adrenoceptor, were used, and whole-cell [(3)H]-CGP 12177 radioligand binding and [(3)H]-cAMP accumulation were measured.Key Results: Several agonists were found to be highly subtype selective because of selective affinity (e.g. salmeterol and formoterol, for the beta(2)-adrenoceptor over the beta(1) or beta(3)), while others (e.g. isoprenaline) had little affinity-selectivity. However, the intrinsic efficacy of salmeterol, formoterol and isoprenaline was similar across all three receptor subtypes. Other ligands (e.g. denopamine for beta(1); clenbuterol, AZ 40140d, salbutamol for beta(2)) were found to have subtype-selective intrinsic efficacy. Several ligands appeared to activate two agonist conformations of the beta(1)- and beta(3)-adrenoceptors.Conclusions and Implications: There are agonists with subtype selectivity based upon both selective affinity and selective intrinsic efficacy. Therefore, there is scope to develop better selective agonists based upon both selective affinity and selective intrinsic efficacy. [ABSTRACT FROM AUTHOR]

Published

2010

20. Effects of cytochrome P450 3A (CYP3A) and the drug transporters P-glycoprotein (MDR1/ABCB1) and MRP2 (ABCC2) on the pharmacokinetics of lopinavir.

Author

Van Waterschoot, RAB, Ter Heine, R, Wagenaar, E, Van Der Kruijssen, CMM, Rooswinkel, RW, Huitema, ADR, Beijnen, JH, Schinkel, AH, van Waterschoot, R A B, van der Kruijssen, C M M, Rooswinkel, R W, Huitema, A D R, Beijnen, J H, and Schinkel, A H

Subjects

*CYTOCHROME P-450, *P-glycoprotein, *PHARMACOKINETICS, *LOPINAVIR-ritonavir, *BIOAVAILABILITY, *BIOLOGY experiments, *ANIMAL experimentation, *CARRIER proteins, *COMPARATIVE studies, *DOGS, *DRUG interactions, *GLYCOPROTEINS, *HETEROCYCLIC compounds, *INTESTINES, *LIVER, *RESEARCH methodology, *MEDICAL cooperation, *MICE, *OXIDOREDUCTASES, *RESEARCH, *EVALUATION research, *HIV protease inhibitors, *RITONAVIR, *PHARMACODYNAMICS

Abstract

Background and Purpose: Lopinavir is extensively metabolized by cytochrome P450 3A (CYP3A) and is considered to be a substrate for the drug transporters ABCB1 (P-glycoprotein) and ABCC2 (MRP2). Here, we have assessed the individual and combined effects of CYP3A, ABCB1 and ABCC2 on the pharmacokinetics of lopinavir and the relative importance of intestinal and hepatic metabolism. We also evaluated whether ritonavir increases lopinavir oral bioavailability by inhibition of CYP3A, ABCB1 and/or ABCC2.Experimental Approach: Lopinavir transport was measured in Madin-Darby canine kidney cells expressing ABCB1 or ABCC2. Oral lopinavir kinetics (+/- ritonavir) was studied in mice with genetic deletions of Cyp3a, Abcb1a/b and/or Abcc2, or in transgenic mice expressing human CYP3A4 exclusively in the liver and/or intestine.Key Results: Lopinavir was transported by ABCB1 but not by ABCC2 in vitro. Lopinavir area under the plasma concentration - time curve (AUC)(oral) was increased in Abcb1a/b(-/-) mice (approximately ninefold vs. wild-type) but not in Abcc2(-/-) mice. Increased lopinavir AUC(oral) (>2000-fold) was observed in cytochrome P450 3A knockout (Cyp3a(-/-)) mice compared with wild-type mice. No difference in AUC(oral) between Cyp3a(-/-) and Cyp3a/Abcb1a/b/Abcc2(-/-) mice was observed. CYP3A4 activity in intestine or liver, separately, reduced lopinavir AUC(oral) (>100-fold), compared with Cyp3a(-/-) mice. Ritonavir markedly increased lopinavir AUC(oral) in all CYP3A-containing mouse strains.Conclusions and Implications: CYP3A was the major determinant of lopinavir pharmacokinetics, far more than Abcb1a/b. Both intestinal and hepatic CYP3A activity contributed importantly to low oral bioavailability of lopinavir. Ritonavir increased lopinavir bioavailability primarily by inhibiting CYP3A. Effects of Abcb1a/b were only detectable in the presence of CYP3A, suggesting saturation of Abcb1a/b in the absence of CYP3A activity. [ABSTRACT FROM AUTHOR]

Published

2010

21. Tuning in to the ‘right’ calcium channel regulation in experimental models of diabetes.

Author

Sturek, M

Subjects

*CALCIUM channels, *BIOLOGY experiments, *ANIMAL models of diabetes, *MOLECULAR biology, *CELLULAR mechanics, *VASCULAR smooth muscle, *GENE expression, *CELL metabolism, *CALCIUM metabolism, *CLINICAL trials, *MUSCLE contraction, *SMOOTH muscle, *HYPERGLYCEMIA, *BLOOD vessels, *DIABETES, *ATHEROSCLEROSIS, *VASODILATION, *WASTING syndrome, *MICE, *ANIMALS

Abstract

Elucidation of cellular and molecular mechanisms underlying vascular disease is of fundamental importance to the development of pharmacological agents to target these pathways. Pinho et al. in this issue of the BJP provide highly compelling evidence that the δ isoform of phosphatidyl inositol 3-kinase (PI3K δ) was upregulated and accounted for the increase in L-type, voltage-gated, Ca channel current in aortic vascular smooth muscle (VSM) cells of a mouse model of type 1 diabetes. There are several key issues of broad fundamental significance to this work. Firstly, what is the ‘right’ answer about calcium channel regulation in diabetes? Conflicting reports of increased and decreased Ca channel current may be due to specificity of the vascular bed and species. Then, the time course of diabetic vasculopathy may influence the expression of contractile versus proliferative phenotypes of VSM. Also the metabolic characterization of diabetes may enlighten or confound any study of diabetic vascular disease. These issues need attention to move forward work in this area. [ABSTRACT FROM AUTHOR]

Published

2010

22. Declaration of transparency and scientific rigour: checklist for design & analysis.

Subjects

*SCIENTIFIC experimentation, *CYTOLOGICAL research, *BIOLOGY experiments, *CHEMISTRY experiments, *ANALYSIS of variance, *RANDOMIZED controlled trials, *EXPERIMENTAL design

Published

2018