Your search keyword '"isobologram"' showing total 26 results

1. Serotonin enhances oxybuprocaine- and proxymetacaine-induced cutaneous analgesia in rats.

Author

Chou, An-Kuo, Chiu, Chong-Chi, Wang, Jhi-Joung, Chen, Yu-Wen, and Hung, Ching-Hsia

Subjects

*SEROTONIN, *ANALGESIA, *PHARMACOLOGY, *DRUGS, *PHARMACY

Abstract

Abstract The aim of the study was to investigate the analgesic effects of adding serotonin to oxybuprocaine or proxymetacaine preparations. We employed a rat model of the cutaneous trunci muscle reflex (CTMR) to conduct the dose-response curves and duration of drugs (oxybuprocaine, proxymetacaine, or serotonin) as an infiltrative anesthetic. The use of isobolographic methods to analyze the drug-drug interactions. We showed that oxybuprocaine and proxymetacaine, as well as serotonin produced dose-dependent skin antinociception. On the basis of 50% effective dose (ED 50), the rank order of drug potency was serotonin [7.22 (6.45–8.09) μmol/kg] < oxybuprocaine [1.03 (0.93–1.15) μmol/kg] < proxymetacaine [0.59 (0.53–0.66) μmol/kg] (P < 0.01 for each comparison). The sensory block duration of serotonin was longer (P < 0.01) than that of oxybuprocaine or proxymetacaine at the equipotent doses (ED 25 , ED 50 , and ED 75). The mixture of serotonin with oxybuprocaine or proxymetacaine produced a better analgesic effect than the drug itself. We have concluded that oxybuprocaine, proxymetacaine, or serotonin displays dose-related cutaneous analgesia. Oxybuprocaine or proxymetacaine is more potent and has a shorter duration of cutaneous analgesia than serotonin. Serotonin produces a synergistic antinociceptive interaction with oxybuprocaine or proxymetacaine. [ABSTRACT FROM AUTHOR]

Published

2019

2. Lumefantrine attenuates Plasmodium falciparum artemisinin resistance during the early ring stage

Author

Prapon Wilairat, Maria G. Gomez-Lorenzo, Thanat Chookajorn, Kesinee Chotivanich, Krittikorn Kümpornsin, Laura M. Sanz, Cristina de Cozar, Marcus C. S. Lee, Namfon Kotanan, Duangkamon Loesbanluechai, Nicholas J. White, and Francisco-Javier Gamo

Subjects

Drug, Regular article, Artemisinins, media_common.quotation_subject, Plasmodium falciparum, Protozoan Proteins, Drug resistance, Infectious and parasitic diseases, RC109-216, Pharmacology, Lumefantrine, Antimalarials, chemistry.chemical_compound, Isobologram, parasitic diseases, medicine, Humans, Pharmacology (medical), Artemether, Malaria, Falciparum, Artemisinin, media_common, biology, business.industry, biology.organism_classification, medicine.disease, Malaria, Infectious Diseases, chemistry, Parasitology, business, medicine.drug

Abstract

Emerging artemisinin resistance in Plasmodium falciparum malaria has the potential to become a global public health crisis. In Southeast Asia, this phenomenon clinically manifests in the form of delayed parasite clearance following artemisinin treatment. Reduced artemisinin susceptibility is limited to the early ring stage window, which is sufficient to allow parasites to survive the short half-life of artemisinin exposure. A screen of known clinically-implemented antimalarial drugs was performed to identify a drug capable of enhancing the killing activity of artemisinins during this critical resistance window. As a result, lumefantrine was found to increase the killing activity of artemisinin against an artemisinin-resistant clinical isolate harboring the C580Y kelch13 mutation. Isobologram analysis revealed synergism during the early ring stage resistance window, when lumefantrine was combined with artemether, an artemisinin derivative clinically partnered with lumefantrine. These findings suggest that lumefantrine should be clinically explored as a partner drug in artemisinin-based combination therapies to control emerging artemisinin resistance., Graphical abstract Image 1, Highlights • Artemisinin booster compound screening targeting the early ring resistance window in Plasmodium falciparum was performed. • Lumefantrine improves the activity of artesunate against the parasite during the resistance window. • Artemether and lumefantrine are synergistic during the early ring stage resistance window.

Published

2021

3. Synergistic effect of ursolic acid and piperine in CCl4 induced hepatotoxicity

Author

Sayan Biswas, Pallab Kanti Haldar, Pulok K. Mukherjee, Amit Kar, and Nanaocha Sharma

Subjects

Polyunsaturated Alkamides, CCL4, Pharmacology, Protective Agents, isobologram, chemistry.chemical_compound, Alkaloids, Pharmacokinetics, Ursolic acid, Piperidines, Animals, Humans, Benzodioxoles, Hepatoprotective Agent, Carbon Tetrachloride, Chemistry, Combination index, General Medicine, Hepatoprotective, Triterpenes, Bioavailability, Rats, Liver, combination index, Piperine, Chemical and Drug Induced Liver Injury, pharmacokinetics, Research Article

Abstract

Background Ursolic acid (UA) is a potent plant-based hepatoprotective agent having poor bioavailability, which hampers its therapeutic efficacy. The present study tries to overcome this limitation by combining it with piperine (PIP), a proven bioenhancer and hepatoprotective agent. Methods The type of interaction (synergism, addition, or antagonism) resulting between UA and PIP was analyzed and quantified by isobologram and combination index analysis. The hepatoprotective activity of UA and PIP was evaluated by measuring the level of hepatic marker enzymes. Pharmacokinetic analysis was carried out to ascertain the improvement of bioavailability. Results The combinations significantly decrease the enzyme levels, which indicate better hepatoprotective activity compared to single drugs. The relative oral bioavailability of UA was increased about tenfold (from AUC0–t =12.78 ± 2.59 µg/h/ml to 125.15 ± 1.84 µg/h/ml) along with the improvement of plasma concentration and elimination half-life. Conclusions The findings indicated that the combination of PIP and UA is an effective strategy in enhancing the bioavailability and hepatoprotective potential of UA.KEY MESSAGESUrsolic acid in a combination with piperine provides a synergistic hepatoprotective effect in carbon tetrachloride induced liver damage in rats.Piperine improves the pharmacokinetic properties of ursolic acid when given in combination.Piperine improves the relative oral bioavailability of ursolic acid by tenfold when combined together.

Published

2021

4. Antinociceptive Synergism of Pomegranate Peel Extract and Acetylsalicylic Acid in an Animal Pain Model

Author

Luis Guillermo González-Olivares, José Antonio Guerrero-Solano, Minarda De la O-Arciniega, Claudia Velázquez-González, Mirandeli Bautista, Osmar Antonio Jaramillo-Morales, and Monserrat Fernández-Moya

Subjects

Drug, Formalin Test, media_common.quotation_subject, Pharmaceutical Science, Organic chemistry, Pharmacology, Article, Pomegranate, Analytical Chemistry, isobologram, Nociceptive Pain, pomegranate peel, Pharmacotherapy, QD241-441, formalin test, synergism, Drug Discovery, Animals, pain, Physical and Theoretical Chemistry, Rats, Wistar, Punica granatum L, media_common, Pain Measurement, combination, Analgesics, Aspirin, Chemistry, Drug Synergism, acetylsalicylic acid, Inflammatory pain, Effective dose (pharmacology), antinociceptive, Rats, Antioxidant capacity, Disease Models, Animal, Nociception, Chemistry (miscellaneous), Molecular Medicine, Phytotherapy

Abstract

Several modern drugs, which are derived from traditional herbal medicine are used in contemporary pharmacotherapy. Currently, the study of drug–plant interactions in pain has increased in recent years, looking for greater efficacy of the drug and reduce side effects. The antinociception induced by intragastric co-administration of the combination of pomegranate peel extract (PoPEx) and acetylsalicylic acid (ASA) was assessed using the isobolographic analysis in formalin test (nociceptive and inflammatory pain). The effective dose that produced 30% of antinociception (ED30) was calculated for both drugs from the logarithmic dose–response curves, subsequently generating a curve with the combination on fixed proportions (1:1) of PoPEx and ASA. Through isobolographic analysis, this experimental ED30 was compared with the calculated theoretical additive ED30. The result was a synergistic interaction, the experimental ED30 was significantly smaller (p &lt, 0.05) than the theoretical ED30. The antinociceptive mechanism of the PoPEx-ASA combination involves the l-Arginine/NO/cGMP pathway, antioxidant capacity, and high content of total phenols. These findings suggest that an interaction between PoPEx and ASA could be a novel treatment for inflammatory and nociceptive pain, also diminish the secondary reactions of ASA.

Published

2021

5. Evaluation of the Antinociceptive, Antiallodynic, Antihyperalgesic and Anti-Inflammatory Effect of Polyalthic Acid

Author

Héctor I. Rocha-González, Yaraset López-Lorenzo, Geovanna Nallely Quiñonez-Bastidas, Juan Gerardo Reyes-García, María Elena Sánchez-Mendoza, Jesús Arrieta, Francisco J. Flores-Murrieta, and Juan Rodríguez-Silverio

Subjects

Naproxen, Time Factors, medicine.drug_class, Anti-Inflammatory Agents, Pharmaceutical Science, Administration, Oral, polyalthic acid, Pharmacology, Anti-inflammatory, Naltrexone, Article, Analytical Chemistry, isobologram, 03 medical and health sciences, chemistry.chemical_compound, QD241-441, 0302 clinical medicine, synergism, Drug Discovery, antiallodynic effect, medicine, Animals, naproxen, Physical and Theoretical Chemistry, Rats, Wistar, Ligation, antinociception, 030304 developmental biology, 0303 health sciences, Analgesics, Dose-Response Relationship, Drug, Organic Chemistry, Drug Synergism, Carrageenan, Allodynia, Nociception, Spinal Nerves, Opioid, chemistry, Chemistry (miscellaneous), Hyperalgesia, Molecular Medicine, Female, medicine.symptom, Diterpenes, 030217 neurology & neurosurgery, medicine.drug

Abstract

Nonsteroidal anti-inflammatory drugs (NSAIDs) are very commonly used, but their adverse effects warrant investigating new therapeutic alternatives. Polyalthic acid, a labdane-type diterpenoid, is known to produce gastroprotection, tracheal smooth muscle relaxation, and antitumoral, antiparasitic and antibacterial activity. This study aimed to evaluate the antinociceptive, antiallodynic, antihyperalgesic and anti-inflammatory effect of polyalthic acid on rats. Moreover, the effectiveness of treating hyperalgesia with a combination of polyalthic acid and naproxen was analyzed, as well as the type of drug–drug interaction involved. Nociception was examined by injecting 1% formalin into the right hind paw and thermal hyperalgesia and inflammation by injecting a 1% carrageenan solution into the left hind paw of rats. Allodynia was assessed on an L5/L6 spinal nerve ligation model. Polyalthic acid generated significant antinociceptive (56–320 mg/kg), antiallodynic (100–562 mg/kg), and antihyperalgesic and anti-inflammatory (10–178 mg/kg) effects. Antinociception mechanisms were explored by pretreating the rats with naltrexone, ODQ and methiothepin, finding the effect blocked by the former two compounds, which indicates the participation of opioid receptors and guanylate cyclase. An isobolographic analysis suggests synergism between polyalthic acid and naproxen in the combined treatment of hyperalgesia.

Published

2021

6. Subcutaneous l-tyrosine elicits cutaneous analgesia in response to local skin pinprick in rats.

Author

Hung, Ching-Hsia, Chiu, Chong-Chi, Liu, Kuo-Sheng, Chen, Yu-Wen, and Wang, Jhi-Joung

Subjects

*TYROSINE, *DRUG therapy, *CLINICAL trials, *PATHOLOGY, *PHARMACOLOGY

Abstract

The purpose of the study was to estimate the ability of l -tyrosine to induce cutaneous analgesia and to investigate the interaction between l -tyrosine and the local anesthetic lidocaine. After subcutaneously injecting the rats with l -tyrosine and lidocaine in a dose-dependent manner, cutaneous analgesia (by blocking the cutaneous trunci muscle reflex-CTMR) was evaluated in response to the local pinprick. The drug–drug interaction was analyzed by using an isobolographic method. We showed that both l -tyrosine and lidocaine produced dose-dependent cutaneous analgesia. On the 50% effective dose (ED 50 ) basis, the rank of drug potency was lidocaine (5.09 [4.88–5.38] μmol)> l -tyrosine (39.1 [36.5–41.8] μmol) ( P <0.05). At the equipotent doses (ED 25 , ED 50 , and ED 75 ), the duration of cutaneous analgesia caused by l -tyrosine lasted longer than that caused by lidocaine ( P <0.01). Lidocaine co-administered with l -tyrosine exhibited an additive effect on infiltrative cutaneous analgesia. Our pre-clinical study demonstrated that l -tyrosine elicits the local/cutaneous analgesia, and the interaction between l -tyrosine and lidocaine is additive. l -tyrosine has a lower potency but much greater duration of cutaneous analgesia than lidocaine. Adding l -tyrosine to lidocaine preparations showed greater duration of cutaneous analgesia compared with lidocaine alone. [ABSTRACT FROM AUTHOR]

Published

2015

7. Vernonia brasiliana (L.) Druce induces ultrastructural changes and apoptosis-like death of Leishmania infantum promastigotes

Author

Carla Junqueira Moragas-Tellis, Kátia da Silva Calabrese, Ana Lúcia Abreu-Silva, Thaize Quiroga Chometon, Paulo Victor Ramos de Souza, Álvaro Luiz Bertho, Renata Mondêgo-Oliveira, Noemi Nosomi Taniwaki, Joicy Cortez de Sá Sousa, Daiana de Jesus Hardoim, Maria Dutra Behrens, Fernando Almeida-Souza, and Maria do Socorro dos Santos Chagas

Subjects

0301 basic medicine, Programmed cell death, Phosphorylcholine, Antiprotozoal Agents, Apoptosis, RM1-950, DH82 cells, Cell Line, law.invention, 03 medical and health sciences, Dogs, 0302 clinical medicine, law, Isobologram, Oils, Volatile, medicine, Animals, Plant Oils, Drug Interactions, Flow cytometry, Leishmania infantum, Fragmentation (cell biology), Leishmaniasis, Essential oil, Membrane Potential, Mitochondrial, Polycyclic Sesquiterpenes, Pharmacology, chemistry.chemical_classification, Reactive oxygen species, Miltefosine, biology, Chemistry, General Medicine, biology.organism_classification, Molecular biology, Mitochondria, 030104 developmental biology, 030220 oncology & carcinogenesis, Kinetoplast, β-caryophyllene, Therapeutics. Pharmacology, Reactive Oxygen Species, Vernonia, Transmission electron microscopy, medicine.drug

Abstract

The present study aimed to evaluate the antileishmanial effect, the mechanisms of action and the association with miltefosine of Vernonia brasiliana essential oil against Leishmania infantum promastigotes. This essential oil was obtained by hydrodistillation and its chemical composition was determined by gas chromatography-mass spectrometry (GC–MS). The antileishmanial activity against L. infantum promastigotes and cytotoxicity on DH82 cells were evaluated by MTT colorimetric assay. Ultrastructural alterations were evaluated by transmission electron microscopy. Changes in mitochondrial membrane potential, in the production of reactive oxygen species, and analysis of apoptotic events were determined by flow cytometry. The association between the essential oil and miltefosine was evaluated using the modified isobologram method. The most abundant component of the essential oil was β-caryophyllene (21.47 %). Anti-Leishmania assays indicated an IC50 of 39.01 ± 1.080 μg/mL for promastigote forms after 72 h of treatment. The cytotoxic concentration for DH82 cells was 63.13 ± 1.211 μg/mL after 24 h of treatment. The effect against L. infantum was proven through the ultrastructural changes caused by the oil, such as kinetoplast and mitochondrial swelling, vesicles in the flagellar pocket, discontinuity of the nuclear membrane, nuclear fragmentation and condensation, and loss of organelles. It was observed that the oil leads to a decrease in the mitochondrial membrane potential (35.10 %, p = 0.0031), increased reactive oxygen species production, and cell death by late apoptosis (17.60 %, p = 0.020). The combination of the essential oil and miltefosine exhibited an antagonistic effect. This study evidences the antileishmanial action of V. brasiliana essential oil against L. infantum promastigotes.

Published

2021

8. Positive Allosteric Modulation of CB1 Cannabinoid Receptor Signaling Enhances Morphine Antinociception and Attenuates Morphine Tolerance Without Enhancing Morphine- Induced Dependence or Reward

Author

Richard A. Slivicki, Vishakh Iyer, Sonali S. Mali, Sumanta Garai, Ganesh A. Thakur, Jonathon D. Crystal, and Andrea G. Hohmann

Subjects

0301 basic medicine, medicine.drug_class, Physical dependence, (+)-Naloxone, Pharmacology, lcsh:RC321-571, isobologram, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, Opioid receptor, Medicine, lcsh:Neurosciences. Biological psychiatry. Neuropsychiatry, Molecular Biology, Original Research, neuropathic pain, business.industry, withdrawal, Chronic pain, allosteric modulator, endocannabinoid, medicine.disease, Conditioned place preference, 030104 developmental biology, Opioid, Neuropathic pain, Morphine, opioid, medicine.symptom, business, 030217 neurology & neurosurgery, medicine.drug, Neuroscience

Abstract

Opioid analgesics represent a critical treatment for chronic pain in the analgesic ladder of the World Health Organization. However, their use can result in a number of unwanted side-effects including incomplete efficacy, constipation, physical dependence, and overdose liability. Cannabinoids enhance the pain-relieving effects of opioids in preclinical studies and dampen unwanted side-effects resulting from excessive opioid intake. We recently reported that a CB1 positive allosteric modulator (PAM) exhibits antinociceptive efficacy in models of pathological pain and lacks the adverse side effects of direct CB1 receptor activation. In the present study, we evaluated whether a CB1 PAM would enhance morphine’s therapeutic efficacy in an animal model of chemotherapy-induced neuropathic pain and characterized its impact on unwanted side-effects associated with chronic opioid administration. In paclitaxel-treated mice, both the CB1 PAM GAT211 and the opioid analgesic morphine reduced paclitaxel-induced behavioral hypersensitivities to mechanical and cold stimulation in a dose-dependent manner. Isobolographic analysis revealed that combinations of GAT211 and morphine resulted in anti-allodynic synergism. In paclitaxel-treated mice, a sub-threshold dose of GAT211 prevented the development of tolerance to the anti-allodynic effects of morphine over 20 days of once daily dosing. However, GAT211 did not reliably alter somatic withdrawal signs (i.e., jumps, paw tremors) in morphine-dependent neuropathic mice challenged with naloxone. In otherwise naïve mice, GAT211 also prolonged antinociceptive efficacy of morphine in the tail-flick test and reduced the overall right-ward shift in the ED50 for morphine to produce antinociception in the tail-flick test, consistent with attenuation of morphine tolerance. Pretreatment with GAT211 did not alter somatic signs of μ opioid receptor dependence in mice rendered dependent upon morphine via subcutaneous implantation of a morphine pellet. Moreover, GAT211 did not reliably alter μ-opioid receptor-mediated reward as measured by conditioned place preference to morphine. Our results suggest that a CB1 PAM may be beneficial in enhancing and prolonging the therapeutic properties of opioids while potentially sparing unwanted side-effects (e.g., tolerance) that occur with repeated opioid treatment.

Published

2020

9. Preclinical Antimalarial Combination Study of M5717, a Plasmodium falciparum Elongation Factor 2 Inhibitor, and Pyronaridine, a Hemozoin Formation Inhibitor

Author

Thomas Spangenberg, Matthias Rottmann, Beatrice Greco, Xiaoyan Yin, Satish K. Dhingra, Christin Gumpp, Claude Oeuvray, Lassina Badolo, Brian Jonat, David A. Fidock, and Marla J. Giddins

Subjects

Hemeproteins, Drug, media_common.quotation_subject, Plasmodium falciparum, Drug Resistance, drug combination, malaria, Mice, SCID, Drug resistance, Biology, Pharmacology, isobologram, Antimalarials, Mice, 03 medical and health sciences, Peptide Elongation Factor 2, Pharmacokinetics, In vivo, parasitic diseases, Animals, SCID mouse, Experimental Therapeutics, Pharmacology (medical), Malaria, Falciparum, Naphthyridines, 030304 developmental biology, media_common, Pyronaridine, 0303 health sciences, 030306 microbiology, Hemozoin, M5717, biology.organism_classification, Infectious Diseases, Drug development, pyronaridine, Quinolines, Drug Therapy, Combination, resistant mutant

Abstract

Antimalarial drug resistance in the Plasmodium falciparum parasite poses a constant challenge for drug development. To mitigate this risk, new antimalarial medicines should be developed as fixed-dose combinations. Assessing the pharmacodynamic interactions of potential antimalarial drug combination partners during early phases of development is essential in developing the targeted parasitological and clinical profile of the final drug product. Here, we have studied the combination of M5717, a P. falciparum translation elongation factor 2 inhibitor, and pyronaridine, an inhibitor of hemozoin formation., Antimalarial drug resistance in the Plasmodium falciparum parasite poses a constant challenge for drug development. To mitigate this risk, new antimalarial medicines should be developed as fixed-dose combinations. Assessing the pharmacodynamic interactions of potential antimalarial drug combination partners during early phases of development is essential in developing the targeted parasitological and clinical profile of the final drug product. Here, we have studied the combination of M5717, a P. falciparum translation elongation factor 2 inhibitor, and pyronaridine, an inhibitor of hemozoin formation. Our test cascade consisted of in vitro isobolograms as well as in vivo studies in the P. falciparum severe combined immunodeficient (SCID) mouse model. We also analyzed pharmacokinetic and pharmacodynamic parameters, including genomic sequencing of recrudescent parasites. We observed no pharmacokinetic interactions with the combination of M5717 and pyronaridine. M5717 did not negatively impact the rate of kill of the faster-acting pyronaridine, and the latter was able to suppress the selection of M5717-resistant mutants, as well as significantly delay the recrudescence of parasites both with suboptimal and optimal dosing regimens.

Published

2020

10. Flavonoid combinations cause synergistic inhibition of proinflammatory mediator secretion from lipopolysaccharide-induced RAW 264.7 cells.

Author

Harasstani, Omar, Moin, Saidi, Tham, Chau, Liew, Choi, Ismail, Norazren, Rajajendram, Revathee, Harith, Hanis, Zakaria, Zainul, Mohamad, Azam, Sulaiman, Mohamad, and Israf, Daud

Subjects

*FLAVONOIDS, *INFLAMMATORY mediators, *NITRIC oxide, *PROSTAGLANDINS, *TUMOR necrosis factors, *ANTI-inflammatory agents, *PHARMACOLOGY, *DRUG synergism

Abstract

We evaluated several flavonoid combinations for synergy in the inhibition of proinflammatory mediator synthesis in the RAW 264.7 cellular model of inflammation. The inhibitory effect of chrysin, kaempferol, morin, silibinin, quercetin, diosmin and hesperidin upon nitric oxide (NO), prostaglandin E2 (PGE2) and tumour necrosis factor-α (TNF-α) secretion from the LPS-induced RAW 264.7 monocytic macrophage was assessed and IC50 values obtained. Flavonoids that showed reasonable inhibitory effects in at least two out of the three assays were combined in a series of fixed IC50 ratios and reassessed for inhibition of NO, PGE2 and TNF-α. Dose–response curves were generated and interactions were analysed using isobolographic analysis. The experiments showed that only chrysin, kaempferol, morin, and silibinin were potent enough to produce dose–response effects upon at least two out of the three mediators assayed. Combinations of these four flavonoids showed that several combinations afforded highly significant synergistic effects. Some flavonoids are synergistic in their anti-inflammatory effects when combined. In particular chrysin and kaempferol significantly synergised in their inhibitory effect upon NO, PGE2 and TNF-α secretion. These findings open further avenues of research into combinatorial therapeutics of inflammatory-related diseases and the pharmacology of flavonoid synergy. [ABSTRACT FROM AUTHOR]

Published

2010

11. Interactions between tafenoquine and artemisinin-combination therapy partner drug in asexual and sexual stage Plasmodium falciparum

Author

Liwang Cui, Mynthia Cabrera, and Karen Kemirembe

Subjects

0301 basic medicine, Primaquine, Tafenoquine, Drug interaction, Plasmodium falciparum, 030106 microbiology, Gametocyte, Pharmacology, lcsh:Infectious and parasitic diseases, Antimalarials, 03 medical and health sciences, chemistry.chemical_compound, Chloroquine, Isobologram, Piperaquine, parasitic diseases, medicine, lcsh:RC109-216, Pharmacology (medical), Artemisinin, Pyronaridine, biology, Drug Synergism, biology.organism_classification, ACT, 8-Aminoquinoline, Artemisinins, Malaria, 3. Good health, Infectious Diseases, chemistry, Invited Article, Aminoquinolines, Parasitology, medicine.drug

Abstract

The 8-aminoquinoline tafenoquine (TFQ), a primaquine derivative, is currently in late-stage clinical development for the radical cure of P. vivax. Here drug interactions between TFQ and chloroquine and six artemisinin-combination therapy (ACT) partner drugs in P. falciparum asexual stages and gametocytes were investigated. TFQ was mostly synergistic with the ACT-partner drugs in asexual parasites regardless of genetic backgrounds. However, at fixed ratios of 1:3, 1:1 and 3:1, TFQ only interacted synergistically with naphthoquine, pyronaridine and piperaquine in gametocytes. This study indicated that TFQ and ACT-partner drugs will likely have increased potency against asexual stages of the malaria parasites, whereas some drugs may interfere with each other against the P. falciparum gametocytes., Graphical abstract Image 1, Highlights • Interactions of tafenoquine with other antimalarials are studied in P. falciparum. • Synergistic interactions occur with most drugs in asexual erythrocytic stages. • Tafenoquine will likely increase the potency of other drugs against asexual stages. • Synergism is found with naphthoquine, pyronaridine and piperaquine in gametocytes. • Tafenoquine may interfere with other drugs against P. falciparum gametocytes.

Published

2017

12. Synergistic antifungal activity of the lipophilic fraction of Hypericum carinatum and fluconazole

Author

Bruna Pippi, Gilsane Lino von Poser, Camila Hatwig, Alexandre Meneghello Fuentefria, Luís Flávio Souza de Oliveira, Gabriela de Carvalho Meirelles, and Francisco Maikon Corrêa de Barros

Subjects

0301 basic medicine, Checkerboard, 030106 microbiology, Phloroglucinol, lcsh:RS1-441, Pharmacology, Hypericaceae, Microbiology, lcsh:Pharmacy and materia medica, 03 medical and health sciences, chemistry.chemical_compound, Pharmacology, Toxicology and Pharmaceutics(all), Candida krusei, Hypericum carinatum, Isobologram, medicine, General Pharmacology, Toxicology and Pharmaceutics, Fluconazole, Candida, Cryptococcus neoformans, biology, Farmácia, Synergistic activity, biology.organism_classification, Antimicrobial, Yeast, 030104 developmental biology, chemistry, Hypericum, medicine.drug

Abstract

Hypericum species, Hypericaceae, are recognized as a source of therapeutical agents. Purified fractions and isolated compounds have been shown antimicrobial activity. As the indiscriminate use of antifungals and the increase of infections caused by emerging species are leading to the search of new alternative treatments, the aim of this study was to continue the study with Hypericum carinatum Griseb. lipophilic fraction, rich in phloroglucinol derivatives, investigating the effect of its association with fluconazole against emerging yeasts (Candida krusei, C. famata, C. parapsilosis and Cryptococcus neoformans). The synergistic activity between H. carinatum lipophilic fraction and fluconazole was assessed by two methodologies for multiple dose–response analysis: checkerboard and isobologram. Regarding synergistic experiments, the effect of the association was higher than the effect of fluconazole alone against Candida krusei and C. famata isolates (MIC fluconazole decreased about eight and four folds, respectively), suggesting that, somehow, H. carinatum lipophilic fraction compounds are facilitating the action of this drug. On the other hand, when tested against Cryptococcus neoformans and C. parapsilosis, fluconazole showed better results than the association. Thus, against Candida krusei and C. famata, the lipophilic fraction of H. carinatum was able to reduce the MIC values of fluconazole and could be considered as a potential alternative to be used against emerging yeast species. Keywords: Candida, Checkerboard, Fluconazole, Hypericum carinatum, Isobologram, Synergistic activity

Published

2017

13. Investigating interactions between phentermine, dexfenfluramine, and 5-HT2C agonists, on food intake in the rat

Author

Dominic P. Behan, Kevin Whelan, Michael Morgan, Erin K. Sanabria, Andrew J. Grottick, and Carleton R. Sage

Subjects

Male, Agonist, Phentermine, Food intake, medicine.medical_specialty, Fenfluramine, medicine.drug_class, Pharmacology, Lorcaserin, Rats, Sprague-Dawley, Eating, Dexfenfluramine, Isobologram, Internal medicine, Appetite Depressants, Hypophagia, Receptor, Serotonin, 5-HT2C, Animals, Medicine, Original Investigation, business.industry, Drug Synergism, Rats, Synergy, BELVIQ®, Endocrinology, Fen-phen, Serotonin, business, Serotonin 5-HT2 Receptor Agonists, medicine.drug

Abstract

Rationale Synergistic or supra-additive interactions between the anorectics (dex)fenfluramine and phentermine have been reported previously in the rat and in the clinic. Studies with 5-HT2C antagonists and 5-HT2C knockouts have demonstrated dexfenfluramine hypophagia in the rodent to be mediated by actions at the 5-HT2C receptor. Given the recent FDA approval of the selective 5-HT2C agonist lorcaserin (BELVIQ®) for weight management, we investigated the interaction between phentermine and 5-HT2C agonists on food intake. Objectives This study aims to confirm dexfenfluramine-phentermine (dex-phen) synergy in a rat food intake assay, to extend these findings to other 5-HT2C agonists, and to determine whether pharmacokinetic interactions could explain synergistic findings with particular drug combinations. Methods Isobolographic analyses were performed in which phentermine was paired with either dexfenfluramine, the 5-HT2C agonist AR630, or the 5-HT2C agonist lorcaserin, and inhibition of food intake measured in the rat. Subsequent studies assessed these same phentermine-drug pair combinations spanning both the full effect range and a range of fixed ratio drug combinations. Satellite groups received single doses of each drug either alone or in combination with phentermine, and free brain concentrations were measured. Results Dex-phen synergy was confirmed in the rat and extended to the 5-HT2C agonist AR630. In contrast, although some synergistic interactions between lorcaserin and phentermine were observed, these combinations were largely additive. Synergistic interactions between phentermine and dexfenfluramine or AR630 were accompanied by combination-induced increases in brain levels of phentermine. Conclusions Dex-phen synergy in the rat is caused by a pharmacokinetic interaction, resulting in increased central concentrations of phentermine.

Published

2014

14. Analyses of the combination of 6-MP and dasatinib in cell culture

Author

Holger Behrsing, Beverly A. Teicher, Ralph E. Parchment, Myrtle Davis Millin, and Gurmeet Kaur

Subjects

Cancer Research, Cell, Dasatinib, In Vitro Techniques, Biology, Pharmacology, isobologram, Breast cancer, Neoplasms, Antineoplastic Combined Chemotherapy Protocols, medicine, Humans, 6-mercaptopurine, Tumor Stem Cell Assay, response surface, Mercaptopurine, Cancer, Drug Synergism, Articles, Cell cycle, medicine.disease, Thiazoles, Pyrimidines, medicine.anatomical_structure, Oncology, combination index, Toxicity, MCF-7 Cells, Cancer research, Bone marrow, medicine.drug

Abstract

A major tenet of cancer therapeutics is that combinations of anticancer agents with different mechanisms of action and different toxicities may be effective treatment regimens. Evaluation of additivity/synergy in cell culture may be used to identify drug combination opportunities and to assess risk of additive/synergistic toxicity. The combination of 6-mercaptopurine and dasatinib was assessed for additivity/synergy using the combination index (CI) method and a response surface method in six human tumor cell lines including MCF-7 and MDA-MB‑468 breast cancer, NCI-H23 and NCI-H460 non‑small cell lung cancer, and A498 and 786-O renal cell cancer, based on two experimental end‑points: ATP content and colony formation. Clonal colony formation by human bone marrow CFU-GM was used to assess risk of enhanced toxicity. The concentration ranges tested for each drug were selected to encompass the clinical Cmax concentrations. The combination regimens were found to be additive to sub‑additive by both methods of data analysis, but synergy was not detected. The non-small cell lung cancer cell lines were the most responsive among the tumor lines tested and the renal cell carcinoma lines were the least responsive. The bone marrows CFU-GM were more sensitive to the combination regimens than were the tumor cell lines. Based upon these data, it appears that the possibility of enhanced efficacy from combining 6-mercaptopurine (6-MP) and dasatinib would be associated with increased risk of severe bone marrow toxicity, so the combination is unlikely to provide a therapeutic advantage for treating solid tumor patients where adequate bone marrow function must be preserved.

Published

2013

15. Synergistic effects of Chinese herbal medicine: a comprehensive review of methodology and current research

Author

Hosen Kiat, Valentina Razmovski-Naumovski, Xian Zhou, Sai Wang Seto, Kelvin Chan, Alan Bensoussan, and Dennis Hsu-Tung Chang

Subjects

0301 basic medicine, RM, medicine.medical_specialty, Interaction, Alternative medicine, Primary health care, Combination index, Context (language use), Review, Traditional Chinese medicine, complex mixtures, 03 medical and health sciences, 0302 clinical medicine, RZ, Isobologram, Asian country, medicine, Pharmacology (medical), Pharmacology, Traditional medicine, business.industry, Management science, system biology, lcsh:RM1-950, Evidence-based medicine, Synergy, 030104 developmental biology, lcsh:Therapeutics. Pharmacology, 030220 oncology & carcinogenesis, Medicinal herbs, Chinese herbal medicine, business

Abstract

© 2016 Zhou, Seto, Chang, Kiat, Razmovski-Naumovski, Chan and Bensoussan. Traditional Chinese medicine (TCM) is an important part of primary health care in Asian countries that has utilized complex herbal formulations (consisting 2 or more medicinal herbs) for treating diseases over thousands of years. There seems to be a general assumption that the synergistic therapeutic effects of Chinese herbal medicine (CHM) derive from the complex interactions between the multiple bioactive components within the herbs and/or herbal formulations. However, evidence to support these synergistic effects remains weak and controversial due to several reasons, including the very complex nature of CHM, misconceptions about synergy and methodological challenges to study design. In this review, we clarify the definition of synergy, identify common errors in synergy research and describe current methodological approaches to test for synergistic interaction. We discuss the strengths and weaknesses of these models in the context of CHM and summarize the current status of synergy research in CHM. Despite the availability of some scientific data to support the synergistic effects of multi-herbal and/or herb-drug combinations, the level of evidence remains low, and the clinical relevancy of most of these findings is undetermined. There remain significant challenges in the development of suitable methods for synergistic studies of complex herbal combinations.

Published

2016

16. An isobolographic analysis of the antinociceptive effect of xylopic acid in combination with morphine or diclofenac

Author

Wonder Kofi Mensah Abotsi, Elvis Ofori Ameyaw, Eric Woode, and Eric Boakye-Gyasi

Subjects

Xylopia aethiopica, Formalin Test, mice, potentiation, biology, business.industry, Analgesic, Pharmacology, biology.organism_classification, stomatognathic diseases, Diclofenac, Nociception, Isobologram, synergism, Morphine, Medicine, Original Article, nociception, business, Patient compliance, Adverse effect, medicine.drug

Abstract

Background: A common practice of managing pain globally is the combination of analgesics and this is aimed at facilitating patient compliance, simplifying prescription, and improving efficacy without increasing adverse effects. Fruit extracts of Xylopia aethiopica are used traditionally in the management of pain disorders and xylopic acid (XA) present in the fruit extract have been shown to possess analgesic properties in animals. There is the likelihood of concomitant use of XA and the commonly used analgesics in traditional settings. This study, therefore, evaluated the pharmacologic interaction between XA/morphine and xylopic/diclofenac combinations. Methods: The formalin test and acetic acid writhing test were used to study the antinociceptive activity of XA, morphine, and diclofenac. The isobolographic analysis was used to study the antinociceptive interactions between XA co-administered with morphine or diclofenac. Results: Results obtained revealed that XA (10–100 mg/kg), morphine (1–10 mg/kg), and diclofenac (1–10 mg/kg) produced dose-related antinociception with different potencies in the formalin and acetic acid writhing tests. Isobolographic analysis of XA/morphine and XA/diclofenac combinations revealed potentiation of their antinociceptive effects. The degree of potentiation calculated as interaction index showed synergism for both combinations in all the nociceptive tests. Conclusion: In conclusion, the present study demonstrated synergism for the co-administration of XA with morphine or diclofenac.

Published

2015

17. Anti-plasmodial and chloroquine resistance suppressive effects of embelin

Author

O I Zaid, M S Hasidah, Khalid Jameel Kadhim Al-Zihiry, Rusliza Basir, Sattar Rahi, M N Sabariah, and R Abd Majid

Subjects

0301 basic medicine, Embelia ribes, DPPH, Plasmodium falciparum, 030231 tropical medicine, Serum albumin, Pharmaceutical Science, Pharmacology, isobologram, resistance, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Chloroquine, Drug Discovery, medicine, embelin, biology, Chemistry, Hemozoin, biology.organism_classification, In vitro, 030104 developmental biology, Mechanism of action, SYBR-green-I, biology.protein, Original Article, medicine.symptom, medicine.drug

Abstract

Background: Emergence of chloroquine (CQ) resistance among different strains of Plasmodium falciparum is the worst catastrophe that has ever perplexed the dedicated efforts to eradicate malaria. This urged the scientists to search for new alternatives or sensitizers to augment its antiplasmodium effect. Materials and Method: In this experiment, the potential of embelin, isolated from Embelia ribes, to inhibit the growth and sensitize CQ action was screened using SYBRE-green-I based drug sensitivity and isobologram assays, respectively. Its effect on red blood cells stability was screened to assess its safety. To explore its molecular mechanism, its effect on plasmodial Hemozoin and the in vitro β-hematin formation was screened as well. Furthermore, its anti-oxidant activity was measured using the conventional in vitro tests and its molecular characters were obtained using Molispiration program. Results: The results showed that its anti-plasmodial effect was weaker than CQ but synergism was obtained when they were combined at ratios lower than 5:5 CQ/embelin. Furthermore, β-hematin formation was inhibited by embelin without showing any synergism after mixing with CQ. Conclusion: Overall, embelin is not ideal to be suggested as a conventional antiplasmodium but it has a potential to ameliorate CQ resistance. Furthermore, its action is not related to its impact on hemozoin formation. Further, investigations are recommended to illustrate its detailed mechanism of action. Abbreviation used: CQ-DV-PBS-HEPES: Chloroquine-Digestive vacuole-Phosphate-buffer-saline-4-(2-hydroxyethyl-1-piperazin-ethan-sulphoni-acid), EDTA: Ethylen-diamin-tetra-acetic-acid, g.m.wt: Gram molecular weight, cMCM: Complete-malaria-culture-medium, Hct: Hematocrite, PRBCs: Parasitized-redblood-cells, nRBCs: Normal-red-blood-cells, RT: Room temperature, IC: Inhibitory concentration, FIC: Fractional inhibitory concentration, iCM: Incomplete-culturemedium, BSA: Bovin serum albumin, MTT: 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide, DPPH: 2,2-diphenyl-1- picrylhydrazy, BHT: Butylatedhydroxyl-toleuen, PSA: Polar surface area, ClogP: Log partition coefficient (octanol/water), GPCR: G-protein-coupled-receptors, DMSO: Dimethylsulphoxide, NaOH: Sodium hydroxide

Published

2017

18. Enantiomerically pure amino-alcohol quinolines: in vitro anti-malarial activity in combination with dihydroartemisinin, cytotoxicity and in vivo efficacy in a Plasmodium berghei mouse model

Author

Catherine Mullié, Alexia Jonet, Camille Degrouas, Patrice Agnamey, Nicolas Taudon, Pascal Sonnet, Aurélie Pascual, Laboratoire de Glycochimie, des Antimicrobiens et des Agro-ressources - UMR CNRS 7378 (LG2A ), Université de Picardie Jules Verne (UPJV)-Institut de Chimie du CNRS (INC)-Centre National de la Recherche Scientifique (CNRS), Infections Parasitaires : Transmission, Physiopathologie et Thérapeutiques (IP-TPT), Service de Santé des Armées-Assistance Publique - Hôpitaux de Marseille (APHM)-Aix Marseille Université (AMU)-Institut de Recherche pour le Développement (IRD), Unité de Recherche sur les Maladies Infectieuses et Tropicales Emergentes (URMITE), Institut de Recherche pour le Développement (IRD)-Aix Marseille Université (AMU)-Institut National de la Santé et de la Recherche Médicale (INSERM)-IFR48, INSB-INSB-Centre National de la Recherche Scientifique (CNRS), Laboratoire de parasitologie et de mycologie médicales [CHU Amiens], CHU Amiens-Picardie, Institut de Recherche pour le Développement (IRD)-Aix Marseille Université (AMU)-Assistance Publique - Hôpitaux de Marseille (APHM)-Service de Santé des Armées, Institut des sciences biologiques (INSB-CNRS)-Institut des sciences biologiques (INSB-CNRS)-Centre National de la Recherche Scientifique (CNRS), Agents infectieux, résistance et chimiothérapie - UR UPJV 4294 (AGIR ), Université de Picardie Jules Verne (UPJV)-CHU Amiens-Picardie, and HAL AMU, Administrateur

Subjects

Erythrocytes, Plasmodium berghei, [SDV]Life Sciences [q-bio], medicine.medical_treatment, Quinoline, Pharmacology, 0302 clinical medicine, Parasitic Sensitivity Tests, Isobologram, Artemisinin, ComputingMilieux_MISCELLANEOUS, Mice, Inbred BALB C, 0303 health sciences, [SDV.MHEP] Life Sciences [q-bio]/Human health and pathology, Enantiomer, biology, Anti-malarial activity, Drug Synergism, Haemolysis, Artemisinins, 3. Good health, in vivo, Treatment Outcome, Dihydroartemisinin, Infectious Diseases, Combination, Quinolines, Drug Therapy, Combination, Female, medicine.drug, Combination therapy, Plasmodium falciparum, 030231 tropical medicine, Hemolysis, Antimalarials, Inhibitory Concentration 50, 03 medical and health sciences, In vivo, parasitic diseases, medicine, Animals, 030306 microbiology, Research, biology.organism_classification, Survival Analysis, In vitro, Malaria, Disease Models, Animal, Parasitology, [SDV.MHEP]Life Sciences [q-bio]/Human health and pathology

Abstract

International audience; Background: As resistance to marketed anti-malarial drugs continues to spread, the need for new molecules active on Plasmodium falciparum-resistant strains grows. Pure (S) enantiomers of amino-alcohol quinolines previously displayed a good in vitro anti-malarial activity. Therefore, a more thorough assessment of their potential clinical use through a rodent model and an in vitro evaluation of their combination with artemisinin was undertaken. Methods: Screening on a panel of P. falciparum clones with varying resistance profiles and regional origins was performed for the (S)-pentyl and (S)-heptyl substituted quinoline derivatives, followed by an in vitro assessment of their combination with dihydroartemisinin (DHA) on the 3D7 clone and an in vivo assay in a mouse model infected with Plasmodium berghei. Their haemolytic activity was also determined. Results: A steady anti-malarial activity of the compounds tested was found, whatever the resistance profile or the regional origin of the strain. (S)-quinoline derivatives were at least three times more potent than mefloquine (MQ), their structurally close parent. The in vitro combination with DHA yielded an additive or synergic effect for both that was as good as that of the DHA/MQ combination. In vivo, survival rates were similar to those of MQ for the two compounds at a lower dose, despite a lack of clearance of the parasite blood stages. A 50% haemolysis was observed for concentrations at least 1,000-fold higher than the antiplasmodial IC 50 s. Conclusions: The results obtained make those two (S)-amino-alcohol quinoline derivatives good candidates for the development of new artemisinin-based combination therapy (ACT), hopefully with fewer neurologic side effects than those currently marketed ACT, including MQ.

Published

2014

19. Schedule-dependent Synergism and Antagonism between Raltitrexed ('Tomudex') and Methotrexate in Human Colon Cancer Cell Linesin vitro

Author

Saburo Tsunoda, Yasuhiko Kano, Yusuke Furukawa, Kenichi Suzuki, Yasuo Yazawa, and Miyuki Akutsu

Subjects

Cancer Research, medicine.drug_class, Thiophenes, Pharmacology, Antimetabolite, Thymidylate synthase, Article, Drug Administration Schedule, Raltitrexed, chemistry.chemical_compound, In vivo, Isobologram, Antineoplastic Combined Chemotherapy Protocols, Tumor Cells, Cultured, Humans, Medicine, Dose-Response Relationship, Drug, biology, business.industry, Cell growth, Synergism, Drug Synergism, Drug interaction, Colon cancer, Methotrexate, Oncology, chemistry, Colonic Neoplasms, Antifolate, Quinazolines, biology.protein, Drug Screening Assays, Antitumor, business, medicine.drug

Abstract

The folate-dependent enzymes are attractive targets for cancer chemotherapy. Methotrexate (MTX), which inhibits dihydrofolate reductase, has been widely used for the treatment of solid tumors and hematological cancers. Raltitrexed ("Tomudex") ), which inhibits thymidylate synthase, is a novel anticancer agent active against colorectal cancer and some other solid tumors. We studied the optimal schedule of raltitrexed and MTX in combination against four human colon cancer cell lines Colo201, Colo320, LoVo, and WiDr. These cells were simultaneously exposed to raltitrexed and MTX for 24 h, or sequentially exposed to raltitrexed for 24 h followed by MTX for 24 h, or vice versa. Cell growth inhibition after 5 days was determined by using 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide (MTT) assay. The effects of drug combinations at the concentrations of drug that produced 80% and 50% cell growth inhibition (IC(80) and IC(50)) were analyzed by the isobologram method (Steel and Peckham, 1979). Cytotoxic interactions between raltitrexed and MTX were schedule-dependent. The simultaneous exposure to raltitrexed and MTX showed additive effects in Colo201, LoVo and WiDr cells and antagonistic effects in Colo320 cells. The sequential exposure to raltitrexed followed by MTX produced additive effects in all four cell lines. The sequential exposure to MTX followed by raltitrexed produced synergistic effects in Colo201, LoVo and WiDr cells and additive effects in Colo320 cells. These findings suggest that the sequential administration of MTX followed by raltitrexed produces more than the expected cytotoxicity and may be the optimal schedule at the cellular level. Further in vivo and clinical studies will be necessary to determine the toxicity and to test the antitumor effects of sequential administration of MTX followed by raltitrexed proposed on the basis of the in vitro synergism.

Published

2001

20. Schedule-dependent Interactions between Raltitrexed and Cisplatin in Human Carcinoma Cell Linesin vitro

Author

Yasuo Yazawa, Yasuhiko Kano, Miyuki Akutsu, Saburo Tsunoda, and Kenichi Suzuki

Subjects

Cancer Research, medicine.medical_treatment, Thiophenes, Pharmacology, Thymidylate synthase, Drug Administration Schedule, Article, Raltitrexed, In vivo, Neoplasms, Isobologram, Antineoplastic Combined Chemotherapy Protocols, Tumor Cells, Cultured, medicine, Humans, Drug combination, Cytotoxicity, Cisplatin, Chemotherapy, biology, Cell growth, business.industry, Drug interaction, Oncology, Immunology, Quinazolines, biology.protein, business, medicine.drug

Abstract

Raltitrexed ('Tomudex') is a new anticancer agent which inhibits thymidylate synthase. To provide a rational basis for clinical trial design of the combination of raltitrexed and cisplatin, we studied the cytotoxic effects of this combination using various schedules in vitro and four human colon cancer cell lines, Colo201, Colo320, LoVo, and WiDr. Cell growth inhibition after 5 days was determined by using 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide (MTT) reduction assay. The effects of drug combinations at the concentration producing 80% cell growth inhibition (IC(80)) level were analyzed by the isobologram method. Simultaneous exposure to raltitrexed and cisplatin for 24 h, and sequential exposure to raltitrexed followed by cisplatin produced additive effects in the Colo201, Colo320, and LoVo cells, and additive and synergistic effects in WiDr cells. Sequential exposure to cisplatin followed by raltitrexed produced additive effects in the Colo201 cells and antagonistic effects in other three cell lines. Simultaneous and continuous exposure to both agents for 5 days produced additive effects in all four cell lines. These findings suggest that the simultaneous administration of raltitrexed and cisplatin, or the sequential administration of raltitrexed followed by cisplatin, generally produce the expected cytotoxicity at the cellular level and are optimal schedules, while the sequential administration of cisplatin followed by raltitrexed produces antagonistic effects and is inappropriate for this combination. Further in vivo and clinical studies will be necessary to determine the toxicity and antitumor effects of this schedule.

Published

2000

21. Cytostatic versus cytocidal profiling of quinoline drug combinations via modified fixed-ratio isobologram analysis

Author

Alexander P. Gorka, Lauren M. Jacobs, and Paul D. Roepe

Subjects

Drug, Tafenoquine, Combination therapy, Cell Survival, media_common.quotation_subject, Plasmodium falciparum, Quinoline, Drug resistance, P. falciparum, Pharmacology, Biology, Antimalarials, Inhibitory Concentration 50, chemistry.chemical_compound, Isobologram, Animals, Humans, Potency, IC50, media_common, Cytocidal, Research, Drug Synergism, Malaria, Drug Combinations, Infectious Diseases, chemistry, Quinolines, Drug Therapy, Combination, Parasitology, Antagonism, Cell Division

Abstract

Background Drug combination therapy is the frontline of malaria treatment. There is an ever-accelerating need for new, efficacious combination therapies active against drug resistant malaria. Proven drugs already in the treatment pipeline, such as the quinolines, are important components of current combination therapy and also present an attractive test bank for rapid development of new concepts. Methods The efficacy of several drug combinations versus chloroquine-sensitive and chloroquine-resistant strains was measured using both cytostatic and cytocidal potency assays. Conclusions These screens identify quinoline and non-quinoline pairs that exhibit synergy, additivity, or antagonism using the fixed-ratio isobologram method and find tafenoquine – methylene blue combination to be the most synergistic. Also, interestingly, for selected pairs, additivity, synergy, or antagonism defined by quantifying IC50 (cytostatic potency) does not necessarily predict similar behaviour when potency is defined by LD50 (cytocidal potency). These data further support an evolving new model for quinoline anti-malarials, wherein haem and haemozoin are the principle target for cytostatic activity, but may not be the only target relevant for cytocidal activity.

Published

2013

22. Cannabidivarin-rich cannabis extracts are anticonvulsant in mouse and rat via a CB1 receptor-independent mechanism

Author

Hill, T D M, Cascio, M-G, Romano, B, Duncan, M, Pertwee, R G, Williams, C M, Whalley, B J, Hill, A J, Hill, T. D. M., Cascio, M. -. G., Romano, Barbara, Duncan, M., Pertwee, R. G., Williams, C. M., Whalley, B. J., and Hill, A. J.

Subjects

Male, seizure, Motor Activity, Rats, Inbred WKY, isobologram, radioligand binding assay, Plant Extract, cannabidiol, Mice, Receptor, Cannabinoid, CB1, Seizures, Anticonvulsant, Animals, Cannabi, tolerability, Cannabinoid, Cannabis, Pharmacology, Plants, Medicinal, Dose-Response Relationship, Drug, Hand Strength, Cannabinoids, Plant Extracts, Animal, cannabidivarin, Pilocarpine, Brain, Research Papers, Rats, Disease Models, Animal, Mice, Inbred DBA, epilepsy, Pentylenetetrazole, Rat, Anticonvulsants, Noise, Phytotherapy, Protein Binding

Abstract

Background and Purpose Epilepsy is the most prevalent neurological disease and is characterized by recurrent seizures. Here, we investigate (i) the anticonvulsant profiles of cannabis-derived botanical drug substances (BDSs) rich in cannabidivarin (CBDV) and containing cannabidiol (CBD) in acute in vivo seizure models and (ii) the binding of CBDV BDSs and their components at cannabinoid CB1 receptors. Experimental Approach The anticonvulsant profiles of two CBDV BDSs (50-422 mg·kg-1) were evaluated in three animal models of acute seizure. Purified CBDV and CBD were also evaluated in an isobolographic study to evaluate potential pharmacological interactions. CBDV BDS effects on motor function were also investigated using static beam and grip strength assays. Binding of CBDV BDSs to cannabinoid CB1 receptors was evaluated using displacement binding assays. Key Results CBDV BDSs exerted significant anticonvulsant effects in the pentylenetetrazole (≥100 mg·kg-1) and audiogenic seizure models (≥87 mg·kg-1), and suppressed pilocarpine-induced convulsions (≥100 mg·kg-1). The isobolographic study revealed that the anticonvulsant effects of purified CBDV and CBD were linearly additive when co-administered. Some motor effects of CBDV BDSs were observed on static beam performance; no effects on grip strength were found. The Δ9- tetrahydrocannabinol and Δ9-tetrahydrocannabivarin content of CBDV BDS accounted for its greater affinity for CB1 cannabinoid receptors than purified CBDV. Conclusions and Implications CBDV BDSs exerted significant anticonvulsant effects in three models of seizure that were not mediated by the CB1 cannabinoid receptor and were of comparable efficacy with purified CBDV. These findings strongly support the further clinical development of CBDV BDSs for the treatment of epilepsy.

Published

2013

23. Increased toxicity of a trinuclear Pt-compound in a human squamous carcinoma cell line by polyamine depletion

Author

Stina Oredsson, Johan Kjellström, and Johan Wennerberg

Subjects

Cancer Research, Spermine, Biology, Pharmacology, lcsh:RC254-282, chemistry.chemical_compound, Isobologram, medicine, Genetics, Polyamines, alpha-difluoromethylornithine, lcsh:QH573-671, Cytotoxicity, α-difluoromethylornithine, Head and neck carcinoma, Cisplatin, BBR3464, N1,N11-diethylnorspermine, lcsh:Cytology, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, N-1, Squamous carcinoma, Spermidine, N-11-diethylnorspermine, Polyamine Analogue, chemistry, Biochemistry, Oncology, Cancer and Oncology, Putrescine, Primary Research, Polyamine, medicine.drug

Abstract

Background Mononuclear platinum anticancer agents hold a pivotal place in the treatment of many forms of cancers, however, there is a potential to improve response to evade resistance development and toxic side effects. BBR3464 is a promising trinuclear platinum anticancer agent, which is a polyamine mimic. The aim was to investigate the influence of polyamine pool reduction on the cytotoxic effects of the trinuclear platinum complex BBR3464 and cisplatin. Polyamine pool reduction was achieved by treating cells with either the polyamine biosynthesis inhibitor α-difluoromethylornithine (DFMO) or the polyamine analogue N1,N11-diethylnorspermine (DENSPM). Methods A human squamous cell carcinoma cell line, LU-HNSCC-4, established from a primary head and neck tumour was used to evaluate cellular effects of each drug alone or combinations thereof. High-performance liquid-chromatography was used to quantify intracellular polyamine contents. Inductively coupled mass spectroscopy was used to quantify intracellular platinum uptake. Cells were exposed to DFMO or DENSPM during 48 h at concentrations ranging from 0 to 5 mM or 0 to 10 μM, respectively. Thereafter, non-treated and treated cells were exposed to cisplatin or BBR3464 during 1 h at concentrations ranging from 0 to 100 μM. A 96-well assay was used to determine cytotoxicity after five days after treatment. Results The cytotoxic effect of BBR3464 on LU-HNSCC-4 cells was increased after cells were pre-treated with DENSPM or DFMO, and the interaction was found to be synergistic. In contrast, the interaction between cisplatin and DFMO or DENSPM was near-additive to antagonistic. The intracellular levels of the polyamines putrescine and spermidine were decreased after treatment with DFMO, and treatment with DENSPM resulted in an increase in putrescine level and concomitant decrease in spermidine and spermine levels. The uptake of BBR3464 was significantly increased after pre-treatment of the cells with DFMO, and varied dependent on the concentration of DENSPM. The uptake of cisplatin was unchanged. Conclusions Taken together, these results demonstrate that combinations of polyamine synthesis inhibitors with BBR3464 appear to be a promising approach to enhance the anticancer activity against HSCC.

Published

2012

24. Interactions of propofol and remifentanil on bispectral index under 66% N2O: analysis by dose-effect curve, isobologram, and combination index

Author

Hyun Joo Ahn, Jie Ae Kim, and Won Ho Kim

Subjects

Clinical Research Article, business.industry, Remifentanil, Combination index, Pharmacology, Effective dose (pharmacology), Anesthesiology and Pain Medicine, Bispectral index, Synergies, Isobologram, Anesthesia, Medicine, Dose reduction, business, Propofol, American society of anesthesiologists, medicine.drug, Dose-effect curve

Abstract

BACKGROUND: Propofol and remifentanil are usually co-administered and have shown synergistic effect for anesthesia. However, the synergistic effect of the two drugs on hypnosis measured by bispectral index (BIS) was controversial in previous studies. The aim of this study was to identify the interaction of propofol and remifentanil on BIS and the optimal dose combinations for hypnosis under 66% N(2)O during surgery. METHODS: Patients (age 55-75 and American Society of Anesthesiologists [ASA] 1-2) undergoing gastrectomy were enrolled in this study. Propofol and remifentanil were co-administered incrementally at 1 : 1 potent ratio (the P1R1 group), at 1 : 2 potent ratio (the P1R2 group), or at 2 : 1 potent ratio (the P2R1 group) using effect site target-controlled infusion and BIS was measured. 66% N(2)O was concomitantly administered to all groups. The dose-effect curves, the 90% effective dose (EC(90)) for adequate hypnosis (BIS 40), isobolograms and combination index were obtained by Calcusyn program (Biosoft) to reveal the interaction of propofol and remifentanil. RESULTS: The P2R1 group showed synergistic action on BIS. However, the other groups needed larger amount of each drug than the doses of additive action. The EC(90) of the P2R1 group was propofol, 3.34 µg/ml and remifentanil, 2.41 ng/ml under 66% of N(2)O. CONCLUSIONS: Propofol dominant co-administration is needed for dose reduction in BIS guided hypnosis.

Published

2010

25. Looking for combination of benznidazole and Trypanosoma cruzi-triosephosphate isomerase inhibitors for Chagas disease treatment

Author

Elena Aguilera, Guzmán Álvarez, Ninfa Vera de Bilbao, Mercedes González, Elva Serna, Susana Torres, Gloria Yaluff, Javier Varela, Hugo Cerecetto, Aguilera Elena, Universidad de la República (Uruguay). Facultad de Ciencias. Instituto de Química Biológica, Varela Javier, Universidad de la República (Uruguay). Facultad de Ciencias. Instituto de Química Biológica, Serna Elva, Universidad Nacional de Asunción (Paraguay), Torres Susana, Universidad Nacional de Asunción (Paraguay), Yaluff Gloria, Universidad Nacional de Asunción (Paraguay), De Bilbao Ninfa Vera, Universidad Nacional de Asunción (Paraguay), Cerecetto Hugo, Universidad de la República (Uruguay). Facultad de Ciencias. Centro de Investigaciones Nucleares, Álvarez Guzmán, Universidad de la República (Uruguay). Facultad de Ciencias. Instituto de Química Biológica, and González Mercedes, Universidad de la República (Uruguay). Facultad de Ciencias. Instituto de Química Biológica

Subjects

0301 basic medicine, Microbiology (medical), Drug, Chagas disease, Male, lcsh:Arctic medicine. Tropical medicine, lcsh:RC955-962, media_common.quotation_subject, Trypanosoma cruzi, 030106 microbiology, lcsh:QR1-502, Antibodies, Protozoan, Pharmacology, lcsh:Microbiology, isobologram, 03 medical and health sciences, Mice, in vivo studies, In vivo, Drug tolerance, synergism, parasitic diseases, Medicine, Animals, Trypanocidal agent, media_common, Mice, Inbred BALB C, biology, business.industry, Drug Synergism, Articles, Drugs, Investigational, biology.organism_classification, medicine.disease, Trypanocidal Agents, In vitro, Drug Combinations, 030104 developmental biology, Benznidazole, Nitroimidazoles, Immunoglobulin G, business, medicine.drug, Triose-Phosphate Isomerase

Abstract

BACKGROUND The current chemotherapy for Chagas disease is based on monopharmacology with low efficacy and drug tolerance. Polypharmacology is one of the strategies to overcome these limitations. OBJECTIVES Study the anti-Trypanosoma cruzi activity of associations of benznidazole (Bnz) with three new synthetic T. cruzi-triosephosphate isomerase inhibitors, 2, 3, and 4, in order to potentiate their actions. METHODS The in vitro effect of the drug combinations were determined constructing the corresponding isobolograms. In vivo activities were assessed using an acute murine model of Chagas disease evaluating parasitaemias, mortalities and IgG anti-T. cruzi antibodies. FINDINGS The effect of Bnz combined with each of these compounds, on the growth of epimastigotes, indicated an additive action or a synergic action, when combining it with 2 or 3, respectively, and an antagonic action when combining it with 4. In vivo studies, for the two chosen combinations, 2 or 3 plus one fifth equivalent of Bnz, showed that Bnz can also potentiate the in vivo therapeutic effects. For both combinations a decrease in the number of trypomastigote and lower levels of anti-T. cruzi IgG-antibodies were detected, as well clear protection against death. MAIN CONCLUSIONS These results suggest the studied combinations could be used in the treatment of Chagas disease.

26. In vitro synergistic effect of fluoroquinolone analogues in combination with artemisinin against Plasmodium falciparum; their antiplasmodial action in rodent malaria model

Author

Roshan Kumar Dutta, Satish K. Awasthi, Drishti Agarwal, Sandeep K. Dixit, Manish Sharma, Ashok K. Singh, and Rinkoo D. Gupta

Subjects

Drug, Erythrocytes, Combination therapy, Plasmodium berghei, media_common.quotation_subject, Plasmodium falciparum, Pharmacology, antiplasmodial activity, isobologram, Antimalarials, Mice, In vivo, parasitic diseases, medicine, Animals, Humans, Artemisinin, Fluoroquinolone derivatives, Cells, Cultured, media_common, biology, business.industry, Research, Drug Synergism, medicine.disease, biology.organism_classification, In vitro, Artemisinins, Infectious Diseases, artemisinin, Parasitology, business, Malaria, medicine.drug, Fluoroquinolones

Abstract

Background Emergence of drug-resistant parasite strains has surfaced as a major obstacle in attempts to ameliorate malaria. Current treatment regimen of malaria relies on the concept of artemisinin-based combination therapy (ACT). Methods Fluoroquinolone analogues, compounds 10, 12 and 18 were investigated for their anti-malarial interaction in combination with artemisinin in vitro, against Plasmodium falciparum 3D7 strain, employing fixed-ratio combination isobologram method. In addition, the efficacy of these compounds was evaluated intraperitoneally in BALB/c mice infected with chloroquine-resistant Plasmodium berghei ANKA strain in the Peters’ four-day suppressive test. Results Promising results were obtained in the form of synergistic or additive interactions. Compounds 10 and 12 were found to have highly synergistic interactions with artemisinin. Antiplasmodial effect was further verified by the convincing ED50 values of these compounds, which ranged between 2.31 and 3.09 (mg/kg BW). Conclusions In vivo studies substantiated the potential of the fluoroquinolone derivatives to be developed as synergistic partners for anti-malarial drug combinations.