M. Ugalde scite author profile

M. Ugalde

5Publications

50Citation Statements Received

111Citation Statements Given

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108

Affiliations

Bank of Mexico, Universidad Nacional Autónoma de México, Centro de Investigación en Materiales Avanzados

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Isobolographic analysis of the sedative interaction between six central nervous system depressant drugs and Valeriana edulis hydroalcoholic extract in mice*

Ugalde

Reza

González-Trujano

et al. 2005

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It has been declared frequently that valerian may potentiate the effect of other central nervous system (CNS) depressant drugs, however there has been a lack of experimental data. We have evaluated the profile of the interactions between the ethanol extract of Valeriana edulis spp procera and six CNS depressant drugs using an exploratory model to test the sedative effect in mice. All the compounds tested showed a dose-dependent sedative effect with the following ED50 values: valerian 181.62, diazepam 1.21, ethanol 1938, pentobarbital 11.86, buspirone 1.04, haloperidol 0.41 and diphenhydramine 17.06 mg kg-1. An isobolographic analysis was used to evaluate the sedative interaction of the intraperitoneal co-administration of 1:1 fixed-ratio combination of equi-effective doses of valerian extract with each CNS depressant drug. The ED50 theoretical (Zadd) and experimental (Zexp) for each combination were: valerian+diazepam,Zadd=91.41 mg kg-1, Zexp=81.64 mg kg-1; valerian+ethanol, Zadd=1060.22 mg kg-1, Zexp=687.89 mg kg-1; valerian+pentobarbital, Zadd=96.74 mg kg-1, Zexp=151.83 mg kg-1; valerian+buspirone, Zadd=91.33 mg kg-1, Zexp=112.73 mg kg-1; valerian+haloperidol, Zadd=91.01 mg kg-1, Zexp=91.52 mg kg-1; valerian+diphenhydramine, Zadd=99.34 mg kg-1, Zexp=123.52 mg kg-1. Neither synergistic nor attenuate effects were found in any of the combinations evaluated. We concluded that the valerian extract did not potentiate the sedative effect of commonly prescribed CNS depressant drugs as was expected. The additive effect found through the isobolographic analysis suggested that the sedative effect of V. edulis resulted from the activation of common mechanisms of haloperidol, diazepam, buspirone, pentobarbital, diphenhydramine and ethanol.

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Pharmacodynamic interaction of the sedative effects of Ternstroemia pringlei (Rose) Standl. with six central nervous system depressant drugs in mice

Balderas

Reza

Ugalde

et al. 2008

Journal of Ethnopharmacology

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Heterocyclic variants of the 1,5‐benzodiazepine system. VI. Derivatives of 2‐methylthio‐4‐(p‐r‐phenyl)‐3H‐1,5‐benzodiazepines

Cortés

Martı́nez

Ugalde

et al. 1991

Journal of Heterocyclic Chem

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Ethyl 3‐[3H‐1,5‐benzodiazepin‐2‐yl]carbazates II were prepared in moderate yields from the title compounds and ethyl carbazate. The compounds II were easily transformed into 1H‐s‐triazolo[4,3‐a][1,5]benzodiazepin‐1‐ones III via a one‐step procedure. Reaction of triazolo‐1,5‐benzodiazepinones III with sodium hydride in methyl iodide gave a mixture of products from which were isolated two compounds IV and V. The structure of all products was confirmed by ir, 1H nmr and mass spectrometry.

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Preparation of rhodium nano-particles using microwaves

Ugalde

Chavira

Figueroa

et al. 2012

J Sol-Gel Sci Technol

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New Synthesis Method to Obtain Pd Nano-Crystals

Ugalde¹,

Chavira²,

Ochoa-Lara³

et al. 2011

JNanoR

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M. Ugalde

Isobolographic analysis of the sedative interaction between six central nervous system depressant drugs and Valeriana edulis hydroalcoholic extract in mice*

Pharmacodynamic interaction of the sedative effects of Ternstroemia pringlei (Rose) Standl. with six central nervous system depressant drugs in mice

Heterocyclic variants of the 1,5‐benzodiazepine system. VI. Derivatives of 2‐methylthio‐4‐(p‐r‐phenyl)‐3H‐1,5‐benzodiazepines

Preparation of rhodium nano-particles using microwaves

New Synthesis Method to Obtain Pd Nano-Crystals

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