MIND-BEST: Web Server for Drugs and Target Discovery; Design, Synthesis, and Assay of MAO-B Inhibitors and Theoretical−Experimental Study of G3PDH Protein from<i>Trichomonas gallinae</i>

González-Dı́az, Humberto; Prado-Prado, Francisco J.; Garcı́a-Mera, Xerardo; Alonso, Nerea; Abeijón, Paula; Caamaño, Olga; Yáñez, Matilde; Munteanu, Cristian R.; Pazos, Alejandro; Dea-Ayuela, María Auxiliadora; Gómez-Muñoz, María Teresa; Garijo, M. Magdalena; Sansano, José M.; Ubeira, Florencio M.

doi:10.1021/pr101009e

Cited by 73 publications

(46 citation statements)

References 133 publications

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“…As shown in this scheme, they were synthesized from the hidroxy mono-or dipropargylaminoindans (1−4), previously described by us, and prepared following ) is the probability with which the model predicts a value of the measure higher than the cutoff for compound 11 procedures described in the literature. 28 Please see details about the techniques used for the characterization of compounds and the results obtained (NMR and IR spectra) in the Supporting Information. 3.2.2.…”

Section: Discussionmentioning

confidence: 99%

“…12,13 We can use different software to calculate molecular descriptors and develop mt-QSAR or mx-QSAR models: DRAGON, 14,15 MOE, 16 TOPS-MODE, 17−19 CODESSA, 20−22 TOMOCOMD, 23,24 or MARCH-INSIDE (MI), 25−27 software used in this work. For instance, we used MI to develop different mt-QSAR classifiers/web-servers such as MIND-BEST 28 or NL MIND-BEST. 29 The first two use MI only, but the third combines DRAGON and MI to calculate descriptors for drugs and proteins, respectively.…”

Section: For Instance Mueller Et Al Reported In Acs Chemicalmentioning

confidence: 99%

“…The 3-OH, 3-OAc, and 3-OBz rasagiline derivatives synthesized and experimentally assayed by our group were not very active against some of the expected targets. 28 This situation encouraged us to study the possible neuroprotective activity of our compounds directly in the neuronal culture. In fact, 3-OH, 3-OAc, and 3-OBz rasagiline derivatives were found to present interesting neuroprotective effects in experimental assays.…”

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confidence: 99%

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Model for High-Throughput Screening of Multitarget Drugs in Chemical Neurosciences: Synthesis, Assay, and Theoretic Study of Rasagiline Carbamates

Alonso

Caamaño

Romero-Duran

et al. 2013

ACS Chem. Neurosci.

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ABSTRACT:The disappointing results obtained in recent clinical trials renew the interest in experimental/computational techniques for the discovery of neuroprotective drugs. In this context, multitarget or multiplexing QSAR models (mt-QSAR/mx-QSAR) may help to predict neurotoxicity/neuroprotective effects of drugs in multiple assays, on drug targets, and in model organisms. In this work, we study a data set downloaded from CHEMBL; each data point (>8000) contains the values of one out of 37 possible measures of activity, 493 assays, 169 molecular or cellular targets, and 11 different organisms (including human) for a given compound. In this work, we introduce the first mx-QSAR model for neurotoxicity/neuroprotective effects of drugs based on the MARCH-INSIDE (MI) method. First, we used MI to calculate the stochastic spectral moments (structural descriptors) of all compounds. Next, we found a model that classified correctly 2955 out of 3548 total cases in the training and validation series with Accuracy, Sensitivity, and Specificity values > 80%. The model also showed excellent results in Computational-Chemistry simulations of High-Throughput Screening (CCHTS) experiments, with accuracy = 90.6% for 4671 positive cases. Next, we reported the synthesis, characterization, and experimental assays of new rasagiline derivatives. We carried out three different experimental tests: assay (1) in the absence of neurotoxic agents, assay (2) in the presence of glutamate, and assay (3) in the presence of H 2 O 2 . Compounds 11 with 27.4%, 8 with 11.6%, and 9 with 15.4% showed the highest neuroprotective effects in assays (1), (2), and (3), respectively. After that, we used the mx-QSAR model to carry out a CCHTS of the new compounds in >400 unique pharmacological tests not carried out experimentally. Consequently, this model may become a promising auxiliary tool for the discovery of new drugs for the treatment of neurodegenerative diseases.

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Section: Discussionmentioning

confidence: 99%

Section: For Instance Mueller Et Al Reported In Acs Chemicalmentioning

confidence: 99%

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confidence: 99%

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Model for High-Throughput Screening of Multitarget Drugs in Chemical Neurosciences: Synthesis, Assay, and Theoretic Study of Rasagiline Carbamates

Alonso

Caamaño

Romero-Duran

et al. 2013

ACS Chem. Neurosci.

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“…The functional groups modify the electronic properties of the targets; as a result they have the potential to block the metabolic pathway or restraint the conformation. Different methods have been used to predict the drug targets interaction based on QSAR [18], reverse docking [19], [20], [21]. The interactions can also be interpreted by, side effect similarity, drug based similarity, and target based similarity, based on interpretation of the networks [22], [23].…”

Section: Molecular Drug Targetsmentioning

confidence: 99%

Natural compounds for the drug targets of Sexually Transmitted Diseases (STD) using virtual screening

2013

IOSR-JPBS

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“…This mt-QSAR derived with MARCH-INSIDE is able to assemble the graphs drug-target networks that appears at a higher level based on the parameters of graphs at a lower structural level. The results obtained with this method to predict drug-target networks have been implemented in two public web-servers called the MIND-BEST and NL MIND-BEST [17,18], which can be available at the platform Bio-AIMS (http://miaja.tic. udc.es/Bio-AIMS/index.php).…”

Section: Introductionmentioning

confidence: 99%

Using Feature Selection Technique for Drug-Target Interaction Networks Prediction

Jiang²,

Wang³

et al. 2011

CMC

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Elucidating the interaction relationship between target proteins and all drugs is critical for the discovery of new drug targets. However, it is a big challenge to integrate and optimize different feature information into one single "knowledge view" for drug-target interaction prediction. In this article, a feature selection method was proposed to rank the original feature sets. Then, an improved bipartite learning graph method was used to predict four types of drug-target datasets based on the optimized feature subsets. The cross-validation results demonstrate that the proposed method can provide superior performance than previous method on four classes of drug target families.

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MIND-BEST: Web Server for Drugs and Target Discovery; Design, Synthesis, and Assay of MAO-B Inhibitors and Theoretical−Experimental Study of G3PDH Protein fromTrichomonas gallinae

Cited by 73 publications

References 133 publications

Model for High-Throughput Screening of Multitarget Drugs in Chemical Neurosciences: Synthesis, Assay, and Theoretic Study of Rasagiline Carbamates

Model for High-Throughput Screening of Multitarget Drugs in Chemical Neurosciences: Synthesis, Assay, and Theoretic Study of Rasagiline Carbamates

Natural compounds for the drug targets of Sexually Transmitted Diseases (STD) using virtual screening

Using Feature Selection Technique for Drug-Target Interaction Networks Prediction

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