Virtual screening applications in short-chain dehydrogenase/reductase research

Beck, Katharina R.; Kaserer, Teresa; Schuster, Daniela; Odermatt, Alex

doi:10.1016/j.jsbmb.2017.03.008

Cited by 25 publications

(9 citation statements)

References 199 publications

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“…Consisted of more than 163,120 members [21], SDR enzymes are found in different classes of oxidoreductases, isomerases, and lyases [21,22], with multiple functions such as carbonyl-alcohol oxidoreduction, steroid isomerase, enoyl-CoA reduction, decarboxylase, dehalogenase, dehydratase, C=N reduction and epimerase [22][23][24], covering broad substrates such as sugars, steroids, retinoids, lipids, polyols, prostaglandins and androstenedione [24,25]. SDRs could be further classified into six types at least according to their sequence differences, i.e., "Classical," "Extended," "Atypical," "Intermediate," "Divergent," "Complex" and some members "Unassigned" (Table 1) [21,22,26].…”

Section: Characteristics and Functions Of Hsdhs From Sdrsmentioning

confidence: 99%

Molecular Mechanism Study on Stereo-Selectivity of α or β Hydroxysteroid Dehydrogenases

et al. 2021

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Hydroxysteroid dehydrogenases (HSDHs) are from two superfamilies of short-chain dehydrogenase (SDR) and aldo–keto reductase (AKR). The HSDHs were summarized and classified according to their structural and functional differences. A typical pair of enzymes, 7α–hydroxysteroid dehydrogenase (7α–HSDH) and 7β–hydroxysteroid dehydrogenase (7β–HSDH), have been reported before. Molecular docking of 7-keto–lithocholic acid(7–KLA) to the binary of 7β–HSDH and nicotinamide adenine dinucleotide phosphate (NADP+) was realized via YASARA, and a possible binding model of 7β-HSDH and 7-KLA was obtained. The α side of 7–KLA towards NADP+ in 7β–HSDH, while the β side of 7–KLA towards nicotinamide adenine dinucleotide (NAD+) in 7α-HSDH, made the orientations of C7–OH different in products. The interaction between Ser193 and pyrophosphate of NAD(P)+ [Ser193–OG···3.11Å···O1N–PN] caused the upturning of PN–phosphate group, which formed a barrier with the side chain of His95 to make 7–KLA only able to bind to 7β–HSDH with α side towards nicotinamide of NADP+. A possible interaction of Tyr253 and C24 of 7–KLA may contribute to the formation of substrate binding orientation in 7β–HSDH. The results of sequence alignment showed the conservation of His95, Ser193, and Tyr253 in 7β–HSDHs, exhibiting a significant difference to 7α–HSDHs. The molecular docking of other two enzymes, 17β–HSDH from the SDR superfamily and 3(17)α–HSDH from the AKR superfamily, has furtherly verified that the stereospecificity of HSDHs was related to the substrate binding orientation.

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Section: Characteristics and Functions Of Hsdhs From Sdrsmentioning

confidence: 99%

Molecular Mechanism Study on Stereo-Selectivity of α or β Hydroxysteroid Dehydrogenases

et al. 2021

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“…From among the introduced approaches, drug repurposing (DR) methods, which seek the hidden benefits of the existing drugs in treating different diseases, have produced promising outcomes. Given the capabilities of the computational approaches in reducing the spent time and cost of the drug discovery projects [ 4 ], many studies have been conducted to identify the candidate medicines for treating COVID-19. In this review, based on the utilized computational DR methods, the studies (at the time of conducting this review) have been divided into four classes, including (i) machine learning (ML), (ii) network-based (NB), (iii) structure-based DR (SBDR) and (iv) hybrid approaches.…”

Section: Introductionmentioning

confidence: 99%

Structure-based drug repurposing against COVID-19 and emerging infectious diseases: methods, resources and discoveries

Masoudi-Sobhanzadeh

Salemi

Pourseif

et al. 2021

Briefings in Bioinformatics

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To attain promising pharmacotherapies, researchers have applied drug repurposing (DR) techniques to discover the candidate medicines to combat the coronavirus disease 2019 (COVID-19) outbreak. Although many DR approaches have been introduced for treating different diseases, only structure-based DR (SBDR) methods can be employed as the first therapeutic option against the COVID-19 pandemic because they rely on the rudimentary information about the diseases such as the sequence of the severe acute respiratory syndrome coronavirus 2 genome. Hence, to try out new treatments for the disease, the first attempts have been made based on the SBDR methods which seem to be among the proper choices for discovering the potential medications against the emerging and re-emerging infectious diseases. Given the importance of SBDR approaches, in the present review, well-known SBDR methods are summarized, and their merits are investigated. Then, the databases and software applications, utilized for repurposing the drugs against COVID-19, are introduced. Besides, the identified drugs are categorized based on their targets. Finally, a comparison is made between the SBDR approaches and other DR methods, and some possible future directions are proposed.

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“…However, these vaccine targets cannot fully protect against the virulent challenge, and a suitable vaccine is still unavailable (20)(21)(22). The short-chain dehydrogenases/reductases family (SDR family) is a large family of enzymes in eukaryotes and a potential vaccine target (23), which is involved in the synthesis of molecules, including lipids, vitamins, drugs, and carbohydrates (24). A 368-amino acid protein encoded as "oxidoreductase" from the T. gondii SDR family in the Uniprot database (https://www.uniprot.org/) aroused our particular attention.…”

Section: Introductionmentioning

confidence: 99%

With Chitosan and PLGA as the Delivery Vehicle, Toxoplasma gondii Oxidoreductase-Based DNA Vaccines Decrease Parasite Burdens in Mice

Cao

Gao

et al. 2021

Front. Immunol.

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Toxoplasma gondii (T. gondii) is an intracellular parasitic protozoan that can cause serious public health problems. However, there is no effectively preventive or therapeutic strategy available for human and animals. In the present study, we developed a DNA vaccine encoding T. gondii oxidoreductase from short-chain dehydrogenase/reductase family (TgSDRO-pVAX1) and then entrapped in chitosan and poly lactic-co-glycolic acid (PLGA) to improve the efficacy. When encapsulated in chitosan (TgSDRO-pVAX1/CS nanospheres) and PLGA (TgSDRO-pVAX1/PLGA nanospheres), adequate plasmids were loaded and released stably. Before animal immunizations, the DNA vaccine was transfected into HEK 293-T cells and examined by western blotting and laser confocal microscopy. Th1/Th2 cellular and humoral immunity was induced in immunized mice, accompanied by modulated secretion of antibodies and cytokines, promoted the maturation and MHC expression of dendritic cells, and enhanced the percentages of CD4+ and CD8+ T lymphocytes. Immunization with TgSDRO-pVAX1/CS and TgSDRO-pVAX1/PLGA nanospheres conferred significant immunity with lower parasite burden in the mice model of acute toxoplasmosis. Furthermore, our results also lent credit to the idea that TgSDRO-pVAX1/CS and TgSDRO-pVAX1/PLGA nanospheres are substitutes for each other. In general, the current study proposed that TgSDRO-pVAX1 with chitosan or PLGA as the delivery vehicle is a promising vaccine candidate against acute toxoplasmosis.

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Virtual screening applications in short-chain dehydrogenase/reductase research

Cited by 25 publications

References 199 publications

Molecular Mechanism Study on Stereo-Selectivity of α or β Hydroxysteroid Dehydrogenases

Molecular Mechanism Study on Stereo-Selectivity of α or β Hydroxysteroid Dehydrogenases

Structure-based drug repurposing against COVID-19 and emerging infectious diseases: methods, resources and discoveries

With Chitosan and PLGA as the Delivery Vehicle, Toxoplasma gondii Oxidoreductase-Based DNA Vaccines Decrease Parasite Burdens in Mice

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