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3. Contributors

Author

Aguayo, Luis G., primary, Ahmed, Marium, additional, Ahmed, Mohamed H., additional, Ahmed, Musaab, additional, Albuquerque, Hélio M.T., additional, Alonso, Alicia, additional, Ashkar, Rana, additional, Azzaz, Fodil, additional, Baier, Carlos J., additional, Barrantes, Francisco J., additional, Bednarska-Makaruk, Małgorzata, additional, Bell, Andrew S., additional, Benito-Vicente, Asier, additional, Brown, Michael F., additional, Bukiya, Anna N., additional, Burgos, Carlos F., additional, Chahinian, Henri, additional, Chatuphonprasert, Waranya, additional, Chong, Parkson Lee-Gau, additional, Cicero, Arrigo F.G., additional, Cincione, Ivan R., additional, Clemente, Tatiana M., additional, Cook, George A., additional, Cournia, Zoe, additional, Di Scala, Coralie, additional, Doktorova, Milka, additional, Doole, Fathima T., additional, Dopico, Alex M., additional, Drosos, Alexandros A., additional, Du, Hong, additional, Elam, Marshall B., additional, Ellinger, Isabella, additional, Fantini, Jacques, additional, Ferrari, Filipe, additional, Galicia-Garcia, Unai, additional, García-Arribas, Aritz B., additional, Gilk, Stacey D., additional, Goñi, Félix M., additional, Gonzalez-Sanmiguel, Juliana, additional, Grabowski, Gregory A., additional, Gupta, Sudipta, additional, Herfel, Tina, additional, Hu, DanRong, additional, Huang, Juyang, additional, Jebari-Benslaiman, Shifa, additional, Jiang, Qiu-Xing, additional, Karr, Samantha, additional, Khelashvili, George, additional, Kiriakidi, Sofia, additional, Kovacs, Tamas, additional, Kumarage, Teshani, additional, Lardinois, Claude K., additional, Larrea-Sebal, Asier, additional, Levitan, Irena, additional, Li, Hanxuan, additional, Li, Wei, additional, Lohoff, Falk W., additional, Ługowska, Agnieszka, additional, Martin, Cesar, additional, Martins, Vítor M., additional, Mavromoustakos, Thomas, additional, Mc Auley, Mark T., additional, Mital, Dushyant, additional, Moore,, Bob M., additional, Morgan, Amy E., additional, Mouritsen, Ole G., additional, Mysiewicz, Steven, additional, North, Kelsey C., additional, O’Connell, Emma M., additional, Pasenkiewicz-Gierula, Marta, additional, Qian, ZhiYong, additional, Roa, Jorge P., additional, Rosenhouse-Dantsker, Avia, additional, Santos, Clementina M.M., additional, Silva, Artur M.S., additional, Slayden, Alexandria, additional, Soliman, Ghada A., additional, Stein, Natalia, additional, Stein, Ricardo, additional, Subczynski, Witold K., additional, Sugár, István P., additional, Szente, Lajos, additional, Uribe, Kepa B., additional, Varga, Zoltan, additional, Venetsanopoulou, Aliki I., additional, Voulgari, Paraskevi V., additional, Welty, Francine K., additional, Widomska, Justyna, additional, Yahi, Nouara, additional, Zadak, Zdenek, additional, and Zakany, Florina, additional

Published
2022
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7. Effects of Cholesterol on GPCR Function: Insights from Computational and Experimental Studies

Author

Kiriakidi, Sofia, Kolocouris, Antonios, Liapakis, George, Ikram, Saima, Durdagi, Serdar, Mavromoustakos, Thomas, COHEN, IRUN R., Editorial Board Member, LAJTHA, ABEL, Editorial Board Member, LAMBRIS, JOHN D., Editorial Board Member, PAOLETTI, RODOLFO, Editorial Board Member, REZAEI, NIMA, Editorial Board Member, Rosenhouse-Dantsker, Avia, editor, and Bukiya, Anna N., editor

Published
2019
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10. Direct Access to Benzolactams and Benzolactones via Nickel Catalyzed Carbonylation with CO2.

Author

Giovanelli, Riccardo, Monda, Giulia, Kiriakidi, Sofia, Silva López, Carlos, Bertuzzi, Giulio, and Bandini, Marco

Subjects
AMINO group, LEWIS acids, CARBON dioxide, LACTAMS, NICKEL, CARBONYLATION
Abstract

A new nickel catalyzed cross‐electrophile coupling for accessing γ‐lactams (isoindolinones) as well as γ‐lactones (isobenzofuranones) via carbonylation with CO2 is documented. The protocol exploits the synergistic role of redox‐active Ni(II) complexes and AlCl3 as a CO2 activator/oxygen scavenger, leading to the formation of a wide range of cyclic amides and esters (28 examples) in good to high yields (up to 87 %). A dedicated computational investigation revealed the multiple roles played by AlCl3. In particular, the simultaneous transient protection of the pendant amino group of the starting reagents and the formation of the electrophilically activated CO2‐AlCl3 adduct are shown to concur in paving the way for an energetically favorable mechanistic pathway. [ABSTRACT FROM AUTHOR]

Published
2024
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13. Deciphering Nitroaromatics Reduction: Theoretical Insights into Dioxomolybdenum Catalysis with Biomass‐Derived Pinacol.

Author

Kiriakidi, Sofia, Silva López, Carlos, Sanz, Roberto, and Faza, Olalla Nieto

Subjects
*NITROAROMATIC compounds, *CATALYSIS, *DENSITY functional theory, *ACETONE, *GROUP 15 elements, *NITROBENZENE
Abstract

Density Functional Theory is used to unravel the mechanism of the nitrobenzene to aniline reduction, catalyzed by dioxomolybdenum (VI) dichloride. The use of pinacol as an oxoaccepting reagent and the production of only acetone and water as byproducts, signals a novel and environmentally friendly way to add value to the oxygen‐rich biomass‐derived polyols. The reaction proceeds through three consecutive cycles, each one responsible for one of the three reductive steps needed to yield aniline from nitrobenzene, with nitrosobenzene and hydroxylamine as intermediates. Each cycle regenerates the catalyst and releases one water and two acetone molecules. The mechanism involves singlet/triplet state crossings, a crucial feature in polyoxomolibdate catalyzed processes. The role of the Mo‐coordinated water as the provider of the mysterious protons needed to reduce the nitro group, was revealed. The disclosure of this challenging mechanism and its rate limiting step can contribute to the design of more effective Mo(VI) catalysts. [ABSTRACT FROM AUTHOR]

Published
2024
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15. Quercetin: A Potential Polydynamic Drug.

Author

Georgiou, Nikitas, Kakava, Margarita Georgia, Routsi, Efthymios Alexandros, Petsas, Errikos, Stavridis, Nikolaos, Freris, Christoforos, Zoupanou, Nikoletta, Moschovou, Kalliopi, Kiriakidi, Sofia, and Mavromoustakos, Thomas

Subjects
NATURAL products, FLAVONOIDS, QUERCETIN
Abstract

The study of natural products as potential drug leads has gained tremendous research interest. Quercetin is one of those natural products. It belongs to the family of flavonoids and, more specifically, flavonols. This review summarizes the beneficial pharmaceutical effects of quercetin, such as its anti-cancer, anti-inflammatory, and antimicrobial properties, which are some of the quercetin effects described in this review. Nevertheless, quercetin shows poor bioavailability and low solubility. For this reason, its encapsulation in macromolecules increases its bioavailability and therefore pharmaceutical efficiency. In this review, a brief description of the different forms of encapsulation of quercetin are described, and new ones are proposed. The beneficial effects of applying new pharmaceutical forms of nanotechnology are outlined. [ABSTRACT FROM AUTHOR]

Published
2023
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20. Two routes to hydrogen evolution for a Co-polypyridyl complex with two open sites

Author

Toro, Liqin Xue, Kiriakidi, Sofia, Thapper, Anders, Ott, Sascha, Lundberg, Marcus, Toro, Liqin Xue, Kiriakidi, Sofia, Thapper, Anders, Ott, Sascha, and Lundberg, Marcus

Abstract

Cobalt polypyridyl complexes efficiently catalyze hydrogen evolution in aqueous media and exhibit high stability under reducing conditions. Their stability and activity can be tuned through electronic and steric considerations, but the rationalization of these effects requires detailed mechanistic understanding. As an example, tetradentate ligands with two non-permanently occupied coordination sites show higher activity with these sites in cis compared to trans configuration. Here reaction mechanisms of the Co-polypyridyl complex [Co-II(bpma)Cl-2] (bpma = bipyridinylmethyl-pyridinylmethyl-methyl-amine) have been studied using hybrid density-functional theory. This complex has two exchangeable cis sites, and provides a flexible ligand environment with both pyridyl and amine coordination. Two main pathways with low barriers are found. One pathway, which includes both open sites, is hydrogen evolution from a Co-II-H intermediate with a water ligand as the proton donor. In the second pathway H-H bond formation occurs between the hydride and the protonated bpma ligand, with one open site acting as a spectator. The two pathways have similar barriers at higher pH, while the latter becomes more dominant at lower pH. The calculations consider a large number of interconnected variables; protonation sites, isomers, spin multiplicities, and the identities of the open binding sites, as well as their combinations, thus exploring many simultaneous dimensions within each pathway. The results highlight the effects of having two open cis-coordination sites and how their relative binding affinities change during the reaction pathway. They also illustrate why Co-II-H intermediates are more active than Co-III-H ones, and why pyridyl protonation gives lower reaction barriers than amine protonation.

Published
2022
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27. Molecular investigation of artificial and natural sweeteners as potential anti-inflammatory agents

Author

Chontzopoulou, Eleni, primary, Papaemmanouil, Christina D., additional, Chatziathanasiadou, Maria V., additional, Kolokouris, Dimitrios, additional, Kiriakidi, Sofia, additional, Konstantinidi, Athina, additional, Gerogianni, Ioanna, additional, Tselios, Theodore, additional, Kostakis, Ioannis K., additional, Chrysina, Evangelia D., additional, Hadjipavlou-Litina, Dimitra, additional, Tzeli, Demeter, additional, Tzakos, Andreas G., additional, and Mavromoustakos, Thomas, additional

Published
2021
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28. Applications of theoretical and biophysical studies on rational drug design

Author

Kiriakidi Sofia

Subjects
Θετικές Επιστήμες, Science
Abstract

Σε αυτή τη διατριβή μελετήθηκαν διάφορες πτυχές του ορθολογικού σχεδιασμού φαρμάκων, χρησιμοποιώντας μια πληθώρα υπολογιστικών τεχνικών. Αρχικά μελετήθηκε ο μηχανισμός κυκλοποίησης ενεργοποιημένων αλλενίων με καταλύτη σύμπλοκα του χρυσού, εφαρμόζοντας κβαντικούς υπολογισμούς. Τόσο αλλενικά τμήματα όσο και παράγωγά τους χρησιμοποιούνται ως δομικά τμήματα φαρμακευτικών μορίων σε μεγάλη ποικιλία φαρμακευτικών κατηγοριών, χάρη στη μεγάλη δραστικότητα και τη στερεοειδικότητά τους. Ο επόμενος στόχος αυτής της εργασίας ήταν η διερεύνηση του μηχανισμού φθορισμού ενός νέου ιατροτεχνολογικού προϊόντος με διαγνωστικές και χημειοθεραπευτικές ικανότητες, εφαρμόζοντας κβαντικούς υπολογισμούς διεγερμένης κατάστασης. Συγκεκριμένα, μελετήθηκε ένα ανάλογο της γεμσιταβίνης το οποίο παρουσιάζει φθορισμό ως προφάρμακο, επιτρέποντας την παρακολούθηση της στοχευμένης διανομής του φαρμάκου σε πραγματικό χρόνο, ενώ παράλληλα απελευθερώνει το κυτταροτοξικό φάρμακο κι έναν φθορίζοντα σηματοδότη στο περιβάλλον του καρκινικού όγκου. Τα θεωρητικά μας αποτελέσματα προέβλεψαν σωστά τον παραπάνω μηχανισμό φθορισμού, γεγονός που επιβεβαιώνεται και από τις πρώτες φθορισμομετρικές αναλύσεις. Τέλος, σε αυτή τη διατριβή μελετήθηκε ο μηχανισμός πρόσδεσης της καντεσαρτάνης στον υποδοχέα ΑΤ1R μέσω προσομοιώσεων Μοριακής Δυναμικής. Παρατηρήθηκε πως σε απλές λιπιδικές διπλοστιβάδες από DPPC η καντεσαρτάνη προσεγγίζει τον υποδοχέα μέσω της λιπιδικής μεμβράνης (έμμεσος μηχανισμός) ενώ η εξωκυττάρια είσοδος του ΑΤ1R (άμεσος μηχανισμός) εμποδίζεται από το Ν-τελικό του άκρο. Όταν μοντελοποίηθηκαν πιο σύνθετες λιπιδικές μεμβράνες με 40% χοληστερόλη, οι προσομοιώσεις μας έδειξαν πως η χοληστερόλη προσδένεται στον υποδοχέα σε μια ειδική περιοχή η οποία έχει χαρακτηριστεί ως Cholesterol Consensus Motif. Η πρόσδεση της χοληστερόλης σε αυτή την περιοχή προκαλεί αλλοστερικές αλλαγές στον υποδοχέα, καθιστώντας την εξωκυττάρια περιοχή του περισσότερο προσβάσιμη, ενώ παράλληλα αυξάνει την τάξη στις λιπιδικές μεμβράνες, επιβραδύνοντας την πλευρική διάχυση της καντεσαρτάνης προς αυτόν, μέσω της λιπιδικής στιβάδας. In this thesis, several aspects of rational drug design were studied by employing a plethora of computational techniques. Initially, the gold catalyzed cyclization mechanism of functionalized allenes was studied, by implementing quantum chemistry calculations. Both allenic moieties and their derivatives are used as drug building blocks in a wide variety of pharmaceutical categories, due to their reactivity and stereoselectivity. The next aim of this study was the fluorescence mechanism investigation of a novel theranostic device with the use of excited state quantum chemistry. In particular, a gemcitabine analogue which shows fluorescence as a prodrug was studied, allowing for the real-time observation of the drug delivery while when it is in the tumour environment, it releases the cytotoxic drug along with a fluorescent mark. Our theoretical results correctly predicted the above mechanism and were confirmed by preliminary fluorimetry assays. Finally, the drug binding mechanism of candesartan to AT1R was studied in this thesis, with the use of Molecular Dynamics. We observed that in pure DPPC bilayers candesartan approaches the receptor through the lipid membrane (indirect mechanism) while the extracellular entrance of the receptor (direct mechanism) is blocked by its N-terminus. When complex lipid membranes were modelled with 40% of cholesterol, our simulations showed that cholesterol binds the receptor in a special area characterized as Cholesterol Consensus Motif. The binding of cholesterol induces allosteric modulations on the receptor, resulting in a more accessible extracellular entrance while the ordering that induces on the lipid bilayer delays candesartan lateral diffusion to the receptor, through the lipid membrane.

Published
2021

31. Host–Guest Interactions between Candesartan and Its Prodrug Candesartan Cilexetil in Complex with 2-Hydroxypropyl-β-cyclodextrin: On the Biological Potency for Angiotensin II Antagonism

Author

Ntountaniotis, Dimitrios, primary, Andreadelis, Ioannis, additional, Kellici, Tahsin F., additional, Karageorgos, Vlasios, additional, Leonis, Georgios, additional, Christodoulou, Eirini, additional, Kiriakidi, Sofia, additional, Becker-Baldus, Johanna, additional, Stylos, Evgenios K., additional, Chatziathanasiadou, Maria V., additional, Chatzigiannis, Christos M., additional, Damalas, Dimitrios E., additional, Aksoydan, Busecan, additional, Javornik, Uroš, additional, Valsami, Georgia, additional, Glaubitz, Clemens, additional, Durdagi, Serdar, additional, Thomaidis, Nikolaos S., additional, Kolocouris, Antonios, additional, Plavec, Janez, additional, Tzakos, Andreas G., additional, Liapakis, George, additional, and Mavromoustakos, Thomas, additional

Published
2019
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32. Direct Access to Benzolactams and Benzolactones via Nickel Catalyzed Carbonylation with CO2.

Author

Giovanelli, Riccardo, Monda, Giulia, Kiriakidi, Sofia, Silva López, Carlos, Bertuzzi, Giulio, and Bandini, Marco

Subjects
*AMINO group, *LEWIS acids, *CARBON dioxide, *LACTAMS, *NICKEL, *CARBONYLATION
Abstract

A new nickel catalyzed cross‐electrophile coupling for accessing γ‐lactams (isoindolinones) as well as γ‐lactones (isobenzofuranones) via carbonylation with CO2 is documented. The protocol exploits the synergistic role of redox‐active Ni(II) complexes and AlCl3 as a CO2 activator/oxygen scavenger, leading to the formation of a wide range of cyclic amides and esters (28 examples) in good to high yields (up to 87 %). A dedicated computational investigation revealed the multiple roles played by AlCl3. In particular, the simultaneous transient protection of the pendant amino group of the starting reagents and the formation of the electrophilically activated CO2‐AlCl3 adduct are shown to concur in paving the way for an energetically favorable mechanistic pathway. [ABSTRACT FROM AUTHOR]

Published
2024
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34. Development of a DHA-Losartan hybrid as a potent inhibitor of multiple pathway-induced platelet aggregation

Author

Tsiailanis, Antonis D. Vrettos, I, Eirinaios Choleva, Maria and Kiriakidi, Sofia Ganai, Ab Majeed Patha, Tabasum Khan and Karpoormath, Rajshekhar Mavromoustakos, Thomas Fragopoulou, Elizabeth Tzakos, Andreas G. and Tsiailanis, Antonis D. Vrettos, I, Eirinaios Choleva, Maria and Kiriakidi, Sofia Ganai, Ab Majeed Patha, Tabasum Khan and Karpoormath, Rajshekhar Mavromoustakos, Thomas Fragopoulou, Elizabeth Tzakos, Andreas G.

Abstract

Despite the scientific progression in the prevention and treatment of cardiovascular diseases (CVDs) they remain the leading cause of mortality and disability worldwide. The classic treatment involves the simultaneous dosing of two antiplatelet drugs, aspirin and clopidogrel/prasugrel. However, besides drug resistance, severe side effects have been also manifested including acute bleeding and toxicity. Thus, new therapeutic agents with enhanced efficacy and diminished side effects are of importance. Towards this end, omega-3 (omega-3) fatty acids have demonstrated potent efficacy against CVDs through inhibiting platelet aggregation that bears a pivotal role in atherothrombosis. Another factor that displays a critical role in the pathogenesis of cardiovascular diseases is the renin-angiotensin system (RAS), and especially the AT(1)R blocker losartan that has been reported to exert antiplatelet activity mediated by this receptor. Along these lines, we envisaged developing a molecular hybrid consisted of docosahexaenoic acid (omega-3 fatty acid) and losartan, that could exert a notable antiplatelet effect against CVDs. The design and synthesis of the new DHA-losartan hybrid, designated DHA-L, bestowed with the additive properties of the parent compounds, is reported. In silico studies were first exploited to validate the potential of DHA-L to retain losartan's ability to bind AT(1)R. The antiplatelet activity of DHA-L was evaluated against in vitro platelet aggregation induced by several platelet agonists. Notably, the hybrid illustrated a pleiotropic antiplatelet profile inhibiting platelet aggregation through multiple platelet activation pathways including P2Y12, PAR-1 (Protease-Activated Receptor-1), PAF (Platelet Activating Factor), COX-1 (cyclooxygenase-1) and collagen receptors. The stability of DHA-L in human plasma and in a wide range of pH values was also evaluated over time using an HPLC protocol. The hybridization approach described herein could pave th

35. Molecular investigation of artificial and natural sweeteners as potential anti-inflammatory agents

Author

Chontzopoulou, Eleni Papaemmanouil, Christina D. and Chatziathanasiadou, V, Maria Kolokouris, Dimitrios Kiriakidi, Sofia Konstantinidi, Athina Gerogianni, Ioanna Tselios, Theodore Kostakis, Ioannis K. Chrysina, Evangelia D. and Hadjipavlou-Litina, Dimitra Tzeli, Demeter Tzakos, Andreas G. and Mavromoustakos, Thomas and Chontzopoulou, Eleni Papaemmanouil, Christina D. and Chatziathanasiadou, V, Maria Kolokouris, Dimitrios Kiriakidi, Sofia Konstantinidi, Athina Gerogianni, Ioanna Tselios, Theodore Kostakis, Ioannis K. Chrysina, Evangelia D. and Hadjipavlou-Litina, Dimitra Tzeli, Demeter Tzakos, Andreas G. and Mavromoustakos, Thomas

Abstract

Repurposing existing drugs, as well as natural and artificial sweeteners for novel therapeutic indications could speed up the drug discovery process since numerous associated risks and costs for drug development can be surpassed. In this study, natural and artificial sweeteners have been evaluated by in silico and experimental studies for their potency to inhibit lipoxygenase enzyme, an enzyme participating in the inflammation pathway. A variety of different methods pinpointed that aspartame inhibits the lipoxygenase isoform 1 (LOX-1). In particular, “LOX-aspartame” complex, that was predicted by docking studies, was further evaluated by Molecular Dynamics (MD) simulations in order to assess the stability of the complex. The binding energy of the complex has been calculated after MD simulations using Molecular Mechanics/Generalized Born Surface Area (MM/GBSA) method. Furthermore, Quantum Mechanics/Molecular Mechanics (QM/MM) calculations have been applied for geometry optimization of the “enzyme-ligand” complex. After having fully characterized the “LOX-aspartame” complex in silico, followed in vitro biological assays confirmed that aspartame inhibits LOX-1 (IC50=50 +/- 3.0 mu M) and blocks its biological response. The atomic details of aspartame’s interaction profile with LOX-1 were revealed through Saturation Transfer Difference (STD) NMR (Nuclear Magnetic Resonance). Finally, aspartame was also tested with Molecular Docking and Molecular Dynamics studies for its potent binding to a number of different LOX isoforms of many organisms, including human. The in silico methods indicated that aspartame could serve as a novel starting point for drug design against LOX enzyme. Communicated by Ramaswamy H. Sarma

36. Exploring Hypertension: The Role of AT1 Receptors, Sartans, and Lipid Bilayers.

Author

Georgiou N, Chontzopoulou E, Routsi EA, Stavrakaki IG, Petsas E, Zoupanou N, Kakava MG, Tzeli D, Mavromoustakos T, and Kiriakidi S

Abstract

The rational design of AT1 receptor antagonists represents a pivotal approach in the development of therapeutic agents targeting cardiovascular pathophysiology. Sartans, a class of compounds engineered to inhibit the binding and activation of Angiotensin II on the AT1 receptor, have demonstrated significant clinical efficacy. This review explores the multifaceted role of sartans in mitigating hypertension and related complications. We highlight the integration of crystallography, computational simulations, and NMR spectroscopy to elucidate sartan-AT1 receptor interactions, providing a foundation for the next-generation antagonist design. The review also delves into the challenges posed by the high lipophilicity and suboptimal bioavailability of sartans, emphasizing advancements in nanotechnology and novel drug delivery systems. Additionally, we discuss the impact of lipid bilayers on the AT1 receptor conformation and drug binding, underscoring the importance of the lipidic environment in receptor-drug interactions. We suggest that optimizing drug design to account for these factors could enhance the therapeutic potential of AT1 receptor antagonists, paving the way for improved cardiovascular health outcomes., Competing Interests: The authors declare no competing financial interest., (© 2024 The Authors. Published by American Chemical Society.)

Published
2024
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37. Study of Candesartan Cilexetil: 2-Hydroxypropyl-β-Cyclodextrin Interactions: A Computational Approach Using Steered Molecular Dynamics Simulations.

Author

Kiriakidi S and Mavromoustakos T

Subjects
Solubility, 2-Hydroxypropyl-beta-cyclodextrin chemistry, Benzimidazoles chemistry, Biphenyl Compounds chemistry, Models, Chemical, Molecular Dynamics Simulation, Tetrazoles chemistry
Abstract

Cyclodextrins (CDs) are widely used in the pharmaceutical industry as transporters of lipophilic drugs due to their amphiphilic nature. The detailed study of the molecular interactions of drug complexes with CDs is very important in designing the best formulation for the transportation of lipophilic drugs. The drug: CD binding should be strong enough so that the complex is stable in the aquatic environment of the extracellular fluids, but also not very strong in order for the drug to be capable for being released in the proximity of the target receptor. In a recent study, we investigated the ΔG of binding between the commercially available, nontoxic 2-hydroxypropyl-β-cyclodextrin (2-HP-B-CD) and the antihypertensive drug candesartan cilexetil (CC), with the use of steered (or biased) molecular dynamics (sMD) and umbrella sampling method. This chapter describes comprehensively how to perform sMD and umbrella sampling in order to calculate the ΔG binding of CC to the 2-HP-B-CD.

Published
2021
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38. 2D DOSY NMR: A Valuable Tool to Confirm the Complexation in Drug Delivery Systems.

Author

Chatzigiannis CM, Kiriakidi S, Tzakos AG, and Mavromoustakos T

Subjects
2-Hydroxypropyl-beta-cyclodextrin chemistry, Drug Carriers chemistry, Nuclear Magnetic Resonance, Biomolecular, Temozolomide chemistry
Abstract

Many bioactive substances face the problem of limited bioavailability, mainly due to low aqueous solubility and poor metabolic stability. Their complexation with drug delivery systems offers a more optimum pharmacological profile. Some of these drug delivery systems that have promising potential form complexes with bioactive compounds such as cyclodextrins and calixarenes. The monitoring of the success and the type of the complexation are of great importance and two-dimensional diffusion-ordered NMR spectroscopy (2D DOSY) is a valuable tool for the studying of these complexes and described as "NMR chromatography." Herein we report the procedure for the complexation of the natural product quercetin in 2-hydroxypropyl-β-cyclodextrin and the anticancer drug temozolomide in p-sulfonatocalix[4]arene and the determination of the complexation with 2D DOSY spectroscopy.

Published
2021
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