Your search keyword '"Aleksander Canko"' showing total 7 results

1. Existence of Quantum Pharmacology in Sartans: Evidence in Isolated Rabbit Iliac Arteries

Author

Laura Kate Gadanec, Jordan Swiderski, Vasso Apostolopoulos, Kostantinos Kelaidonis, Veroniki P. Vidali, Aleksander Canko, Graham J. Moore, John M. Matsoukas, and Anthony Zulli

Subjects

angiotensin II, angiotensin II receptor blockers, bisartans, inverse agonism, sartans, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Quantum pharmacology introduces theoretical models to describe the possibility of ultra-high dilutions to produce biological effects, which may help to explain the placebo effect observed in hypertensive clinical trials. To determine this within physiology and to evaluate novel ARBs, we tested the ability of known angiotensin II receptor blockers (ARBs) (candesartan and telmisartan) used to treat hypertension and other cardiovascular diseases, as well as novel ARBs (benzimidazole-N-biphenyl tetrazole (ACC519T), benzimidazole-bis-N,N′-biphenyl tetrazole (ACC519T(2)) and 4-butyl-N,N0-bis[[20-2Htetrazol-5-yl)biphenyl-4-yl]methyl)imidazolium bromide (BV6(K+)2), and nirmatrelvir (the active ingredient in Paxlovid) to modulate vascular contraction in iliac rings from healthy male New Zealand White rabbits in responses to various vasopressors (angiotensin A, angiotensin II and phenylephrine). Additionally, the hemodynamic effect of ACC519T and telmisartan on mean arterial pressure in conscious rabbits was determined, while the ex vivo ability of BV6(K+)2 to activate angiotensin-converting enzyme-2 (ACE2) was also investigated. We show that commercially available and novel ARBs can modulate contraction responses at ultra-high dilutions to different vasopressors. ACC519T produced a dose-dependent reduction in rabbit mean arterial pressure while BV6(K+)2 significantly increased ACE2 metabolism. The ability of ARBs to inhibit contraction responses even at ultra-low concentrations provides evidence of the existence of quantum pharmacology. Furthermore, the ability of ACC519T and BV6(K+)2 to modulate blood pressure and ACE2 activity, respectively, indicates their therapeutic potential against hypertension.

Published

2023

2. Synthesis of Novel Pyrazolo[3,4-b]pyridines with Affinity for β-Amyloid Plaques

Author

Veroniki P. Vidali, Georgia Nigianni, Georgia D. Athanassopoulou, Aleksander Canko, Barbara Mavroidi, Dimitris Matiadis, Maria Pelecanou, and Marina Sagnou

Subjects

pyrazolo[3,4-b]pyridines, β-amyloid plaque probes, AD diagnosis, Inorganic chemistry, QD146-197

Abstract

Three novel pyrazolo[3,4-b]pyridines were synthesized via the cyclization of 5-amino-1-phenylpyrazole with the corresponding unsaturated ketone in the catalytic presence of ZrCl4. The ketones were afforded by modifying a stabilized ylide facilitated Wittig reaction in fairly high yields. The novel compounds exhibited exciting photophysical properties with the dimethylamine phenyl-bearing pyrazolopyridine showing exceptionally large Stoke’s shifts. Finally, both the dimethylamino- and the pyrene-substituted compounds demonstrated high and selective binding to amyloid plaques of Alzheimer’s disease (AD) patient brain slices upon fluorescent confocal microscopy observation. These results reveal the potential application of pyrazolo[3,4-b]pyridines in the development of AD amyloid plaque probes of various modalities for AD diagnosis.

Published

2022

3. Synthesis and Biological Evaluation of Hydroxylated Monocarbonyl Curcumin Derivatives as Potential Inducers of Neprilysin Activity

Author

Dimitris Matiadis, See-Ting Ng, Eric H.-L. Chen, Georgia Nigianni, Veroniki P. Vidali, Aleksander Canko, Rita P.-Y. Chen, and Marina Sagnou

Subjects

monocarbonyl curcumin derivatives, neprilysin, amyloid cleavage, Aβ amyloid peptide, Alzheimer’s disease, Biology (General), QH301-705.5

Abstract

Background: Alzheimer’s disease (AD) involves impairment of Aβ clearance. Neprilysin (NEP) is the most efficient Aβ peptidase. Enhancement of the activity or expression of NEP may provide a prominent therapeutic strategy against AD. Aims: Ten hydroxylated monocarbonyl curcumin derivatives were designed, synthesized and evaluated for their NEP upregulating potential using sensitive fluorescence-based Aβ digestion and inhibition assays. Results: Compound 4 was the most active one, resulting in a 50% increase in Aβ cleavage activity. Cyclohexanone-bearing derivatives exhibited higher activity enhancement compared to their acetone counterparts. Inhibition experiments with the NEP-specific inhibitor thiorphan resulted in dramatic cleavage reduction. Conclusion: The increased Aβ cleavage activity and the ease of synthesis of 4 renders it an extremely attractive lead compound.

Published

2021

4. First total synthesis of type II abyssomicins: (±)-abyssomicin 2 and (±)-neoabyssomicin B

Author

Aleksander Canko, Georgia D. Athanassopoulou, Vassilis Psycharis, Catherine P. Raptopoulou, Julie M. Herniman, Vasileios Mouchtouris, Angeliki Sofia Foscolos, Elias A. Couladouros, and Veroniki P. Vidali

Subjects

Organic Chemistry, Physical and Theoretical Chemistry, Biochemistry

Abstract

The intramolecular Diels-Alder reaction (IMDA) of a butenolide derivative, as an entry to the type II abyssomicin scaffold, and the total synthesis of (±)-abyssomicin 2 and (±)-neoabyssomicin B are reported for the first time. A facile route to the IMDA precursor, the formation of a type I intermediate and two paths to (±)-neoabyssomicin B are also discussed.

Published

2023

5. An Improved Biomimetic Formal Synthesis of Abyssomicin C and atrop -Abyssomicin C

Author

Aleksander Canko, Angelos D. Peroulias, Emmanuel A. Bouzas, Julie Herniman, Veroniki P. Vidali, Evangelos T. Georgas, and Elias A. Couladouros

Subjects

Formal synthesis, Chemistry, Stereochemistry, Biomimetic synthesis, Organic Chemistry, Abyssomicin C, Physical and Theoretical Chemistry, Atrop-abyssomicin C, Cycloaddition

Published

2020

6. Synthesis and Biological Evaluation of Hydroxylated Monocarbonyl Curcumin Derivatives as Potential Inducers of Neprilysin Activity

Author

Veroniki P. Vidali, Aleksander Canko, See-Ting Ng, Georgia Nigianni, Marina Sagnou, Dimitris Matiadis, Eric H.-L. Chen, and Rita P.-Y. Chen

Subjects

QH301-705.5, Medicine (miscellaneous), Cleavage (embryo), General Biochemistry, Genetics and Molecular Biology, Article, neprilysin, 03 medical and health sciences, chemistry.chemical_compound, Aβ amyloid peptide, 0302 clinical medicine, Inducer, Biology (General), Neprilysin, monocarbonyl curcumin derivatives, 030304 developmental biology, Biological evaluation, 0303 health sciences, Chemistry, fungi, Thiorphan, Neprilysin activity, Biochemistry, Curcumin, Lead compound, amyloid cleavage, Alzheimer’s disease, 030217 neurology & neurosurgery

Abstract

Background: Alzheimer’s disease (AD) involves impairment of Aβ clearance. Neprilysin (NEP) is the most efficient Aβ peptidase. Enhancement of the activity or expression of NEP may provide a prominent therapeutic strategy against AD. Aims: Ten hydroxylated monocarbonyl curcumin derivatives were designed, synthesized and evaluated for their NEP upregulating potential using sensitive fluorescence-based Aβ digestion and inhibition assays. Results: Compound 4 was the most active one, resulting in a 50% increase in Aβ cleavage activity. Cyclohexanone-bearing derivatives exhibited higher activity enhancement compared to their acetone counterparts. Inhibition experiments with the NEP-specific inhibitor thiorphan resulted in dramatic cleavage reduction. Conclusion: The increased Aβ cleavage activity and the ease of synthesis of 4 renders it an extremely attractive lead compound.

Published

2021

7. Cell-active carbazole derivatives as inhibitors of the zika virus protease

Author

Gerasimos A. Rassias, Subhash G. Vasudevan, Sai Wang, Aleksander Canko, Shu Ann Chan, Chin Piaw Gwee, Minos-Timotheos Matsoukas, Entzy Kaplanai, Vasiliki Zogali, Crystall M.D. Swarbrick, Dahai Luo, Julien Lescar, Dimitrios Kiousis, Kitti Wing Ki Chan, Lee Kong Chian School of Medicine (LKCMedicine), and School of Biological Sciences

Subjects

Models, Molecular, Proteases, Cell Survival, viruses, medicine.medical_treatment, Carbazoles, Microbial Sensitivity Tests, Dengue virus, Viral Nonstructural Proteins, medicine.disease_cause, 01 natural sciences, Antiviral Agents, Zika virus, 03 medical and health sciences, Flaviviridae, Structure-Activity Relationship, Zika, Cell Line, Tumor, Drug Discovery, medicine, Humans, Protease Inhibitors, 030304 developmental biology, Pharmacology, 0303 health sciences, NS3, Protease, biology, Dose-Response Relationship, Drug, Molecular Structure, 010405 organic chemistry, Chemistry, Flavivirus, Organic Chemistry, Serine Endopeptidases, Rational design, Biological sciences [Science], General Medicine, Zika Virus, biology.organism_classification, Virology, 0104 chemical sciences, RNA Helicases

Abstract

Zika virus (ZIKV) infection recently resulted in an international health emergency the Americas in and despite its high profile there is currently no approved treatment for ZIKV infection with millions of people being at risk. ZIKV is a member of Flaviviridae family which includes prominent members such as dengue virus (DENV) and West Nile virus (WNV). One of the best validated targets for developing anti-flaviviral treatment for DENV and WNV infection is the NS2B/NS3 protease. However the inhibitors reported to date have shown limited promise for further clinical development largely due to poor cellular activity. Prompted by the conserved nature of the viral NS2B/NS3 protease across flaviviruses, we envisaged that small molecule inhibitors of the ZIKVpro may be developed by applying rational design on previously reported scaffolds with demonstrated activity against other flaviviral proteases. Starting with an earlier WNVpro hit we performed a scaffold hopping exercise and discovered that certain carbazole derivatives bearing amidine groups possessed submicromolar potency and significant cellular activity against ZIKV. We successfully addressed various issues with the synthesis of novel N-substituted carbazole-based amidines thus permitting a targeted SAR campaign. The in vitro biochemical and cell-based inhibitory profiles exhibited by the lead molecule described in this work (ZIKVpro IC50 0.52 μM, EC50 1.25 μM), is among the best reported to date. Furthermore, these molecules possess capacity for further optimization of pharmacokinetics and may evolve to broad spectrum flaviviral protease inhibitors. National Research Foundation (NRF) The research was supported by National Medical Research Council grant NMRC/CBRG/0103/2016 (PI), National Research Foundation grant NRF2016NRF-CRP001-063 (Co-PI) to SGV.

Published

2019