1,3-Thiazine, 1,2,3,4-Dithiadiazole, and Thiohydrazide Derivatives Affect Lipid Bilayer Properties and Ion-Permeable Pores Induced by Antifungals

1,3-Thiazine, 1,2,3,4-Dithiadiazole, and Thiohydrazide Derivatives Affect Lipid Bilayer Properties and Ion-Permeable Pores Induced by Antifungals

Over the past decade, thiazines, thiadiazoles, and thiohydrazides have attracted increasing attention due to their sedative, antimicrobial, antiviral, antifungal, and antitumor activities. The clinical efficacy of such drugs, as well as the possibility of developing resistance to antimicrobials, wil...

Full description

Bibliographic Details
Main Authors: Anastasiia A. Zakharova, Svetlana S. Efimova, Valeriy N. Yuskovets, Igor P. Yakovlev, Zara M. Sarkisyan, Olga S. Ostroumova
Format: Article
Language:English
Published: Frontiers Media S.A. 2020-06-01
Series:Frontiers in Cell and Developmental Biology
Subjects:
dithiadiazoles
thiazines
thiohydrazides
lipid bilayers
antifungals
ion-permeable pores
Online Access:https://www.frontiersin.org/article/10.3389/fcell.2020.00535/full
id doaj-cc2885f2fc1040e78ec244153f0b2990
record_format Article
spelling doaj-cc2885f2fc1040e78ec244153f0b29902020-11-25T03:50:17ZengFrontiers Media S.A.Frontiers in Cell and Developmental Biology2296-634X2020-06-01810.3389/fcell.2020.005355519011,3-Thiazine, 1,2,3,4-Dithiadiazole, and Thiohydrazide Derivatives Affect Lipid Bilayer Properties and Ion-Permeable Pores Induced by AntifungalsAnastasiia A. Zakharova0Svetlana S. Efimova1Valeriy N. Yuskovets2Igor P. Yakovlev3Zara M. Sarkisyan4Olga S. Ostroumova5Laboratory of Membrane and Ion Channel Modeling, Institute of Cytology, Russian Academy of Sciences, Saint Petersburg, RussiaLaboratory of Membrane and Ion Channel Modeling, Institute of Cytology, Russian Academy of Sciences, Saint Petersburg, RussiaDepartment of Organic Chemistry, Saint-Petersburg State Chemical Pharmaceutical University, Saint Petersburg, RussiaDepartment of Organic Chemistry, Saint-Petersburg State Chemical Pharmaceutical University, Saint Petersburg, RussiaDepartment of General and Medical Chemistry, Saint-Petersburg State Pediatric Medical University, Saint Petersburg, RussiaLaboratory of Membrane and Ion Channel Modeling, Institute of Cytology, Russian Academy of Sciences, Saint Petersburg, RussiaOver the past decade, thiazines, thiadiazoles, and thiohydrazides have attracted increasing attention due to their sedative, antimicrobial, antiviral, antifungal, and antitumor activities. The clinical efficacy of such drugs, as well as the possibility of developing resistance to antimicrobials, will depend on addressing a number of fundamental problems, including the role of membrane lipids during their interaction with plasma membranes. The effects of the eight 1,3- thiazine-, 1,2,3,4- dithiadiazole-, and thiohydrazide-related compounds on the physical properties of model lipid membranes and the effects on reconstituted ion channels induced by the polyene macrolide antimycotic nystatin and antifungal cyclic lipopeptides syringomycin E and fengycin were observed. We found that among the tested agents, the fluorine-containing compound N′-(3,5-difluorophenyl)-benzenecarbothiohydrazide (C6) was the most effective at increasing the electric barrier for anion permeation into the hydrophobic region of the membrane and reducing the conductance of anion-permeable syringomycin pores. A decrease in the membrane boundary potential with C6 adsorption also facilitated the immersion of positively charged syringomycin molecules into the lipid bilayer and increases the pore-forming ability of the lipopeptide. Using differential scanning microcalorimetry, we showed that C6 led to disordering of membrane lipids, possibly by potentiating positive curvature stress. Therefore, we used C6 as an agonist of antifungals forming the pores that are sensitive to membrane curvature stress and lipid packing, i.e., nystatin and fengycin. The dramatic increase in transmembrane current induced by syringomycin E, nystatin, and fengycin upon C6 treatment suggests its potential in combination therapy for treating invasive fungal infections.https://www.frontiersin.org/article/10.3389/fcell.2020.00535/fulldithiadiazolesthiazinesthiohydrazideslipid bilayersantifungalsion-permeable pores
collection DOAJ
language English
format Article
sources DOAJ
author Anastasiia A. Zakharova
Svetlana S. Efimova
Valeriy N. Yuskovets
Igor P. Yakovlev
Zara M. Sarkisyan
Olga S. Ostroumova
spellingShingle Anastasiia A. Zakharova
Svetlana S. Efimova
Valeriy N. Yuskovets
Igor P. Yakovlev
Zara M. Sarkisyan
Olga S. Ostroumova
1,3-Thiazine, 1,2,3,4-Dithiadiazole, and Thiohydrazide Derivatives Affect Lipid Bilayer Properties and Ion-Permeable Pores Induced by Antifungals
Frontiers in Cell and Developmental Biology
dithiadiazoles
thiazines
thiohydrazides
lipid bilayers
antifungals
ion-permeable pores
author_facet Anastasiia A. Zakharova
Svetlana S. Efimova
Valeriy N. Yuskovets
Igor P. Yakovlev
Zara M. Sarkisyan
Olga S. Ostroumova
author_sort Anastasiia A. Zakharova
title 1,3-Thiazine, 1,2,3,4-Dithiadiazole, and Thiohydrazide Derivatives Affect Lipid Bilayer Properties and Ion-Permeable Pores Induced by Antifungals
title_short 1,3-Thiazine, 1,2,3,4-Dithiadiazole, and Thiohydrazide Derivatives Affect Lipid Bilayer Properties and Ion-Permeable Pores Induced by Antifungals
title_full 1,3-Thiazine, 1,2,3,4-Dithiadiazole, and Thiohydrazide Derivatives Affect Lipid Bilayer Properties and Ion-Permeable Pores Induced by Antifungals
title_fullStr 1,3-Thiazine, 1,2,3,4-Dithiadiazole, and Thiohydrazide Derivatives Affect Lipid Bilayer Properties and Ion-Permeable Pores Induced by Antifungals
title_full_unstemmed 1,3-Thiazine, 1,2,3,4-Dithiadiazole, and Thiohydrazide Derivatives Affect Lipid Bilayer Properties and Ion-Permeable Pores Induced by Antifungals
title_sort 1,3-thiazine, 1,2,3,4-dithiadiazole, and thiohydrazide derivatives affect lipid bilayer properties and ion-permeable pores induced by antifungals
publisher Frontiers Media S.A.
series Frontiers in Cell and Developmental Biology
issn 2296-634X
publishDate 2020-06-01
description Over the past decade, thiazines, thiadiazoles, and thiohydrazides have attracted increasing attention due to their sedative, antimicrobial, antiviral, antifungal, and antitumor activities. The clinical efficacy of such drugs, as well as the possibility of developing resistance to antimicrobials, will depend on addressing a number of fundamental problems, including the role of membrane lipids during their interaction with plasma membranes. The effects of the eight 1,3- thiazine-, 1,2,3,4- dithiadiazole-, and thiohydrazide-related compounds on the physical properties of model lipid membranes and the effects on reconstituted ion channels induced by the polyene macrolide antimycotic nystatin and antifungal cyclic lipopeptides syringomycin E and fengycin were observed. We found that among the tested agents, the fluorine-containing compound N′-(3,5-difluorophenyl)-benzenecarbothiohydrazide (C6) was the most effective at increasing the electric barrier for anion permeation into the hydrophobic region of the membrane and reducing the conductance of anion-permeable syringomycin pores. A decrease in the membrane boundary potential with C6 adsorption also facilitated the immersion of positively charged syringomycin molecules into the lipid bilayer and increases the pore-forming ability of the lipopeptide. Using differential scanning microcalorimetry, we showed that C6 led to disordering of membrane lipids, possibly by potentiating positive curvature stress. Therefore, we used C6 as an agonist of antifungals forming the pores that are sensitive to membrane curvature stress and lipid packing, i.e., nystatin and fengycin. The dramatic increase in transmembrane current induced by syringomycin E, nystatin, and fengycin upon C6 treatment suggests its potential in combination therapy for treating invasive fungal infections.
topic dithiadiazoles
thiazines
thiohydrazides
lipid bilayers
antifungals
ion-permeable pores
url https://www.frontiersin.org/article/10.3389/fcell.2020.00535/full
work_keys_str_mv AT anastasiiaazakharova 13thiazine1234dithiadiazoleandthiohydrazidederivativesaffectlipidbilayerpropertiesandionpermeableporesinducedbyantifungals
AT svetlanasefimova 13thiazine1234dithiadiazoleandthiohydrazidederivativesaffectlipidbilayerpropertiesandionpermeableporesinducedbyantifungals
AT valeriynyuskovets 13thiazine1234dithiadiazoleandthiohydrazidederivativesaffectlipidbilayerpropertiesandionpermeableporesinducedbyantifungals
AT igorpyakovlev 13thiazine1234dithiadiazoleandthiohydrazidederivativesaffectlipidbilayerpropertiesandionpermeableporesinducedbyantifungals
AT zaramsarkisyan 13thiazine1234dithiadiazoleandthiohydrazidederivativesaffectlipidbilayerpropertiesandionpermeableporesinducedbyantifungals
AT olgasostroumova 13thiazine1234dithiadiazoleandthiohydrazidederivativesaffectlipidbilayerpropertiesandionpermeableporesinducedbyantifungals
_version_ 1724491277088587776

Similar Items