• Je něco špatně v tomto záznamu ?

Polychlorinated environmental toxicants affect sphingolipid metabolism during neurogenesis in vitro

J. Slováčková, J. Slavík, P. Kulich, J. Večeřa, O. Kováč, H. Paculová, N. Straková, R. Fedr, JP. Silva, F. Carvalho, M. Machala, J. Procházková

. 2021 ; 463 (-) : 152986. [pub] 20211007

Jazyk angličtina Země Irsko

Typ dokumentu srovnávací studie, časopisecké články, práce podpořená grantem

Perzistentní odkaz   https://www.medvik.cz/link/bmc22003371

Sphingolipids (SLs) are important signaling molecules and functional components of cellular membranes. Although SLs are known as crucial regulators of neural cell physiology and differentiation, modulations of SLs by environmental neurotoxicants in neural cells and their neuronal progeny have not yet been explored. In this study, we used in vitro models of differentiated neuron-like cells, which were repeatedly exposed during differentiation to model environmental toxicants, and we analyzed changes in sphingolipidome, cellular morphology and gene expression related to SL metabolism or neuronal differentiation. We compared these data with the results obtained in undifferentiated neural cells with progenitor-like features. As model polychlorinated organic pollutants, we used 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD), 3,3'-dichlorobiphenyl (PCB11) and 2,2',4,4',5,5'-hexachlorobiphenyl (PCB153). PCB153 revealed itself as the most prominent deregulator of SL metabolism and as potent toxicant during early phases of in vitro neurogenesis. TCDD exerted only minor changes in the levels of analysed lipid species, however, it significantly changed the rate of pro-neuronal differentiation and deregulated expression of neuronal markers during neurogenesis. PCB11 acted as a potent disruptor of in vitro neurogenesis, which induced significant alterations in SL metabolism and cellular morphology in both differentiated neuron-like models (differentiated NE4C and NG108-15 cells). We identified ceramide-1-phosphate, lactosylceramides and several glycosphingolipids to be the most sensitive SL species to exposure to polychlorinated pollutants. Additionally, we identified deregulation of several genes related to SL metabolism, which may be explored in future as potential markers of developmental neurotoxicity.

Citace poskytuje Crossref.org

000      
00000naa a2200000 a 4500
001      
bmc22003371
003      
CZ-PrNML
005      
20220127150313.0
007      
ta
008      
220113s2021 ie f 000 0|eng||
009      
AR
024    7_
$a 10.1016/j.tox.2021.152986 $2 doi
035    __
$a (PubMed)34627992
040    __
$a ABA008 $b cze $d ABA008 $e AACR2
041    0_
$a eng
044    __
$a ie
100    1_
$a Slováčková, Jana $u Department of Chemistry and Toxicology, Veterinary Research Institute, Hudcova 296/70, 62100, Brno, Czech Republic
245    10
$a Polychlorinated environmental toxicants affect sphingolipid metabolism during neurogenesis in vitro / $c J. Slováčková, J. Slavík, P. Kulich, J. Večeřa, O. Kováč, H. Paculová, N. Straková, R. Fedr, JP. Silva, F. Carvalho, M. Machala, J. Procházková
520    9_
$a Sphingolipids (SLs) are important signaling molecules and functional components of cellular membranes. Although SLs are known as crucial regulators of neural cell physiology and differentiation, modulations of SLs by environmental neurotoxicants in neural cells and their neuronal progeny have not yet been explored. In this study, we used in vitro models of differentiated neuron-like cells, which were repeatedly exposed during differentiation to model environmental toxicants, and we analyzed changes in sphingolipidome, cellular morphology and gene expression related to SL metabolism or neuronal differentiation. We compared these data with the results obtained in undifferentiated neural cells with progenitor-like features. As model polychlorinated organic pollutants, we used 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD), 3,3'-dichlorobiphenyl (PCB11) and 2,2',4,4',5,5'-hexachlorobiphenyl (PCB153). PCB153 revealed itself as the most prominent deregulator of SL metabolism and as potent toxicant during early phases of in vitro neurogenesis. TCDD exerted only minor changes in the levels of analysed lipid species, however, it significantly changed the rate of pro-neuronal differentiation and deregulated expression of neuronal markers during neurogenesis. PCB11 acted as a potent disruptor of in vitro neurogenesis, which induced significant alterations in SL metabolism and cellular morphology in both differentiated neuron-like models (differentiated NE4C and NG108-15 cells). We identified ceramide-1-phosphate, lactosylceramides and several glycosphingolipids to be the most sensitive SL species to exposure to polychlorinated pollutants. Additionally, we identified deregulation of several genes related to SL metabolism, which may be explored in future as potential markers of developmental neurotoxicity.
650    _2
$a zvířata $7 D000818
650    _2
$a buněčná diferenciace $x účinky léků $7 D002454
650    _2
$a buněčné linie $7 D002460
650    _2
$a látky znečišťující životní prostředí $x toxicita $7 D004785
650    _2
$a neurogeneze $x účinky léků $7 D055495
650    _2
$a neurony $x účinky léků $x metabolismus $7 D009474
650    _2
$a neurotoxické syndromy $x etiologie $x genetika $7 D020258
650    _2
$a polychlorované bifenyly $x farmakologie $x toxicita $7 D011078
650    _2
$a polychlorované dibenzodioxiny $x toxicita $7 D000072317
650    _2
$a sfingolipidy $x metabolismus $7 D013107
655    _2
$a srovnávací studie $7 D003160
655    _2
$a časopisecké články $7 D016428
655    _2
$a práce podpořená grantem $7 D013485
700    1_
$a Slavík, Josef $u Department of Chemistry and Toxicology, Veterinary Research Institute, Hudcova 296/70, 62100, Brno, Czech Republic
700    1_
$a Kulich, Pavel $u Department of Chemistry and Toxicology, Veterinary Research Institute, Hudcova 296/70, 62100, Brno, Czech Republic
700    1_
$a Večeřa, Josef $u Department of Chemistry and Toxicology, Veterinary Research Institute, Hudcova 296/70, 62100, Brno, Czech Republic
700    1_
$a Kováč, Ondrej $u Department of Chemistry and Toxicology, Veterinary Research Institute, Hudcova 296/70, 62100, Brno, Czech Republic
700    1_
$a Paculová, Hana $u Department of Chemistry and Toxicology, Veterinary Research Institute, Hudcova 296/70, 62100, Brno, Czech Republic
700    1_
$a Straková, Nicol $u Department of Chemistry and Toxicology, Veterinary Research Institute, Hudcova 296/70, 62100, Brno, Czech Republic
700    1_
$a Fedr, Radek $u Department of Cytokinetics, Institute of Biophysics of the Czech Academy of Sciences, Královopolská 135, 61265, Brno, Czech Republic
700    1_
$a Silva, João Pedro $u Laboratory of Toxicology, Department of Biological Sciences, Faculty of Pharmacy, University of Porto, Portugal
700    1_
$a Carvalho, Félix $u Laboratory of Toxicology, Department of Biological Sciences, Faculty of Pharmacy, University of Porto, Portugal
700    1_
$a Machala, Miroslav $u Department of Chemistry and Toxicology, Veterinary Research Institute, Hudcova 296/70, 62100, Brno, Czech Republic. Electronic address: machala@vri.cz
700    1_
$a Procházková, Jiřina $u Department of Chemistry and Toxicology, Veterinary Research Institute, Hudcova 296/70, 62100, Brno, Czech Republic; Department of Cytokinetics, Institute of Biophysics of the Czech Academy of Sciences, Královopolská 135, 61265, Brno, Czech Republic. Electronic address: prochazkova@ibp.cz
773    0_
$w MED00004533 $t Toxicology $x 1879-3185 $g Roč. 463, č. - (2021), s. 152986
856    41
$u https://pubmed.ncbi.nlm.nih.gov/34627992 $y Pubmed
910    __
$a ABA008 $b sig $c sign $y p $z 0
990    __
$a 20220113 $b ABA008
991    __
$a 20220127150309 $b ABA008
999    __
$a ok $b bmc $g 1750975 $s 1154520
BAS    __
$a 3
BAS    __
$a PreBMC
BMC    __
$a 2021 $b 463 $c - $d 152986 $e 20211007 $i 1879-3185 $m Toxicology $n Toxicology $x MED00004533
LZP    __
$a Pubmed-20220113

Najít záznam

Citační ukazatele

Možnosti archivace