-
Something wrong with this record ?
Diurnal variation in cholesterol 7α-hydroxylase activity is determined by the -203A>C polymorphism of the CYP7A1 gene
M. Vlachova, T. Blahova, V. Lanska, M. Leníček, J. Pitha, L. Vítek, J. Kovar,
Language English Country Croatia
Document type Journal Article
Grant support
NT13151
MZ0
CEP Register
NLK
Directory of Open Access Journals
from 2001
Free Medical Journals
from 1996
Freely Accessible Science Journals
from 1996
PubMed Central
from 2006
Europe PubMed Central
from 2006
Medline Complete (EBSCOhost)
from 2005-02-01
ROAD: Directory of Open Access Scholarly Resources
from 1997
- MeSH
- Enzyme Activation MeSH
- Cholestenones blood MeSH
- Cholesterol 7-alpha-Hydroxylase genetics metabolism MeSH
- Cholesterol blood MeSH
- Circadian Rhythm physiology MeSH
- Adult MeSH
- Humans MeSH
- Area Under Curve MeSH
- Polymorphism, Genetic * MeSH
- Promoter Regions, Genetic MeSH
- Up-Regulation MeSH
- Bile Acids and Salts biosynthesis MeSH
- Check Tag
- Adult MeSH
- Humans MeSH
- Male MeSH
- Publication type
- Journal Article MeSH
AIM: To determine whether the promoter polymorphism -203A>C of cholesterol-7α-hydroxylase encoding gene (CYP7A1) affects diurnal variation in CYP7A1 enzyme activity. METHODS: The study included 16 healthy male volunteers - 8 homozygous for -203A and 8 homozygous for the -203C allele of CYP7A1. Three 15-hour examinations (from 7am to 10pm) were carried out for each of the participants: after one-day treatment with cholestyramine; after one-day treatment with chenodeoxycholic acid (CDCA); and a control examination without any treatment. The plasma concentration of 7α-hydroxy-4-cholesten-3-one (C4), a marker of CYP7A1 activity, was determined in all the experiments at 90-min intervals. RESULTS: CYP7A1 activity was up-regulated after treatment with cholestyramine and suppressed after treatment with CDCA. There were no differences between -203A and -203C allele carriers in the response of enzyme activity to both drugs. In the control experiment, -203A allele carriers displayed diurnal variation in enzyme activity, whereas CYP7A1 activity did not change in -203C allele carriers. These results were confirmed by modeling the dynamics of C4 using polynomial regression. CONCLUSION: The promoter polymorphism of the CYP7A1 gene has a pronounced impact on diurnal variation in CYP7A1 activity.
References provided by Crossref.org
- 000
- 00000naa a2200000 a 4500
- 001
- bmc17013925
- 003
- CZ-PrNML
- 005
- 20190902135433.0
- 007
- ta
- 008
- 170413s2016 ci f 000 0|eng||
- 009
- AR
- 024 7_
- $a 10.3325/cmj.2016.57.111 $2 doi
- 035 __
- $a (PubMed)27106353
- 040 __
- $a ABA008 $b cze $d ABA008 $e AACR2
- 041 0_
- $a eng
- 044 __
- $a ci
- 100 1_
- $a Vlachova, Miluše
- 245 10
- $a Diurnal variation in cholesterol 7α-hydroxylase activity is determined by the -203A>C polymorphism of the CYP7A1 gene / $c M. Vlachova, T. Blahova, V. Lanska, M. Leníček, J. Pitha, L. Vítek, J. Kovar,
- 520 9_
- $a AIM: To determine whether the promoter polymorphism -203A>C of cholesterol-7α-hydroxylase encoding gene (CYP7A1) affects diurnal variation in CYP7A1 enzyme activity. METHODS: The study included 16 healthy male volunteers - 8 homozygous for -203A and 8 homozygous for the -203C allele of CYP7A1. Three 15-hour examinations (from 7am to 10pm) were carried out for each of the participants: after one-day treatment with cholestyramine; after one-day treatment with chenodeoxycholic acid (CDCA); and a control examination without any treatment. The plasma concentration of 7α-hydroxy-4-cholesten-3-one (C4), a marker of CYP7A1 activity, was determined in all the experiments at 90-min intervals. RESULTS: CYP7A1 activity was up-regulated after treatment with cholestyramine and suppressed after treatment with CDCA. There were no differences between -203A and -203C allele carriers in the response of enzyme activity to both drugs. In the control experiment, -203A allele carriers displayed diurnal variation in enzyme activity, whereas CYP7A1 activity did not change in -203C allele carriers. These results were confirmed by modeling the dynamics of C4 using polynomial regression. CONCLUSION: The promoter polymorphism of the CYP7A1 gene has a pronounced impact on diurnal variation in CYP7A1 activity.
- 650 _2
- $a dospělí $7 D000328
- 650 _2
- $a plocha pod křivkou $7 D019540
- 650 _2
- $a žlučové kyseliny a soli $x biosyntéza $7 D001647
- 650 _2
- $a cholestenony $x krev $7 D002783
- 650 _2
- $a cholesterol $x krev $7 D002784
- 650 _2
- $a cholesterol-7-alfa-hydroxylasa $x genetika $x metabolismus $7 D002790
- 650 _2
- $a cirkadiánní rytmus $x fyziologie $7 D002940
- 650 _2
- $a aktivace enzymů $7 D004789
- 650 _2
- $a lidé $7 D006801
- 650 _2
- $a mužské pohlaví $7 D008297
- 650 12
- $a polymorfismus genetický $7 D011110
- 650 _2
- $a promotorové oblasti (genetika) $7 D011401
- 650 _2
- $a upregulace $7 D015854
- 655 _2
- $a časopisecké články $7 D016428
- 700 1_
- $a Blahová, T. $u Tereza Blahova, Laboratory for Atherosclerosis Research, Institute for Clinical and Experimental Medicine, Vídenska 1958-9, 140 21 Prague 4, Czech Republic, tereza.blahova@ikem.cz. $7 _AN089253
- 700 1_
- $a Lánská, Věra $7 xx0062305
- 700 1_
- $a Leníček, Martin $7 xx0097551
- 700 1_
- $a Piťha, Jan, $d 1964- $7 mzk2003187379
- 700 1_
- $a Vítek, Libor, $d 1969- $7 xx0035071
- 700 1_
- $a Kovář, Jan, $d 1952- $7 jn20040114001
- 773 0_
- $w MED00173528 $t Croatian medical journal $x 1332-8166 $g Roč. 57, č. 2 (2016), s. 111-117
- 856 41
- $u https://pubmed.ncbi.nlm.nih.gov/27106353 $y Pubmed
- 910 __
- $a ABA008 $b sig $c sign $y a $z 0
- 990 __
- $a 20170413 $b ABA008
- 991 __
- $a 20190902135801 $b ABA008
- 999 __
- $a ok $b bmc $g 1200390 $s 974703
- BAS __
- $a 3
- BAS __
- $a PreBMC
- BMC __
- $a 2016 $b 57 $c 2 $d 111-117 $i 1332-8166 $m Croatian medical journal $n Croat Med J $x MED00173528
- GRA __
- $a NT13151 $p MZ0
- LZP __
- $a Pubmed-20170413
