Standard

Candidate SNP Markers of Atherosclerosis That May Significantly Change the Affinity of the TATA-Binding Protein for the Human Gene Promoters. / Ponomarenko, M. P.; Rasskazov, D. A.; Chadaeva, I. V. и др.

в: Russian Journal of Genetics, Том 55, № 9, 01.09.2019, стр. 1137-1151.

Результаты исследований: Научные публикации в периодических изданияхстатьяРецензирование

Harvard

Ponomarenko, MP, Rasskazov, DA, Chadaeva, IV, Sharypova, EB, Drachkova, IA, Ponomarenko, PM, Oshchepkova, EA, Savinkova, LK & Kolchanov, NA 2019, 'Candidate SNP Markers of Atherosclerosis That May Significantly Change the Affinity of the TATA-Binding Protein for the Human Gene Promoters', Russian Journal of Genetics, Том. 55, № 9, стр. 1137-1151. https://doi.org/10.1134/S1022795419090114

APA

Ponomarenko, M. P., Rasskazov, D. A., Chadaeva, I. V., Sharypova, E. B., Drachkova, I. A., Ponomarenko, P. M., Oshchepkova, E. A., Savinkova, L. K., & Kolchanov, N. A. (2019). Candidate SNP Markers of Atherosclerosis That May Significantly Change the Affinity of the TATA-Binding Protein for the Human Gene Promoters. Russian Journal of Genetics, 55(9), 1137-1151. https://doi.org/10.1134/S1022795419090114

Vancouver

Ponomarenko MP, Rasskazov DA, Chadaeva IV, Sharypova EB, Drachkova IA, Ponomarenko PM и др. Candidate SNP Markers of Atherosclerosis That May Significantly Change the Affinity of the TATA-Binding Protein for the Human Gene Promoters. Russian Journal of Genetics. 2019 сент. 1;55(9):1137-1151. doi: 10.1134/S1022795419090114

Author

Ponomarenko, M. P. ; Rasskazov, D. A. ; Chadaeva, I. V. и др. / Candidate SNP Markers of Atherosclerosis That May Significantly Change the Affinity of the TATA-Binding Protein for the Human Gene Promoters. в: Russian Journal of Genetics. 2019 ; Том 55, № 9. стр. 1137-1151.

BibTeX

@article{53b761874a1048fdaa11bf5cc7edd623,
title = "Candidate SNP Markers of Atherosclerosis That May Significantly Change the Affinity of the TATA-Binding Protein for the Human Gene Promoters",
abstract = "Atherosclerosis (AS) and AS-related pathologies such as coronary heart disease, myocardial infarction, angina pectoris, and stroke are the leading causes of death in the world. The atherogenesis can be influenced by many factors, in particular, overweight, hypertension, diabetes, hyperlipoproteinemia, and other diseases in anamnesis, as well as genetic predisposition, which may be due to single nucleotide polymorphisms (SNPs) in some cases. In this work, we studied only those regions of promoters of the human protein-coding genes where SNP markers of changes in the affinity of the TATA-binding protein (TBP) for these promoters have already been associated with the atherosclerosis-related pathologies. As a result, within the dbSNP database, we found those unannotated SNPs which change such affinity just as the known biomedical SNP markers do here (according to the predictions made by our Web service SNP_TATA_Z-tester, http://wwwmgs.bionet.nsc.ru/cgi-bin/mgs/tatascan_fox/start.pl). For example, the known SNP marker rs35036378 of the high risks of the primary pT1 tumor reduces the TBP affinity for the ESR2 gene promoter and, thus, the estrogen receptor β abundancy in blood, which is a known physiological marker of calcification of blood vessels in atherogenesis. Near this known SNP marker, we found an unannotated SNP rs766797386, which can also reduce the TBP affinity for the same promoter and, thus, decrease the abundance of the estrogen receptor β in blood. Thus, we propose rs766797386 as a candidate SNP marker for accelerated atherogenesis due to calcification of blood vessels. The possibility of using a diet of natural food with high abundance of calcium (Ca), which is recommended by nutritionists to slow down calcification in the case when individuals have SNP markers of accelerated calcification, is discussed in contrast to the use of Ca-enriched nutritional supplements that can cause the opposite effect. In the same way, a total of 33 candidate SNP markers were predicted and discussed to accelerate or slow down atherogenesis. After clinical verification, the candidate SNP markers predicted by this work can help those who would like to slow down atherogenesis through lifestyle corrections using their genome sequencing data.",
keywords = "atherosclerosis, promoter, single nucleotide polymorphism (SNP), TATA-binding protein (TBP), TBP-binding site (TATA box), MATRIX METALLOPROTEINASE-12, BOX POLYMORPHISMS, TRANSCRIPTION, DEFICIENCY, HUMAN HEREDITARY-DISEASES, DNA, NITRIC-OXIDE, CELL, EXPRESSION, PROGRESSION",
author = "Ponomarenko, {M. P.} and Rasskazov, {D. A.} and Chadaeva, {I. V.} and Sharypova, {E. B.} and Drachkova, {I. A.} and Ponomarenko, {P. M.} and Oshchepkova, {E. A.} and Savinkova, {L. K.} and Kolchanov, {N. A.}",
year = "2019",
month = sep,
day = "1",
doi = "10.1134/S1022795419090114",
language = "English",
volume = "55",
pages = "1137--1151",
journal = "Russian Journal of Genetics",
issn = "1022-7954",
publisher = "PLEIADES PUBLISHING INC",
number = "9",

}

RIS

TY - JOUR

T1 - Candidate SNP Markers of Atherosclerosis That May Significantly Change the Affinity of the TATA-Binding Protein for the Human Gene Promoters

AU - Ponomarenko, M. P.

AU - Rasskazov, D. A.

AU - Chadaeva, I. V.

AU - Sharypova, E. B.

AU - Drachkova, I. A.

AU - Ponomarenko, P. M.

AU - Oshchepkova, E. A.

AU - Savinkova, L. K.

AU - Kolchanov, N. A.

PY - 2019/9/1

Y1 - 2019/9/1

N2 - Atherosclerosis (AS) and AS-related pathologies such as coronary heart disease, myocardial infarction, angina pectoris, and stroke are the leading causes of death in the world. The atherogenesis can be influenced by many factors, in particular, overweight, hypertension, diabetes, hyperlipoproteinemia, and other diseases in anamnesis, as well as genetic predisposition, which may be due to single nucleotide polymorphisms (SNPs) in some cases. In this work, we studied only those regions of promoters of the human protein-coding genes where SNP markers of changes in the affinity of the TATA-binding protein (TBP) for these promoters have already been associated with the atherosclerosis-related pathologies. As a result, within the dbSNP database, we found those unannotated SNPs which change such affinity just as the known biomedical SNP markers do here (according to the predictions made by our Web service SNP_TATA_Z-tester, http://wwwmgs.bionet.nsc.ru/cgi-bin/mgs/tatascan_fox/start.pl). For example, the known SNP marker rs35036378 of the high risks of the primary pT1 tumor reduces the TBP affinity for the ESR2 gene promoter and, thus, the estrogen receptor β abundancy in blood, which is a known physiological marker of calcification of blood vessels in atherogenesis. Near this known SNP marker, we found an unannotated SNP rs766797386, which can also reduce the TBP affinity for the same promoter and, thus, decrease the abundance of the estrogen receptor β in blood. Thus, we propose rs766797386 as a candidate SNP marker for accelerated atherogenesis due to calcification of blood vessels. The possibility of using a diet of natural food with high abundance of calcium (Ca), which is recommended by nutritionists to slow down calcification in the case when individuals have SNP markers of accelerated calcification, is discussed in contrast to the use of Ca-enriched nutritional supplements that can cause the opposite effect. In the same way, a total of 33 candidate SNP markers were predicted and discussed to accelerate or slow down atherogenesis. After clinical verification, the candidate SNP markers predicted by this work can help those who would like to slow down atherogenesis through lifestyle corrections using their genome sequencing data.

AB - Atherosclerosis (AS) and AS-related pathologies such as coronary heart disease, myocardial infarction, angina pectoris, and stroke are the leading causes of death in the world. The atherogenesis can be influenced by many factors, in particular, overweight, hypertension, diabetes, hyperlipoproteinemia, and other diseases in anamnesis, as well as genetic predisposition, which may be due to single nucleotide polymorphisms (SNPs) in some cases. In this work, we studied only those regions of promoters of the human protein-coding genes where SNP markers of changes in the affinity of the TATA-binding protein (TBP) for these promoters have already been associated with the atherosclerosis-related pathologies. As a result, within the dbSNP database, we found those unannotated SNPs which change such affinity just as the known biomedical SNP markers do here (according to the predictions made by our Web service SNP_TATA_Z-tester, http://wwwmgs.bionet.nsc.ru/cgi-bin/mgs/tatascan_fox/start.pl). For example, the known SNP marker rs35036378 of the high risks of the primary pT1 tumor reduces the TBP affinity for the ESR2 gene promoter and, thus, the estrogen receptor β abundancy in blood, which is a known physiological marker of calcification of blood vessels in atherogenesis. Near this known SNP marker, we found an unannotated SNP rs766797386, which can also reduce the TBP affinity for the same promoter and, thus, decrease the abundance of the estrogen receptor β in blood. Thus, we propose rs766797386 as a candidate SNP marker for accelerated atherogenesis due to calcification of blood vessels. The possibility of using a diet of natural food with high abundance of calcium (Ca), which is recommended by nutritionists to slow down calcification in the case when individuals have SNP markers of accelerated calcification, is discussed in contrast to the use of Ca-enriched nutritional supplements that can cause the opposite effect. In the same way, a total of 33 candidate SNP markers were predicted and discussed to accelerate or slow down atherogenesis. After clinical verification, the candidate SNP markers predicted by this work can help those who would like to slow down atherogenesis through lifestyle corrections using their genome sequencing data.

KW - atherosclerosis

KW - promoter

KW - single nucleotide polymorphism (SNP)

KW - TATA-binding protein (TBP)

KW - TBP-binding site (TATA box)

KW - MATRIX METALLOPROTEINASE-12

KW - BOX POLYMORPHISMS

KW - TRANSCRIPTION

KW - DEFICIENCY

KW - HUMAN HEREDITARY-DISEASES

KW - DNA

KW - NITRIC-OXIDE

KW - CELL

KW - EXPRESSION

KW - PROGRESSION

UR - http://www.scopus.com/inward/record.url?scp=85073226872&partnerID=8YFLogxK

U2 - 10.1134/S1022795419090114

DO - 10.1134/S1022795419090114

M3 - Article

AN - SCOPUS:85073226872

VL - 55

SP - 1137

EP - 1151

JO - Russian Journal of Genetics

JF - Russian Journal of Genetics

SN - 1022-7954

IS - 9

ER -

ID: 21857647