Standard

Association of the HTR2A T102C SNP with Weight Gain and Changes in Biochemical Markers in Patients Receiving Antipsychotics. / Tolmachev, Mikhail Yu.; Akhmetova, Liliya Sch; Shnayder, Natalia A.; Ershov, Evgeny E.; Bugorsky, Alexander V.; Kravtsov, Vladimir V.; Taraskina, Anastasia E.; Andreev, Boris V.; Yakhin, Kausar K.; Neznanov, Nikolay G.; Nasyrova, Regina F.

в: International Journal of Biomedicine , Том 8, № 3, 09.2018, стр. 186-191.

Результаты исследований: Научные публикации в периодических изданияхстатьяРецензирование

Harvard

Tolmachev, MY, Akhmetova, LS, Shnayder, NA, Ershov, EE, Bugorsky, AV, Kravtsov, VV, Taraskina, AE, Andreev, BV, Yakhin, KK, Neznanov, NG & Nasyrova, RF 2018, 'Association of the HTR2A T102C SNP with Weight Gain and Changes in Biochemical Markers in Patients Receiving Antipsychotics', International Journal of Biomedicine , Том. 8, № 3, стр. 186-191. https://doi.org/10.21103/Article8(3)_OA3

APA

Tolmachev, M. Y., Akhmetova, L. S., Shnayder, N. A., Ershov, E. E., Bugorsky, A. V., Kravtsov, V. V., Taraskina, A. E., Andreev, B. V., Yakhin, K. K., Neznanov, N. G., & Nasyrova, R. F. (2018). Association of the HTR2A T102C SNP with Weight Gain and Changes in Biochemical Markers in Patients Receiving Antipsychotics. International Journal of Biomedicine , 8(3), 186-191. https://doi.org/10.21103/Article8(3)_OA3

Vancouver

Tolmachev MY, Akhmetova LS, Shnayder NA, Ershov EE, Bugorsky AV, Kravtsov VV и пр. Association of the HTR2A T102C SNP with Weight Gain and Changes in Biochemical Markers in Patients Receiving Antipsychotics. International Journal of Biomedicine . 2018 Сент.;8(3):186-191. https://doi.org/10.21103/Article8(3)_OA3

Author

Tolmachev, Mikhail Yu. ; Akhmetova, Liliya Sch ; Shnayder, Natalia A. ; Ershov, Evgeny E. ; Bugorsky, Alexander V. ; Kravtsov, Vladimir V. ; Taraskina, Anastasia E. ; Andreev, Boris V. ; Yakhin, Kausar K. ; Neznanov, Nikolay G. ; Nasyrova, Regina F. / Association of the HTR2A T102C SNP with Weight Gain and Changes in Biochemical Markers in Patients Receiving Antipsychotics. в: International Journal of Biomedicine . 2018 ; Том 8, № 3. стр. 186-191.

BibTeX

@article{45b8639190904bce80f707228d94097d,
title = "Association of the HTR2A T102C SNP with Weight Gain and Changes in Biochemical Markers in Patients Receiving Antipsychotics",
abstract = "The purpose of our research was to study the association of the HTR2A T102C (rs6313) SNP with anthropometric and biochemical markers in patients treated with typical and atypical antipsychotics in monotherapy mode.Materials and methods: One hundred and seventeen white inpatients (95 men and 22 women) with F2 disorders (ICD-10, 1995) were enrolled in the study. All patients were divided into two groups by the antipsychotic class with which they were treated (Group 1 included 40 patients treated with typical antipsychotics; Group 2 included 77 patients treated with atypical antipsychotics) and two subgroups by weight change criteria during the study (Subgroup 1 included patients with weight change >6%; Subgroup 2 included patients with weight changeResults: There were no statistically significant differences in the distribution of genotypes of the HTR2A T102C (rs6313) SNP between Group 1 and Group 2 (P > 0.05). Kruskal-Wallis one-way analysis of variance between subgroups showed statistically significant differences between carbamide levels in the second visit in Group 2 (P = 0.02). We showed statistically significant differences between TT and CT genotypes of the HTR2A T102C SNP: carbamide level was greater in TT carriers (P = 0.02). The strength of associations and risks between alleles of the HTR2A T102C SNP and antipsychotic-induced weight change were as follows: ORC = 0.49; CIC [0.25; 0.95]; RRC = 0.58 CIC [0.35; 0.97]; ORT = 2.03; CIT [1.05; 3.94]; RRT = 1.7 CIT [1.02; 2.81].Conclusion: Our results of the pilot pharmacogenetic studies show an association of the T allele carriage of the HTR2A T102C (rs6313) SNP with risk of antipsychotic-induced weight gain. The continuation of this study and an increase in the sample size will allow establishing valid pharmacogenetic markers for the risk of antipsychotic-induced weight gain.",
keywords = "antipsychotics, single nucleotide polymorphism, serotonin receptor 2A, HTR2A gene, weight gain, 5-HT2A RECEPTOR GENE, SCHIZOPHRENIA, DRUGS, 2ND-GENERATION, POLYMORPHISM, INDIVIDUALS, PREDICTION, EXPRESSION, OBESITY, REGION",
author = "Tolmachev, {Mikhail Yu.} and Akhmetova, {Liliya Sch} and Shnayder, {Natalia A.} and Ershov, {Evgeny E.} and Bugorsky, {Alexander V.} and Kravtsov, {Vladimir V.} and Taraskina, {Anastasia E.} and Andreev, {Boris V.} and Yakhin, {Kausar K.} and Neznanov, {Nikolay G.} and Nasyrova, {Regina F.}",
year = "2018",
month = sep,
doi = "10.21103/Article8(3)_OA3",
language = "Английский",
volume = "8",
pages = "186--191",
journal = "International Journal of Biomedicine",
issn = "2158-0510",
publisher = "International Medical Research and Development Corporation",
number = "3",

}

RIS

TY - JOUR

T1 - Association of the HTR2A T102C SNP with Weight Gain and Changes in Biochemical Markers in Patients Receiving Antipsychotics

AU - Tolmachev, Mikhail Yu.

AU - Akhmetova, Liliya Sch

AU - Shnayder, Natalia A.

AU - Ershov, Evgeny E.

AU - Bugorsky, Alexander V.

AU - Kravtsov, Vladimir V.

AU - Taraskina, Anastasia E.

AU - Andreev, Boris V.

AU - Yakhin, Kausar K.

AU - Neznanov, Nikolay G.

AU - Nasyrova, Regina F.

PY - 2018/9

Y1 - 2018/9

N2 - The purpose of our research was to study the association of the HTR2A T102C (rs6313) SNP with anthropometric and biochemical markers in patients treated with typical and atypical antipsychotics in monotherapy mode.Materials and methods: One hundred and seventeen white inpatients (95 men and 22 women) with F2 disorders (ICD-10, 1995) were enrolled in the study. All patients were divided into two groups by the antipsychotic class with which they were treated (Group 1 included 40 patients treated with typical antipsychotics; Group 2 included 77 patients treated with atypical antipsychotics) and two subgroups by weight change criteria during the study (Subgroup 1 included patients with weight change >6%; Subgroup 2 included patients with weight changeResults: There were no statistically significant differences in the distribution of genotypes of the HTR2A T102C (rs6313) SNP between Group 1 and Group 2 (P > 0.05). Kruskal-Wallis one-way analysis of variance between subgroups showed statistically significant differences between carbamide levels in the second visit in Group 2 (P = 0.02). We showed statistically significant differences between TT and CT genotypes of the HTR2A T102C SNP: carbamide level was greater in TT carriers (P = 0.02). The strength of associations and risks between alleles of the HTR2A T102C SNP and antipsychotic-induced weight change were as follows: ORC = 0.49; CIC [0.25; 0.95]; RRC = 0.58 CIC [0.35; 0.97]; ORT = 2.03; CIT [1.05; 3.94]; RRT = 1.7 CIT [1.02; 2.81].Conclusion: Our results of the pilot pharmacogenetic studies show an association of the T allele carriage of the HTR2A T102C (rs6313) SNP with risk of antipsychotic-induced weight gain. The continuation of this study and an increase in the sample size will allow establishing valid pharmacogenetic markers for the risk of antipsychotic-induced weight gain.

AB - The purpose of our research was to study the association of the HTR2A T102C (rs6313) SNP with anthropometric and biochemical markers in patients treated with typical and atypical antipsychotics in monotherapy mode.Materials and methods: One hundred and seventeen white inpatients (95 men and 22 women) with F2 disorders (ICD-10, 1995) were enrolled in the study. All patients were divided into two groups by the antipsychotic class with which they were treated (Group 1 included 40 patients treated with typical antipsychotics; Group 2 included 77 patients treated with atypical antipsychotics) and two subgroups by weight change criteria during the study (Subgroup 1 included patients with weight change >6%; Subgroup 2 included patients with weight changeResults: There were no statistically significant differences in the distribution of genotypes of the HTR2A T102C (rs6313) SNP between Group 1 and Group 2 (P > 0.05). Kruskal-Wallis one-way analysis of variance between subgroups showed statistically significant differences between carbamide levels in the second visit in Group 2 (P = 0.02). We showed statistically significant differences between TT and CT genotypes of the HTR2A T102C SNP: carbamide level was greater in TT carriers (P = 0.02). The strength of associations and risks between alleles of the HTR2A T102C SNP and antipsychotic-induced weight change were as follows: ORC = 0.49; CIC [0.25; 0.95]; RRC = 0.58 CIC [0.35; 0.97]; ORT = 2.03; CIT [1.05; 3.94]; RRT = 1.7 CIT [1.02; 2.81].Conclusion: Our results of the pilot pharmacogenetic studies show an association of the T allele carriage of the HTR2A T102C (rs6313) SNP with risk of antipsychotic-induced weight gain. The continuation of this study and an increase in the sample size will allow establishing valid pharmacogenetic markers for the risk of antipsychotic-induced weight gain.

KW - antipsychotics

KW - single nucleotide polymorphism

KW - serotonin receptor 2A

KW - HTR2A gene

KW - weight gain

KW - 5-HT2A RECEPTOR GENE

KW - SCHIZOPHRENIA

KW - DRUGS

KW - 2ND-GENERATION

KW - POLYMORPHISM

KW - INDIVIDUALS

KW - PREDICTION

KW - EXPRESSION

KW - OBESITY

KW - REGION

U2 - 10.21103/Article8(3)_OA3

DO - 10.21103/Article8(3)_OA3

M3 - статья

VL - 8

SP - 186

EP - 191

JO - International Journal of Biomedicine

JF - International Journal of Biomedicine

SN - 2158-0510

IS - 3

ER -

ID: 93794348