Paraoxonase (PON1) L55M and Q192R polymorphisms in major depression and bipolar affective disorder

YILDIZ, MESUT; ÇELIKEL, FERYAL ÇAM; ATEŞ, ÖMER; TAYCAN, SERAP ERDOĞAN; BENLI, İSMAIL; DEMIR, OSMAN

doi:10.1590/0101-60830000000123

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Original articles • Arc. Clin. Psychiatr. 44 (3) • May-Jun 2017 • https://doi.org/10.1590/0101-60830000000123 copy

Paraoxonase (PON1) L55M and Q192R polymorphisms in major depression and bipolar affective disorder

Authorship SCIMAGO INSTITUTIONS RANKINGS

Abstract

Background

Oxidative and nitrosative stress pathways, along with immune-inflammatory response, might play an important role in the pathogenic mechanisms underlying major depression and bipolar disorder.

Objective

The aim of the present study is to investigate paraoxonase 1 polymorphisms and its correlations with disease parameters in patients with major depression and bipolar affective disorder.

Methods

PON1 L55M and Q192R single nucleotide polymorphisms were analyzed in a group consisted of 100 patients with major depression, and 100 patients with bipolar affective disorder and 96 healthy controls. Polymorphisms were analyzed by using polymerase chain reaction.

Results

Our findings reported no association between Q192R and L55M polymorphisms of PON1 and major depression and bipolar disorder. Additionally, there was no association between the PON1 genotypes and disease variables in both depressed and bipolar patients.

Discussion

Evaluating the different stages of patients with affective disorders and and investigating the connection between PON1 polymorphisms and treatment outcomes will help us to clarify the relationship between PON1 and mood disorders.

Major depression; bipolar affective disorder; paraoxonase (PON1); polymorphism; association study

Characteristic	Depressed patients group
Gender, no. male/female (male %/female %)	13/87 (13.0/87.0)
Age, mean ± SD (range) years	38.21 ± 12.07

Characteristic	Bipolar patients group
Gender, no. male/female (male %/female %)	49/51 (49.0/51.0)
Age, mean ± SD (range) years	41.18 ± 12.27
Age of onset, mean ± SD (range) years	25.21 ± 9.86
Bipolar disorder subtype, n (%)
Type 1	87 (87%)
Type 2	13 (13%)
Rapid cycling, n (%)	17 (17%)
Seasonal pattern, n (%)	59 (59%)
Alcohol/drug use, n (%)	10 (10%)
Suicidal behavior, n (%)	26 (26%)
Psychotic feature, n (%)	55 (55%)
Hospitalization, n (%)	69 (69%)
Family history of BPD, n (%)	33 (33%)
Family history of suicide, n (%)	13 (13%)

PON locus	Healthy controls n = 96 (%)	Major depression patients n = 100 (%)	P
PON55L/M			0.56
L/L	40 (41.7)	37 (37.0)
L/M	42 (43.7)	43 (43.0)
M/M	14 (14.6)	20 (20.0)
Alleles			0.15
L	122 (63.5)	117 (58.5)
M	70 (36.5)	83 (41.5)
PON192Q/R			0.61
Q/Q	43 (44.8)	47 (47.0)
Q/R	39 (40.6)	43 (43.0)
R/R	14 (14.6)	10 (10.0)
Alleles			0.24
Q	125 (65.0)	137 (68.5)
R	67 (35.0)	63 (31.5)

PON locus	Healthy controls n = 96 (%)	Bipolar patients n = 100 (%)	P
PON55L/M			0.89
L/L	40 (41.7)	39 (39.0)
L/M	42 (43.7)	47 (47.0)
M/M	14 (14.6)	14 (14.0)
Alleles			0.41
L	122 (63.5)	125 (62.5)
M	70 (36.5)	75 (37.5)
PON192Q/R			0.95
Q/Q	43 (44.8)	44 (44.0)
Q/R	39 (40.6)	40 (40.0)
R/R	14 (14.6)	16 (16.0) 0)
Alleles			0.41
Q	125 (65.0)	128 (64.0)
R	67 (35.0)	72 (36.

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[1] Address for correspondence: Mesut Yildiz. Department of Psychiatry, School of Medicine, Marmara University, Istanbul, Turkey. Telephone: +90 (216) 625 45 45, Fax: +90 (216) 625 46 39. E-mail: mesut.yildiz@marmara.edu.tr