Association of Multiple Genetic Variants with the Extension and Severity of Coronary Artery Disease

Fischer, Simone Cristina Pinto Matheus; Pinto, Simone Pires; Lins, Lívia Campos do Amaral Silva; Bianco, Henrique Tria; Monteiro, Carlos Manoel de Castro; Pinheiro, Luiz Fernando Muniz; Fonseca, Francisco Antonio Helfenstein; Izar, Maria Cristina de Oliveira

doi:10.5935/abc.20170177

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Original Article, Atherosclerosis/Endothelium/Vascular • Arq. Bras. Cardiol. 110 (1) • Jan 2018 • https://doi.org/10.5935/abc.20170177 copy

Association of Multiple Genetic Variants with the Extension and Severity of Coronary Artery Disease

Authorship SCIMAGO INSTITUTIONS RANKINGS

Abstract

Background:

Metabolic syndrome (MS) is a condition that, when associated with ischemic heart disease and cardiovascular events, can be influenced by genetic variants and determine more severe coronary atherosclerosis.

Objectives:

To examine the contribution of genetic polymorphisms to the extension and severity of coronary disease in subjects with MS and recent acute coronary syndrome (ACS).

Methods:

Patients (n = 116, 68% males) aged 56 (9) years, with criteria for MS, were prospectively enrolled to the study during the hospitalization period after an ACS. Clinical and laboratory parameters, high-sensitivity C-reactive protein, thiobarbituric acid reactive substances, adiponectin, endothelial function, and the Gensini score were assessed. Polymorphisms of paraoxonase-1 (PON-1), methylenotetrahydrofolate reductase (MTHFR), endothelial nitric oxide synthase (ENOS), angiotensin-converting enzyme (ACE), angiotensin II type 1 receptor (AT1R), apolipoprotein C3 (APOC3), lipoprotein lipase (LPL) were analysed by polymerase chain reaction (PCR) technique, followed by the identification of restriction fragment length polymorphisms (RFLP, and a genetic score was calculated. Parametric and non-parametric tests were used, as appropriate. Significance was set at p < 0.05.

Results:

Polymorphisms of PON-1, MTHFR and ENOS were not in the Hardy-Weinberg equilibrium. The DD genotype of LPL was associated with higher severity and greater extension of coronary lesions. Genetic score tended to be higher in patients with Gensini score < P50 (13.7 ± 1.5 vs. 13.0 ± 1.6, p = 0.066), with an inverse correlation between genetic and Gensini scores (R = -0.194, p = 0.078).

Conclusions:

The LPL polymorphism contributed to the severity of coronary disease in patients with MS and recent ACS. Combined polymorphisms were associated with the extension of coronary disease, and the lower the genetic score the more severe the disease.

Keywords:
Coronary Artery Disease / genetic; Polymorphism, Genetic; Metabolic Syndrome; Sedentary Lifestyle

Polymorphism	Starters	Annealing temperature	Cycles	Restriction enzyme
PON-1	Forward: 5'-TATTGTTGCTGTGGGACCTGAG-3'	61°C	35	Alw I
Q192R	Reverse: 5'-CACGCTAAACCCAAATACATCTC-3'	61°C	35	Alw I
MTHFR	Forward: 5'-GAAGCAGGGAGCTTTGAGG-3'	63°C	32	Hinf I
C677T	Reverse: 5'-ACGATGGGGCAAGTGATG-3'	63°C	32	Hinf I
ENOS	Forward: 5'-CTGGAGATGAAGGCAGGAGAC-3'	56°C	35	Ban II
G894T	Reverse: 5'-CTCCATCCCACCCAGTCAATC-3'	56°C	35	Ban II
ACE	Forward: 5'-CTGGAGACCACTCCCATCCTTTCT-3'	55°C^* * the touchdown PCR protocol was used for the ACE and LPL genes	32	-
I/D	Reverse: 5'-GTCTCGATCTCCTGACCTCGTG-3'		32	-
AT1R	Forward: 5'-AATGCTTGTAGCCAAAGTCACCT-3'	59°C	35	Dde I
A1166C	Reverse: 5'-GGCTTTGCTTTGTCTTGTTG-3'	59°C	35	Dde I
LPL	Forward: 5'-AAAATCAAGCAACCCTCAAG-3'	57°C^* * the touchdown PCR protocol was used for the ACE and LPL genes	35	Taq I
D9N	Reverse: 5'-TAGGGCAAATTTACTTGCGA-3'		35	Taq I
APOC3	Forward: 5'GGTGACCGATGGCTTCAGTT-3'	58°C	30	Sst I
SST I	Reverse: 5'-CAGAAGTGGATAGAGCGCT-3'	58°C	30	Sst I

Variable	n = 116
Male (%)	74 (68)
Age (years)	56 ± 9
Hypertension (%)	104 (90)
Smoking (%)	35 (30)
Diabetes mellitus (%)	36 (31)
AMI (%)	55 (47)
Unstable angina (%)	61 (53)
Stroke (%)	9 (8)
PVD (%)	12 (10)
BMI (Kg/m²)	30.2 ± 4.7
Waist circumference (cm)	104.4 ± 10.8
Systolic arterial pressure (mmHg)	132 ± 24
Diastolic arterial pressure (mmHg)	86 ± 16
Heart rate (bpm)	68 ± 13
Gensini score (au)	21 (0-36)
Gensini ≥ median (%)	42 (51)
FMD (%)	13.7 ± 8.6
EIR (%)	14.9 (7.3-18.8)

Gene	Allele frequency		Genotypic frequency (%)			p-value (Hardy Weinberg)
PON-1	Q	R	QQ	QR	RR
PON-1	0.63	0.37	36 (31)	76 (65)	4 (4)	0.0004
MTHFR	C	T	CC	CT	TT
MTHFR	0.61	0.39	35 (30)	72 (62)	9 (8)	0.0131
ENOS	G	T	GG	GT	TT
ENOS	0.43	0.57	10 (9)	80 (69)	26 (22)	0.0006
ACE	I	D	II	ID	DD
ACE	0.33	0.67	17 (15)	42 (36)	57 (49)	0.1955
AT1R	A	C	AA	AC	CC
AT1R	0.75	0.25	70 (60)	35 (30)	11 (10)	0.2351
APOC3	S1	S2	S1S1	S1S2	S2S2
APOC3	0.16	0.84	2 (2)	33 (28)	81 (70)	0.8310
LPL	D	N	DD	DN	NN
LPL	0.34	0.66	17 (15)	45 (39)	54 (46)	0.3095

Genetic score
N	116
Mean	13.3
Median	13.5
Standard deviation	1.58
Minimum	10
Maximum	17
Asymmetry	-0.263
Kurtosis	-0.146
P25	12.0
P75	14.0

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