A variante <i>MTHFR</i> 677C&gt;T (RS1801133) está associada a hiperhomocisteinemia, mas não a gravidade clínica em pacientes com doença arterial periférica

Silvestre, Guilherme da Silva; Carrara, Iriana Moratto; Flauzino, Tamires; Lozovoy, Marcell Alysson Batisti; Cecchini, Rubens; Reiche, Edna Maria Vissoci; Simão, Andréa Name Colado

Guilherme da Silva Silvestre

analysis and interpretation

data collection

writing the article

critical revision of the article

final approval of the article

Universidade Estadual de Londrina – UEL, Londrina, PR, Brasil.

Iriana Moratto Carrara

data collection

final approval of the article

Universidade Estadual de Londrina – UEL, Londrina, PR, Brasil.

Centro Universitário Filadélfia – UNIFIL, Londrina, PR, Brasil.

Tamires Flauzino

data collection

final approval of the article

statistical analysis

Universidade Estadual de Londrina – UEL, Londrina, PR, Brasil.

Laboratório Central Diagnósticos de Londrina, Londrina, PR, Brasil.

Marcell Alysson Batisti Lozovoy

data collection

final approval of the article

Universidade Estadual de Londrina – UEL, Londrina, PR, Brasil.

Centro Universitário Filadélfia – UNIFIL, Londrina, PR, Brasil.

Rubens Cecchini

conception and design

final approval of the article

Universidade de São Paulo – USP, Ribeirão Preto, SP, Brasil.

Edna Maria Vissoci Reiche

conception and design

analysis and interpretation

writing the article

critical revision of the article

final approval of the article

Universidade Estadual de Londrina – UEL, Londrina, PR, Brasil.

http://orcid.org/0000-0001-6507-2839

Andréa Name Colado Simão

conception and design

analysis and interpretation

writing the article

critical revision of the article

final approval of the article

statistical analysis

overall responsibility

Universidade Estadual de Londrina – UEL, Londrina, PR, Brasil.

Conflicts of interest: No conflicts of interest declared concerning the publication of this article.

Correspondence Edna Maria Vissoci Reiche Universidade Estadual de Londrina – UEL, Hospital Universitário de Londrina, Laboratório de Pesquisa em Imunologia Aplicada Av. Robert Koch, 60 CEP 86038-440 - Londrina (PR), Brasil Tel.: +55 (43) 3371-2619 E-mail: reiche@sercomtel.com.br

Author information GSS - MSc in Fisiopatologia Clínica e Laboratorial, Board certified (Clínica Médica, Cirurgia Vascular, Angiorradiologia and Cirurgia Endovascular residency, Universidade Estadual de Londrina (UEL). IMC - MSc in Patologia Experimental, PhD candidate in Patologia Experimental, Universidade Estadual de Londrina (UEL); Degree in Biomedicina, Centro Universitário Filadélfia (UNIFIL). TF - PhD in Ciências da Saúde, Degree in Farmácia, Universidade Estadual de Londrina (UEL); Employee, Setor de Biologia Molecular, Laboratório Central Diagnósticos de Londrina. MABL - MSc in Patologia Experimental, PhD in Patologia Experimental, Universidade Estadual de Londrina (UEL); Degree in Farmácia, Universidade Paranaense; Qualification in Análises Clínicas, Centro Universitário Filadélfia (UNIFIL). RC - Postdoctoral fellow, Universidade de Londres-Kings College; PhD in Ciências Biológicas (Bioquímica), Universidade de São Paulo (USP). EMVR - PhD in Medicina and Ciências da Saúde, MSc in Microbiologia; Sênior professor, Programa de Pós-Graduação em Fisiopatologia Clínica e Laboratorial, Centro de Ciências da Saúde, Universidade Estadual de Londrina (UEL). ANCS - PhD in Ciências da Saúde, Universidade Estadual de Londrina (UEL).

	Control (n=113)	PAD (n=157)	p value ^* * Adjusted for age, sex, ethnicity, and body mass index.
Age (years)	43 (37 – 48)	69 (62 – 76)	<0.001
Sex (Female/Male)	54 (47.8)/59 (52.2)	60 (38.2)/97 (61.8)	0.116
Ethnicity (C/NC)	88 (77.9)/25 (22.1)	109 (69.4)/48 (30.6)	0.123
BMI (kg/m²)	25.81 (22.95 – 28.80)	25.31 (21.64 – 29.73)	0.355
Hcy (µmol/L)^ When the Hcy values were adjusted for folate, vitamin B12, kidney disease, alcoholism, sedentary life style, and smoking, the differences between Hcy values did not remain significant (p>0.05).	9.91 (8.47 – 11.30)	13.66 (10.61 – 16.74)	0.020
Folate (ng/mL)	5.4 (3.9 – 7.5)	7.3 (5.1 – 10.6)	0.242
Vitamin B12 (pg/mL)	320 (230-450)	316 (236 – 440)	0.885

Characteristics	Patients with PAD (n=157)
Fontaine classification^* * This variable was not recorded in one patient.
I - asymptomatic	0 (0.0)
IIa - mild claudication	35 (22.4)
IIb - severe claudication	33 (21.2)
III - pain at rest	11 (7.0)
IV - trophic injury	77 (49.4)
Intermittent claudication (IIa + IIb)	68 (43.6)
Critical limb ischemia (III + IV)	88 (56.4)
Aorto-iliac (No/Yes)^ This variable was not recorded in two patients.	115 (74.2)/40 (25.8)
TASC A	7 (4.5)
TASC B	5 (3.2)
TASC C	12 (7.7)
TASC D	16 (10.3)
Femoropopliteal (No/Yes)*	21 (13.5)/134 (86.5)
TASC A	9 (5.8)
TASC B	17 (11.0)
TASC C	36 (23.2)
TASC D	71 (45.8)
Aorto-iliac + femoropopliteal (No/Yes)**	136 (87.7)/19 (12.3)
All patients without distinction by arteries involved: TASC A+B/C+D**	23 (14.8)/132 (85.2)

Genetic model		Controls (n=113)	PAD (n=157)	OR (95% CI)	p-value ^* * Adjusted for age, sex, ethnicity, and body mass index (BMI). OR: odds ratio; CI: confidence interval; C: major allele; T: minor allele.
Allelic	C	156 (69.0)	209 (66.6)	Reference	-
	T	70 (31.0)	105 (33.4)	1.120 (0.778 – 1.628)	0.576
Codominant	CC	54 (47.8)	76 (48.4)	Reference	-
	CT	48 (42.5)	57 (36.3)	1.230 (0.423 – 3.579)	0.704
	TT	11 (9.7)	24 (15.3)	3.415 (0.655 – 17.79)	0.145
Dominant	CC	54 (47.8)	76 (48.4)	Reference	-
	CT+TT	59 (52.2)	81 (51.6)	1.484 (0.536 – 4.105)	0.447
Recessive	CC+CT	102 (90.3)	133 (84.7)	Reference	-
	TT	11 (9.7)	24 (15.3)	3.029 (0.660 – 13.91)	0.154
Overdominant	CC+TT	65 (57.5)	100 (63.7)	Reference	-
	CT	48 (42.5)	57 (36.3)	0.921 (0.346– 2.454)	0.870

Variable	CC (n=76)	CT+TT (n=81)	p value*	CC+CT (n=133)	TT (n=24)	p value ^* * Adjusted for age, sex, ethnicity, BMI, folate, vitamin B12, dyslipidemia, kidney disease, alcoholism, sedentary lifestyle, and smoking
Age (year)	71 (61 – 78)	68 (62 – 74)	0.321	69 (61 – 76)	71 (63 – 76)	0.963
Sex (Female/Male)	26 (34.2)/50 (65.8)	34 (42.0)/47 (58.0)	0.317	50 (37.6)/83 (62.4)	10 (41.7)/14 (58.3)	0.705
Ethnicity (C/NC)	44 (57.9)/ 32 (42.1)	65 (80.2)/16 (19.8)	0.002	88 (66.2)/45 (33.8)	21 (87.5)/3 (12.5)	0.037
BMI (kg/m²)	24.57 (21.26 – 27.92)	26.17 (22.43 – 30.61)	0.157	25.35 (21.67 – 29.73)	24.98 (20.31 – 29.37)	0.489
Homocysteine (µmol/L)	12.94 (10.02 – 15.98)	14.60 (10.86 – 17.83)	0.008	13.22 (10.20 – 15.97)	16.40 (13.65 – 23.77)	0.019
Folate (ng/mL)	7.1 (5.2 – 10.6)	7.5 (4.8 – 10.8)	0.945	7.5 (5.3 – 11.1)	6.3 (3.7 – 9.6)	0.126
Vitamin B12 (pg/mL)	341 (241 – 459)	299 (217 – 418)	0.202	318 (244 – 445)	276 (185 – 395)	0.596
Fontaine IIa+IIb/II+IV	32 (42.1)/44 (57.9)	36 (45.0)/44 (55.0)	0.716	56 (42.4)/76 (57.6)	12 (50.0)/12 (50.0)	0.548
TASC A+B/C+D^ This variable was not recorded in two patients.	10 (13.3)/65 (86.7)	13 (16.2)/67 (83.8)	0.610	20 (15.2)/112 (84.8)	3 (13.0)/20 (87.0)	0.544

[1] Conflicts of interest: No conflicts of interest declared concerning the publication of this article.

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A variante MTHFR 677C>T (RS1801133) está associada a hiperhomocisteinemia, mas não a gravidade clínica em pacientes com doença arterial periférica

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