Type 2 diabetes-associated genetic variants of <i>FTO, LEPR, PPARg</i>, and <i>TCF7L2</i> in gestational diabetes in a Brazilian population

Anghebem-Oliveira, Mauren Isfer; Martins, Bruna Rodrigues; Alberton, Dayane; Ramos, Edneia Amancio de Souza; Picheth, Geraldo; Rego, Fabiane Gomes de Moraes

doi:10.1590/2359-3997000000258

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Sumário

Original Articles • Arch. Endocrinol. Metab. 61 (3) • May-Jun 2017 • https://doi.org/10.1590/2359-3997000000258 copy

Type 2 diabetes-associated genetic variants of FTO, LEPR, PPARg, and TCF7L2 in gestational diabetes in a Brazilian population

Authorship SCIMAGO INSTITUTIONS RANKINGS

ABSTRACT

Objective

Gestational diabetes mellitus (GDM) is a metabolic disorder that shares pathophysiologic features with type 2 diabetes mellitus. The aim of this study was to investigate the association of the polymorphisms fat mass and obesity-associated (FTO) rs1421085, leptin receptor (LEPR) rs1137100, rs1137101, peroxisome proliferator-activated receptor gamma (PPARg) rs1801282, and transcription factor 7-like 2 (TCF7L2) rs7901695 with GDM.

Subjects and methods

252 unrelated Euro-Brazilian pregnant women were classified into two groups according to the 2015 criteria of the American and Brazilian Diabetes Association: healthy pregnant women (n = 125) and pregnant women with GDM (n = 127), matched by age. The polymorphisms were genotyped using fluorescent probes (TaqMan^®).

Results

All groups were in Hardy-Weinberg equilibrium. The genotype and allele frequencies of the studied polymorphisms did not show significant differences between the groups (P > 0.05). In the healthy and GDM groups, the C allele frequencies (95% CI) of the FTO rs1421085 polymorphism were 36.8% [31–43%] and 35.0% [29–41%]; the G allele frequencies (95% CI) of the LEPR rs1137100 polymorphism were 24.8% [19–30%] and 22.8% [18–28%]; the G allele frequencies (95% CI) of the LEPR rs1137101 polymorphism were 43.6% [37–50%] and 42.9% [37–49%]; the G allele frequencies (95% CI) of the PPARg rs1801282 polymorphism were 7.6% [4–11%] and 8.3% [5–12%]; and the C allele frequencies (95% CI) of the TCF7L2 rs7901695 polymorphism were 33.6% [28–39%] and 39.0% [33–45%], respectively.

Conclusion

The studied polymorphisms were not associated with GDM in a Brazilian population.

Diabetes; gestational diabetes mellitus; polymorphisms; genetic variants; genotype

OMIM number	Gene	Chromosome position	Location	Polymorphism		TaqMan® probe
610966	FTO	16q12.2	Intron 1	rs1421085	C>T	C___8917103_10
601007	LEPR	1p31.3	Exon 4 Exon 6	rs1137100 rs1137101	A>G A>G	C____518168_20 C___8722581_10
601487	PPARg	3p25.2	Exon B	rs1801282	C>G	C___1129864_10
602228	TCF7L2	10q25.2– 25.3	Intron 3	rs7901695	C>T	C___384583_10

Characteristics	Control (n = 125)	GDM (n = 127)	P
Age, years	30.6 ± 4.7	31.9 ± 6.4	0.070
Body mass index^a, kg/m²	26.9 ± 5.0	32.7 ± 6.3	< 0.001
Hypertension, %	4.8	14.9	0.007*
Family history for diabetes, %	–	70.1	–
Fasting glucose, mg/dL	84.0 (79–88)	88 (81–95)	< 0.001**
2-h 75g glucose, mg/dL	86.2 (79–102)	161.0 (149–176)	< 0.001**
HbA1c, %	–	5.6 (5.3–5.9)	–
1,5 anhydroglucitol, µg/mL	11.7 ± 6.9	9.8 ± 5.1	0.060
Total cholesterol, mg/dL	213.9 ± 50.0	224.7 ± 45.6	0.074
HDL-cholesterol, mg/dL	55.4 ± 15.8	56.8 ± 12.5	0.451
LDL-cholesterol, mg/dL	130.9 ± 41.5	123.5 ± 38.9	0.146
Triglycerides, mg/dL	124.0 (96–171)	221.0 (175–270)	< 0.001**
Total protein, g/dL	6.9 ± 0.8	6.4 ± 0.5	< 0.001
Albumin, g/dL	4.2 ± 0.6	3.4 ± 0.4	< 0.001
Creatinine, mg/dL	0.80 (0.7–0.9)	0.70 (0.60–0.72)	< 0.001**
Urea, mg/dL	20.4 ± 5.3	16.1 ± 4.8	< 0.001
Uric acid, mg/dL	3.6 (3.0–3.9)	4.3 (3.7–4.9)	< 0.001**

Gene/SNP	Genotypes	Control n = 125	GDM n = 127	P
FTO rs1421085 (C>T)	TT	53 (42.4)	52 (40.9)	0.420*
	TC	52 (41.6)	61 (48.0)
	CC	20 (16.0)	14 (11.1)
	C-allele [95% CI]	36.8 [31–43]	35.0 [29–41]	0.680
LEPR rs1137100 (A>G)	AA	70 (56.0)	73 (57.5)	0.687*
	AG	48 (38.4)	50 (39.4)
	GG	7 (5.6)	4 (3.1)
	G-allele [95% CI]	24.8 [19–30]	22.8 [18–28]	0.604
LEPR rs1137101 (A>G)	AA	43 (34.4)	38 (29.9)	0.228*
	AG	55 (44.0)	69 (54.3)
	GG	27 (21.6)	20 (15.8)
	G-allele [95% CI]	43.6 [37–50]	42.9 [37–49]	0.876
PPARg rs1801282 (C>G)	CC	107 (85.6)	108 (85.0)	0.851*
	CG	17 (13.6)	17 (13.4)
	GG	1 (0.8)	2 (1.6)
	G-allele [95% CI]	7.6 [4–11]	8.3 [5–12]	0.782
TCF7L2 rs7901695 (C>T)	TT	52 (41.6)	44 (34.6)	0.413*
	CT	62 (49.6)	67 (52.8)
	CC	11 (8.8)	16 (12.6)
	C-allele [95% CI]	33.6 [28–39]	39.0 [33–45]	0.209

FTO rs1421085 polymorphism
Population	Characteristics	n	Genotype (%)			Allele (%)	Reference

			TT	TC	CC	C
Euro-Brazilian	GDM Controls	127 125	40.9 42.4	48.0 41.6	11.1 16.0	35.0 36.8	Present work
Chinese Han		90	70.7	24.4	4.9	11.6	HapMap-HCB
European		180	27.4	53.1	19.5	16.7	HapMap-CEU
Japanese		91	67.1	28.2	4.7	18.8	HapMap-JPT
Turkish	Obeses Controls	190 97	30.5 28.8	51.1 52.6	18.4 18.6	43.9 44.8	(48)
Caucasian	Obeses		29.5	30.5	40	55.2	(49)
African		90	86.7	13.3	0	6.6	HapMap-YRI

LEPR rs1137100 polymorphism

Population	Characteristics	N	Genotype (%)			Allele (%)	Reference

			AA	AG	GG	G

Euro-Brazilian	GDM Controls	127 125	57.5 56.0	39.4 38.4	3.1 5.6	22.8 24.8	Present work
African		90	69.6	27.7	2.7	16.5	HapMap-YRI
French	Obeses Controls	877 877	56.7 53.4	37.4 39.2	5.9 7.4	24.6 27.0	(50)
British	Obeses Controls	190 132	54.0 55.0	38.0 39.0	8.0 6.0	27.4 25.8	(51)
European		180	49.6	42.5	8.0	29.2	HapMap-CEU
Brazilians	Hypertension	470	42.8	46.8	10.4	33.8	(52)
Chinese Han		90	2.5	27.5	70.0	83.7	HapMap-HCB
Japanese		91	2.5	40.2	57.3	97.4	HapMap-JPT

LEPR rs1137101 polymorphism
Population	Characteristics	N	Genotype (%)			Allele (%)	Reference

			AA	AG	GG	G

Euro-Brazilian	GDM Controls	127 125	29.9 34.4	54.3 44.0	15.8 21.6	42.9 43.6	Present work
French	Obeses Controls	877 877	31.6 31.6	50.0 47.1	18.4 21.3	43.4 44.9	(50)
British	Obeses Controls	190 132	29.0 28.0	53.0 58.0	18.0 14.0	44.6 42.8	(51)
European		180	25.9	53.6	20.5	47.3	HapMap-CEU
African		90	11.1	58.3	30.6	59.7	HapMap-YRI
Japanese		91	1.2	30.5	68.3	83.5	HapMap-JPT
Chinese Han		90	2.2	17.8	80.0	88.9	HapMap-HCB

PPARg rs1801282 polymorphism
Population	Characteristics	n	Genotype (%)			Allele (%)	Reference

			CC	CG	GG	G

Euro-Brazilian	GDM Controls	127 125	85 85.6	13.4 13.6	1.6 0.8	8.3 7.6	Present work
French	Mothers with glucose tolerance	1708	80	19	1	10.4	(42)
Danish	GDM Women with glucose tolerance	283 2446	75.8 75.2	22.6 22.7	1.6 2.1	12.8 13.5	(22)
Danish	T2DM Controls	1461 4986	76 75	22 23	2 2	13.0 13.9	(53)
Italian	Peripheral arterial disease Controls	201 201	74.1 84.6	23.9 14.9	2.0 0.5	14.0 8.0	(54)
Scandinavian	GDM Controls	637 1232	73.5 74.5	24.8 24.2	1.7 1.3	14.1 13.4	(19)
Scandinavian Arabs	GDM Controls GDM Controls	400 428 100 122	71.5 74.1 91 86.9	27.7 24.5 9 12.3	0.8 1.4 0 0.8	14.6 13.7 4.5 7.0	(44)
Turkish	GDM Controls	62 100	80.7 84	19.3 16	0 0	19.4 16.0	(41)
Korean	GDM Controls	94 41	94.6 82.9	5.4 17.1	0 0	2.7 8.5	(55)
Greek	GDM Controls	148 107	96.6 93.5	3.4 6.5	0 0	3.0 2.0	(5)
Chinese	GDM Controls	55 173	94.5 90.8	5.5 9.2	0 0	3.0 5.0	(56)
Korean	GDM Controls	869 632	91.7 89.7	8.2 10.0	0.1 0.3	4.0 5.0	(43)

TCF7L2 rs7901895 polymorphism

Population	Characteristics	n	Genotype (%)			Allele (%)	Reference

			TT	TC	CC	C

Euro-Brazilian	GDM Controls	127 125	34.6 41.6	52.8 49.6	12.6 8.8	39.0 33.6	Present work
Chinese Han		90	95.3	4.7	0	2.3	HapMap-HCB
Swedish women	GDM Controls	1102 794	51.2 34.2	34.2 43.1	7.6 11.5	26.5 34.4	(45)
Swedish men	T2DM Controls	825 793	52.6 59.2	39.9 36.0	7.5 4.8	27.5 22.8	(57)
European		180	54.5	34.8	10.7	28.1	HapMap-CEU
Japanese		91	94.2	4.7	0.1	3.5	HapMap-JPT
Caucasian African-American	GDM GDM	- -	- -	- -	- -	30 40	(18)
Spanish	GDM Controls	45 25	38 40	44 52	18 8	40 34	(58)
African		90	27.4	56.5	15.9	44.2	HapMap-YRI

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[1] Correspondence to: Fabiane Gomes de Moraes Rego. Departamento de Análises Clínicas, Universidade Federal do Paraná. Rua Prefeito Lothário Meissner, 632. 80210-170 – Curitiba, PR, Brasil. rego@ufpr.br