Leptin receptor gene polymorphisms c.668A>G and c.1968G>C in Sudanese women with preeclampsia: a case-control study.

4区 医学 Q4 Medicine BMC Medical Genetics Pub Date : 2020-08-17 DOI:10.1186/s12881-020-01104-z
Amira Saad, Ishag Adam, Salah Eldin G Elzaki, Hiba A Awooda, Hamdan Z Hamdan
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引用次数: 5

Abstract

Background: Leptin receptor gene (LEPR) variants may affect the leptin levels and act as a risk factor for preeclampsia. Two LEPR gene missense variants rs1137101 (c.668A>G) and rs1805094 (c.1968G>C) were investigated in Sudanese women with preeclampsia.

Methods: A matched case-control study (122 women in each arm) was conducted in Saad Abualila Maternity Hospital in Khartoum, Sudan from May to December 2018. The cases were women with preeclampsia and the controls were healthy pregnant women. Genotyping for LEPR gene variants c.668A>G and c.1968G>C was performed using polymerase chain reaction-restriction fragment length polymorphism. Logistic regression models (adjusted for age, parity, body mass index and hemoglobin level) were conducted.

Results: Genotype frequency of LEPR gene variants c.668A>G and c.1968G>C was in accordance with Hardy-Weinberg equilibrium (P > 0.05) in the controls. Allele G in LEPRc.668A>G variant was significantly more frequent in the cases compared with the controls [43.4% vs. 10.2%; OR = 6.44; 95%CI (3.98-10.40); P < 0.001]. In variant LEPRc.668A>G, genotype AG was the prevalent genotype in the cases compared with the controls, and it was significantly associated with preeclampsia risk [37.7% vs. 15.5%; AOR = 3.48; 95%CI (1.15-10.54); P = 0.027]. Likewise, the GG genotype was the second most common genotype in the cases compared with the controls, and was associated with preeclampsia risk [24.6% vs. 2.5%; AOR = 14.19; 95%CI (1.77-113.76); P = 0.012]. None of the LEPRc.1968G>C variant genotypes were associated with preeclampsia. The CC genotype was not detected in neither the cases nor the controls. The haplotype A-G 70.1% was the prevalent haplotype in this population, and it significantly protected against preeclampsia [OR = 0.14; 95%CI (0.09-0.23); P < 0.001]. However, the haplotype G-G 26.8% was significantly associated with preeclampsia risk [OR = 6.70; 95%CI (4.16-11.05); P < 0.001]. Both variants c.668A>G and c.1968G>C were in strong linkage disequilibrium (D' = 1, r2 = 0.012).

Conclusions: Our data indicate that the rs1137101 (c.668A>G) variant and G-G haplotype may independently associate with the development of preeclampsia.

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苏丹妇女子痫前期瘦素受体基因多态性C . 668a >G和C . 1968g >C:一项病例对照研究
背景:瘦素受体基因(LEPR)变异可能影响瘦素水平,并作为子痫前期的危险因素。在苏丹先兆子痫妇女中研究了两个LEPR基因错配变异rs1137101 (C . 668a >G)和rs1805094 (C . 1968g >C)。方法:2018年5月至12月在苏丹喀土穆的Saad Abualila妇产医院进行匹配病例对照研究(每组122名妇女)。这些病例是患有先兆子痫的妇女,对照组是健康的孕妇。采用聚合酶链反应-限制性片段长度多态性对LEPR基因变异C . 668a >G和C . 1968g >C进行基因分型。采用Logistic回归模型(校正年龄、胎次、体重指数和血红蛋白水平)。结果:对照组LEPR基因C . 668a >G和C . 1968g >C的基因型频率符合Hardy-Weinberg平衡(P > 0.05)。LEPRc的等位基因G。668A>G变异在病例中的发生率明显高于对照组[43.4%比10.2%;或= 6.44;95%可信区间(3.98 - -10.40);与对照组相比,gp、基因型AG是病例中流行的基因型,且与子痫前期风险显著相关[37.7%比15.5%;aor = 3.48;95%可信区间(1.15 - -10.54);p = 0.027]。同样,与对照组相比,GG基因型是病例中第二常见的基因型,与子痫前期风险相关[24.6%对2.5%;aor = 14.19;95%可信区间(1.77 - -113.76);p = 0.012]。没有LEPRc。1968G>C变异基因型与先兆子痫相关。在病例和对照组中均未检测到CC基因型。70.1%的A-G单倍型是该人群中流行的单倍型,它对先兆子痫有显著的保护作用[OR = 0.14;95%可信区间(0.09 - -0.23);P G和C . 1968g >C处于强连锁不平衡状态(D' = 1, r2 = 0.012)。结论:我们的数据表明rs1137101 (c.668A>G)变异和G-G单倍型可能与子痫前期的发生独立相关。
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BMC Medical Genetics
BMC Medical Genetics 医学-遗传学
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12 months
期刊介绍: BMC Medical Genetics is an open access journal publishing original peer-reviewed research articles in the effects of genetic variation in individuals, families and among populations in relation to human health and disease. Note: BMC Medical Genetics is now closed. This journal has merged with BMC Medical Genomics, a broad-scope, open access community journal for all medical genetics and genomics research.
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