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触珠蛋白2-2基因型与肯尼亚沿海地区儿童恶性疟原虫疟疾发病率降低有关。

The haptoglobin 2-2 genotype is associated with a reduced incidence of Plasmodium falciparum malaria in children on the coast of Kenya.

作者信息

Atkinson Sarah H, Mwangi Tabitha W, Uyoga Sophie M, Ogada Edna, Macharia Alex W, Marsh Kevin, Prentice Andrew M, Williams Thomas N

机构信息

KEMRI/Wellcome Trust Programme, Centre of Geographic Medicine Research, Kilifi District Hospital, Kilifi, Kenya.

出版信息

Clin Infect Dis. 2007 Mar 15;44(6):802-9. doi: 10.1086/511868. Epub 2007 Feb 7.

Abstract

BACKGROUND

Haptoglobin (Hp) genotype determines the efficiency of hemoglobin clearance after malaria-induced hemolysis and alters antioxidant and immune functions. The Hp2 allele is thought to have spread under strong selection pressure, but it is unclear whether this is due to protection from malaria or other diseases.

METHODS

We monitored the incidence of febrile malaria and other childhood illnesses with regard to Hp genotype in a prospective cohort of 312 Kenyan children during 558.3 child-years of follow-up. We also conducted 7 cross-sectional surveys to determine the prevalence of Plasmodium falciparum parasitemia.

RESULTS

The Hp2/2 genotype was associated with a 30% reduction in clinical malarial episodes (adjusted incidence rate ratio, 0.67; P=.008 for Hp2/2 vs. Hp1/1 and Hp2/1 combined). Protection increased with age; there was no protection in the first 2 years of life, 30% protection at > or = 2 years of age, and 50% protection from 4-10 years of age. Children with the Hp1/1 genotype had a significantly lower rate of nonmalarial fever (P=.001).

CONCLUSIONS

Balancing selection pressures may have influenced the spread of the Hp gene. Our observations suggest that the Hp2 allele may have spread as a result of protection from malaria, and the Hp1 allele may be sustained by protection from other infections.

摘要

背景

触珠蛋白(Hp)基因型决定疟疾诱导溶血后血红蛋白清除效率,并改变抗氧化和免疫功能。Hp2等位基因被认为是在强大的选择压力下传播的,但尚不清楚这是由于对疟疾或其他疾病的保护作用。

方法

在558.3儿童年的随访期间,我们前瞻性监测了312名肯尼亚儿童队列中发热性疟疾和其他儿童疾病的发病率与Hp基因型的关系。我们还进行了7次横断面调查,以确定恶性疟原虫血症的患病率。

结果

Hp2/2基因型与临床疟疾发作减少30%相关(调整后的发病率比,0.67;Hp2/2与Hp1/1和Hp2/1合并相比,P = 0.008)。保护作用随年龄增加;在生命的前2年没有保护作用,在≥2岁时保护作用为30%,在4 - 10岁时保护作用为50%。Hp1/1基因型的儿童非疟疾发热率显著较低(P = 0.001)。

结论

平衡选择压力可能影响了Hp基因的传播。我们的观察结果表明,Hp2等位基因可能因对疟疾的保护作用而传播,而Hp1等位基因可能因对其他感染的保护作用而得以维持。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/69b7/2659731/d2671eca232b/ukmss-4256-f0001.jpg

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