Genetic modifiers of long-term survival in sickle cell anemia

被引：23

作者：

Wonkam, Ambroise ^{[1
,2
]}

Chimusa, Emile R. ^{[1
,2
]}

Mnika, Khuthala ^{[1
]}

Pule, Gift Dineo ^{[1
]}

Ngo Bitoungui, Valentina Josiane ^{[1
]}

Mulder, Nicola ^{[3
]}

Shriner, Daniel ^{[4
]}

Rotimi, Charles N. ^{[4
]}

Adeyemo, Adebowale ^{[4
]}

机构：

[1] Univ Cape Town, Div Human Genet, Inst Infect Dis & Mol Med IDM, Fac Hlth Sci, Cape Town, South Africa

[2] Univ Cape Town, Inst Infect Dis & Mol Med IDM, Fac Hlth Sci, Cape Town, South Africa

[3] Univ Cape Town, Computat Biol Div, Dept Integrat Biomed Sci, Inst Infect Dis & Mol Med, Cape Town, South Africa

[4] NHGRI, Ctr Res Genom & Global Hlth, NIH, Bethesda, MD 20892 USA

来源：

CLINICAL AND TRANSLATIONAL MEDICINE | 2020年 / 10卷 / 04期

关键词：

Africa; genetic modifiers; sickle cell disease; whole exome sequencing; UNITED-STATES; RISK-FACTORS; DISEASE; MORTALITY; STROKE; TRIAL; METAANALYSIS; ASSOCIATION; PREVENTION; GLUTAMINE;

D O I：

10.1002/ctm2.152

中图分类号：

R73 [肿瘤学];

学科分类号：

100214 ;

摘要：

Background Sickle cell anemia (SCA) is a clinically heterogeneous, monogenic disorder. Medical care has less-than-optimal impact on clinical outcomes in SCA in Africa due to several factors, including patient accessibility, poor access to resources, and non-availability of specific effective interventions for SCA. Methods Against this background, we investigated 192 African participants who underwent whole exome sequencing. Participants included 105 SCA patients spanning variable clinical expression: a "long survivor" group (age over 40 years), a "stroke" group (at least one episode of overt stroke), and a "random" group (patients younger than 40 years without overt cerebrovascular disease). Fifty-eight ethnically matched homozygous hemoglobin A controls were also studied. Findings were validated in an independently recruited sample of 29 SCA patients. Statistical significance of the mutational burden of deleterious and loss-of-function variants per gene against a null model was estimated for each group, and gene-set association tests were conducted to test differences between groups. Results In the "long survivor" group, deleterious/loss-of-function variants were enriched in genes includingCLCN6(a voltage-dependent chloride channel for which rare deleterious variants have been associated with lower blood pressure) andOGHDL(important in arginine metabolism, which is a therapeutic target in SCA). In the "stroke" group, significant genes implicated were associated with increased activity of the blood coagulation cascade and increased complement activation, for example,SERPINC1, which encodes antithrombin. Oxidative stress and glutamate biosynthesis pathways were enriched in "long survivors" group. Published transcriptomic evidence provides functional support for the role of the identified pathways. Conclusions This study provides new gene sets that contribute to variability in clinical expression of SCA. Identified genes and pathways suggest new avenues for other interventions.

引用

页数：15

共 37 条

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