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镰状细胞特征与地方性 Burkitt 淋巴瘤无关:一项基于种族和疟疾流行率匹配的病例对照研究表明,控制 EBV 的因素可能成为这种儿科癌症的预测生物标志物。

Sickle cell trait is not associated with endemic Burkitt lymphoma: an ethnicity and malaria endemicity-matched case-control study suggests factors controlling EBV may serve as a predictive biomarker for this pediatric cancer.

机构信息

Center for Global Health Research, Kenyan Medical Research Institute, Kisumu, Kenya; Department of Biomedical Sciences and Technology, Maseno University, Maseno, Kenya.

出版信息

Int J Cancer. 2014 Feb 1;134(3):645-53. doi: 10.1002/ijc.28378. Epub 2013 Aug 16.

Abstract

Endemic Burkitt lymphoma (eBL) is associated with Epstein-Barr virus (EBV) and Plasmodium falciparum coinfections. Malaria appears to dysregulate immunity that would otherwise control EBV, thereby contributing to eBL etiology. Juxtaposed to human genetic variants associated with protection from malaria, it has been hypothesized that such variants could decrease eBL susceptibility, historically referred to as "the protective hypothesis." Past studies attempting to link sickle cell trait (HbAS), which is known to be protective against malaria, with protection from eBL were contradictory and underpowered. Therefore, using a case-control study design, we examined HbAS frequency in 306 Kenyan children diagnosed with eBL compared to 537 geographically defined and ethnically matched controls. We found 23.8% HbAS for eBL patients, which was not significantly different compared to 27.0% HbAS for controls [odds ratio (OR) = 0.85; 95% confidence interval (CI) 0.61-1.17; p-value = 0.33]. Even though cellular EBV titers, indicative of the number of latently infected B cells, were significantly higher (p-value < 0.0003) in children residing in malaria holoendemic compared to hypoendemic areas, levels were not associated with HbAS genotype. Combined, this suggests that although HbAS protects against severe malaria and hyperparasitemia, it is not associated with viral control or eBL protection. However, based on receiver operating characteristic curves factors that enable the establishment of EBV persistence, in contrast to those involved in EBV lytic reactivation, may have utility as an eBL precursor biomarker. This has implications for future human genetic association studies to consider variants influencing control over EBV in addition to malaria as risk factors for eBL.

摘要

地方性伯基特淋巴瘤(eBL)与 EBV 和疟原虫共感染有关。疟疾似乎会使免疫失调,从而无法控制 EBV,从而导致 eBL 的发生。与人类遗传变异相关的疟疾保护作用相反,人们假设这种变异可能会降低 eBL 的易感性,这在历史上被称为“保护假说”。过去的研究试图将镰状细胞特征(HbAS)与 eBL 的保护作用联系起来,而 HbAS 已知可预防疟疾,但这些研究结果相互矛盾且缺乏效力。因此,我们使用病例对照研究设计,检查了 306 名肯尼亚患有 eBL 的儿童与 537 名在地理上定义和种族匹配的对照者中 HbAS 的频率。我们发现 eBL 患者的 HbAS 频率为 23.8%,与对照组的 27.0% HbAS 相比无显著差异[比值比(OR)=0.85;95%置信区间(CI)0.61-1.17;p 值=0.33]。尽管指示潜伏感染 B 细胞数量的 EBV 细胞滴度在疟疾全流行地区的儿童中明显更高(p 值<0.0003),但这些水平与 HbAS 基因型无关。综合来看,这表明尽管 HbAS 可预防严重疟疾和高寄生虫血症,但与病毒控制或 eBL 保护无关。但是,基于接受者操作特征曲线,可建立 EBV 持续性的因素与 EBV 裂解再激活相关的因素不同,它们可能作为 eBL 前体生物标志物具有实用性。这意味着未来的人类遗传关联研究除了将疟疾作为 eBL 的风险因素外,还应考虑影响 EBV 控制的遗传变异。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/efe2/4232886/d7b9ad4b5adc/ijc0134-0645-f1.jpg

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