镰状细胞贫血中的胎儿血红蛋白。
Fetal hemoglobin in sickle cell anemia.
机构信息
Department of Medicine, Boston University School of Medicine, Boston, MA, USA.
出版信息
Blood. 2011 Jul 7;118(1):19-27. doi: 10.1182/blood-2011-03-325258. Epub 2011 Apr 13.
Abstract
Fetal hemoglobin (HbF) is the major genetic modulator of the hematologic and clinical features of sickle cell disease, an effect mediated by its exclusion from the sickle hemoglobin polymer. Fetal hemoglobin genes are genetically regulated, and the level of HbF and its distribution among sickle erythrocytes is highly variable. Some patients with sickle cell disease have exceptionally high levels of HbF that are associated with the Senegal and Saudi-Indian haplotype of the HBB-like gene cluster; some patients with different haplotypes can have similarly high HbF. In these patients, high HbF is associated with generally milder but not asymptomatic disease. Studying these persons might provide additional insights into HbF gene regulation. HbF appears to benefit some complications of disease more than others. This might be related to the premature destruction of erythrocytes that do not contain HbF, even though the total HbF concentration is high. Recent insights into HbF regulation have spurred new efforts to induce high HbF levels in sickle cell disease beyond those achievable with the current limited repertory of HbF inducers.
摘要
胎儿血红蛋白 (HbF) 是镰状细胞病血液学和临床特征的主要遗传调节剂,这种作用是通过其从镰状血红蛋白聚合物中排除介导的。胎儿血红蛋白基因受到遗传调控,HbF 的水平及其在镰状红细胞中的分布具有高度可变性。一些镰状细胞病患者的 HbF 水平异常高,这与 HBB 样基因簇的塞内加尔和沙特-印度单倍型有关;具有不同单倍型的一些患者也可以有类似的高 HbF。在这些患者中,高 HbF 与通常较轻但非无症状的疾病有关。研究这些患者可能会提供对 HbF 基因调控的更多见解。HbF 似乎对某些疾病并发症的益处大于其他并发症。这可能与不含 HbF 的红细胞过早破坏有关,尽管总 HbF 浓度较高。HbF 调控的新见解促使人们在镰状细胞病中努力诱导高于当前有限的 HbF 诱导剂所能达到的 HbF 水平。
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