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HbF 基因修饰物和镰状细胞病对羟基脲反应的遗传修饰物。

Genetic modifiers of HbF and response to hydroxyurea in sickle cell disease.

机构信息

Department of Pediatrics, Columbia University Medical Center, New York, New York 10032, USA.

出版信息

Pediatr Blood Cancer. 2011 Feb;56(2):177-81. doi: 10.1002/pbc.22754. Epub 2010 Sep 9.

DOI:10.1002/pbc.22754
PMID:20830771
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3006002/
Abstract

Fetal hemoglobin (HbF) levels are generally inversely proportional to severity of sickle cell disease (SCD) for given sickle phenotypes. Molecular regulation of HbF occurs through complex interactions cis and trans to the beta globin gene locus. Novel insights made through population-based genetic epidemiologic studies of non-anemic populations were replicated in SCD groups, despite large differences in HbF levels. Identification of the lymphoid transcription factor BCL11A as a key suppressor of HbF expression validates approaches using population genetics to study HbF expression. We review these methods and findings, and speculate on applying pharmaco-genetics to optimize hydroxyurea therapy aimed at increasing HbF.

摘要

胎儿血红蛋白 (HbF) 水平通常与给定镰状细胞病 (SCD) 表型的严重程度成反比。HbF 的分子调控是通过β珠蛋白基因座的顺式和反式复杂相互作用发生的。通过对非贫血人群进行基于人群的遗传流行病学研究获得的新见解在 SCD 组中得到了复制,尽管 HbF 水平存在很大差异。淋巴转录因子 BCL11A 的鉴定作为 HbF 表达的关键抑制剂,验证了使用群体遗传学方法研究 HbF 表达的方法。我们回顾了这些方法和发现,并推测将药物遗传学应用于优化旨在增加 HbF 的羟基脲治疗。

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