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羟基脲治疗对镰状细胞病全血转录组的影响。

Impact of hydroxycarbamide treatment on the whole-blood transcriptome in sickle cell disease.

作者信息

Bhat Varsha, Potdar Alka A, Yu G Karen, Gibson Greg, Sheehan Vivien A

机构信息

Center for Integrative Genomics, School of Biological Sciences, Georgia Institute of Technology, Atlanta, Georgia, USA.

Pfizer Inc, South San Francisco, California, USA.

出版信息

Br J Haematol. 2025 Feb;206(2):713-720. doi: 10.1111/bjh.19839. Epub 2024 Nov 17.

DOI:10.1111/bjh.19839
PMID:39552261
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC12236451/
Abstract

Hydroxycarbamide (HC) is the most widely used therapeutic for individuals with sickle cell disease (SCD, including sickle cell anemia and other forms of the disease). HC's clinical benefits are primarily associated with its ability to induce foetal haemoglobin (HbF); this limited view of HC's therapeutic potential may lead to its discontinuation when a modest amount of HbF is induced. A better understanding of the HbF-independent effects of HC on genes and pathways relevant to SCD pathophysiology is therefore needed. In this study, we performed bulk RNA-Seq on whole blood samples collected from a cohort of 25 paediatric patients with SCD to identify genes and pathways that are affected by treatment with HC. At the maximum tolerated dose (MTD) of HC, patients showed altered expression levels of several genes and biological pathways. Pathways related to haeme metabolism, interferon-alpha response, and interferon-gamma response were significantly downregulated at HC MTD relative to the matched pre-HC samples. Pathways linked with IL2-STAT5 signalling and TNFα signalling via NF-Kβ were observed to be up-regulated at HC MTD. These results illustrate the range of effects exerted by HC during therapy for SCD and pave the way for an improved understanding of the HbF induction-independent benefits of HC.

摘要

羟基脲(HC)是镰状细胞病(SCD,包括镰状细胞贫血和其他形式的疾病)患者使用最广泛的治疗药物。HC的临床益处主要与其诱导胎儿血红蛋白(HbF)的能力有关;当诱导出适量的HbF时,对HC治疗潜力的这种有限认识可能导致其停用。因此,需要更好地了解HC对与SCD病理生理学相关的基因和通路的非HbF依赖性作用。在本研究中,我们对从25名患有SCD的儿科患者队列中采集的全血样本进行了批量RNA测序,以确定受HC治疗影响的基因和通路。在HC的最大耐受剂量(MTD)下,患者表现出几个基因和生物学通路的表达水平发生改变。相对于匹配的HC治疗前样本,在HC MTD下,与血红素代谢、α-干扰素反应和γ-干扰素反应相关的通路显著下调。在HC MTD下,观察到与IL2-STAT5信号通路和通过NF-Kβ的TNFα信号通路相关的通路上调。这些结果说明了HC在SCD治疗期间发挥的作用范围,并为更好地理解HC的非HbF诱导益处铺平了道路。

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