在放血的小鼠中,鼠生长分化因子 15 对于维持系统铁稳态不是必需的。
The murine growth differentiation factor 15 is not essential for systemic iron homeostasis in phlebotomized mice.
机构信息
Department of Pediatric Oncology, Hematology and Immunology, University Hospital of Heidelberg, Germany.
出版信息
Haematologica. 2013 Mar;98(3):444-7. doi: 10.3324/haematol.2012.069807. Epub 2012 Sep 14.
Abstract
In conditions of increased erythropoiesis, expression of hepcidin, the master regulator of systemic iron homeostasis, is decreased to allow for the release of iron into the blood stream from duodenal enterocytes and macrophages. It has been suggested that hepcidin suppression is controlled by growth differentiation factor 15 (GDF15), a member of the transforming growth factor-β superfamily of cytokines that is secreted from developing erythroblasts. In this study, we analyzed iron-related parameters in mice deficient for GDF15 under steady-state conditions and in response to increased erythropoietic activity induced by blood loss. We demonstrate that GDF15 suppresses the hepatic mRNA expression of some BMP/TGFβ target genes but not of hepcidin, and show that GDF15 is not required to balance iron homeostasis in response to blood loss.
摘要
在红细胞生成增加的情况下,作为系统铁稳态主调控因子的铁调素的表达减少,从而允许铁从十二指肠肠上皮细胞和巨噬细胞释放到血液中。有人提出,铁调素的抑制受生长分化因子 15(GDF15)控制,GDF15 是转化生长因子-β细胞因子超家族的成员,从正在发育的红细胞中分泌。在这项研究中,我们分析了在稳态条件下缺乏 GDF15 的小鼠的铁相关参数,并分析了失血引起的红细胞生成活性增加的反应。我们证明 GDF15 抑制肝脏中某些 BMP/TGFβ 靶基因的 mRNA 表达,但不抑制铁调素的表达,并表明 GDF15 不需要在响应失血时平衡铁稳态。
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