Division of Hematology, Brigham and Women's Hospital, Boston, MA, USA.
Blood. 2011 Mar 3;117(9):2567-76. doi: 10.1182/blood-2010-07-295238. Epub 2010 Nov 10.
Haploinsufficiency for ribosomal protein genes has been implicated in the pathophysiology of Diamond-Blackfan anemia (DBA) and the 5q-syndrome, a subtype of myelodysplastic syndrome. The p53 pathway is activated by ribosome dysfunction, but the molecular basis for selective impairment of the erythroid lineage in disorders of ribosome function has not been determined. We found that p53 accumulates selectively in the erythroid lineage in primary human hematopoietic progenitor cells after expression of shRNAs targeting RPS14, the ribosomal protein gene deleted in the 5q-syndrome, or RPS19, the most commonly mutated gene in DBA. Induction of p53 led to lineage-specific accumulation of p21 and consequent cell cycle arrest in erythroid progenitor cells. Pharmacologic inhibition of p53 rescued the erythroid defect, whereas nutlin-3, a compound that activates p53 through inhibition of HDM2, selectively impaired erythropoiesis. In bone marrow biopsies from patients with DBA or del(5q) myelodysplastic syndrome, we found an accumulation of nuclear p53 staining in erythroid progenitor cells that was not present in control samples. Our findings indicate that the erythroid lineage has a low threshold for the induction of p53, providing a basis for the failure of erythropoiesis in the 5q-syndrome, DBA, and perhaps other bone marrow failure syndromes.
核糖体蛋白基因的单倍体不足与 Diamond-Blackfan 贫血(DBA)和骨髓增生异常综合征的 5q 综合征的病理生理学有关。核糖体功能障碍会激活 p53 途径,但核糖体功能障碍导致红细胞谱系选择性损伤的分子基础尚未确定。我们发现,在靶向 RPS14(5q 综合征缺失的核糖体蛋白基因)或 RPS19(DBA 中最常见突变的基因)的 shRNA 表达后,原发性人造血祖细胞中的 p53 选择性地在红细胞谱系中积累。p53 的诱导导致 p21 在红细胞祖细胞中特异性积累,继而导致细胞周期停滞。p53 的药理学抑制挽救了红细胞缺陷,而 nutlin-3,一种通过抑制 HDM2 激活 p53 的化合物,选择性地损害红细胞生成。在 DBA 或 del(5q)骨髓增生异常综合征患者的骨髓活检中,我们发现核 p53 染色在红细胞祖细胞中积累,而在对照样本中不存在。我们的发现表明,红细胞谱系对 p53 的诱导具有低阈值,为 5q 综合征、DBA 以及可能其他骨髓衰竭综合征中的红细胞生成失败提供了基础。
