Institut National de la Santé et de la Recherche Médicale UMR866, 21000 Dijon, France;Labex LipSTIC and
Institut National de la Santé et de la Recherche Médicale UMR866, 21000 Dijon, France;Labex LipSTIC and.
Proc Natl Acad Sci U S A. 2014 Jul 22;111(29):10592-7. doi: 10.1073/pnas.1405546111. Epub 2014 Jul 7.
The hematopoietic system declines with age. Myeloid-biased differentiation and increased incidence of myeloid malignancies feature aging of hematopoietic stem cells (HSCs), but the mechanisms involved remain uncertain. Here, we report that 4-mo-old mice deleted for transcription intermediary factor 1γ (Tif1γ) in HSCs developed an accelerated aging phenotype. To reinforce this result, we also show that Tif1γ is down-regulated in HSCs during aging in 20-mo-old wild-type mice. We established that Tif1γ controls TGF-β1 receptor (Tgfbr1) turnover. Compared with young HSCs, Tif1γ(-/-) and old HSCs are more sensitive to TGF-β signaling. Importantly, we identified two populations of HSCs specifically discriminated by Tgfbr1 expression level and provided evidence of the capture of myeloid-biased (Tgfbr1(hi)) and myeloid-lymphoid-balanced (Tgfbr1(lo)) HSCs. In conclusion, our data provide a new paradigm for Tif1γ in regulating the balance between lymphoid- and myeloid-derived HSCs through TGF-β signaling, leading to HSC aging.
造血系统会随着年龄的增长而衰退。髓系偏向性分化和髓系恶性肿瘤发病率的增加是造血干细胞(HSCs)衰老的特征,但涉及的机制仍不清楚。在这里,我们报告说,造血干细胞中缺失转录中介因子 1γ(Tif1γ)的 4 月龄小鼠表现出加速衰老表型。为了加强这一结果,我们还表明,在 20 月龄野生型小鼠中,HSCs 随年龄增长而发生 Tif1γ下调。我们确定 Tif1γ 控制 TGF-β1 受体(Tgfbr1)的周转。与年轻的 HSCs 相比,Tif1γ(-/-)和老年 HSCs 对 TGF-β信号更敏感。重要的是,我们鉴定了两种特定的 HSC 群体,其特征是通过 Tgfbr1 表达水平区分的,并提供了捕获偏向髓系(Tgfbr1(hi))和髓系-淋巴系平衡(Tgfbr1(lo))HSC 的证据。总之,我们的数据提供了一个新的范式,即 Tif1γ 通过 TGF-β 信号调节淋巴系和髓系来源的 HSCs 之间的平衡,从而导致 HSC 衰老。