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Aldh1b1 表达定义了成年胰腺中的祖细胞,并且是 Kras 诱导的胰腺肿瘤所必需的。

Aldh1b1 expression defines progenitor cells in the adult pancreas and is required for Kras-induced pancreatic cancer.

机构信息

Paul Langerhans Institute Dresden, Helmholtz Center Munich at the University Clinic Carl Gustav Carus of Technische Universität Dresden, German Research Center for Environmental Health, Helmholtz Zentrum München, D-85764 Neuherberg, Germany.

German Centre for Diabetes Research (DZD e.V.), D-85764 Neuherberg, Germany.

出版信息

Proc Natl Acad Sci U S A. 2019 Oct 8;116(41):20679-20688. doi: 10.1073/pnas.1901075116. Epub 2019 Sep 23.

Abstract

The presence of progenitor or stem cells in the adult pancreas and their potential involvement in homeostasis and cancer development remain unresolved issues. Here, we show that mouse centroacinar cells can be identified and isolated by virtue of the mitochondrial enzyme Aldh1b1 that they uniquely express. These cells are necessary and sufficient for the formation of self-renewing adult pancreatic organoids in an Aldh1b1-dependent manner. Aldh1b1-expressing centroacinar cells are largely quiescent, self-renew, and, as shown by genetic lineage tracing, contribute to all 3 pancreatic lineages in the adult organ under homeostatic conditions. Single-cell RNA sequencing analysis of these cells identified a progenitor cell population, established its molecular signature, and determined distinct differentiation pathways to early progenitors. A distinct feature of these progenitor cells is the preferential expression of small GTPases, including Kras, suggesting that they might be susceptible to Kras-driven oncogenic transformation. This finding and the overexpression of Aldh1b1 in human and mouse pancreatic cancers, driven by activated Kras, prompted us to examine the involvement of Aldh1b1 in oncogenesis. We demonstrated genetically that ablation of completely abrogates tumor development in a mouse model of Kras-induced pancreatic cancer.

摘要

成体胰腺中祖细胞或干细胞的存在及其在维持内稳态和癌症发生中的潜在作用仍未得到解决。在这里,我们证明了鼠中央腺细胞可以通过其独特表达的线粒体酶 Aldh1b1 被识别和分离。这些细胞是 Aldh1b1 依赖性形成自我更新的成年胰腺类器官所必需和充分的。Aldh1b1 表达的中央腺细胞大多处于静止状态、自我更新,并且如遗传谱系追踪所示,在稳态条件下有助于成年器官中的所有 3 种胰腺谱系。对这些细胞进行单细胞 RNA 测序分析确定了一个祖细胞群体,建立了其分子特征,并确定了不同的分化途径到早期祖细胞。这些祖细胞的一个显著特征是小 GTPases 的优先表达,包括 Kras,这表明它们可能容易受到 Kras 驱动的致癌转化。这一发现以及激活 Kras 驱动的人源和鼠源胰腺癌细胞中 Aldh1b1 的过表达促使我们研究 Aldh1b1 在肿瘤发生中的作用。我们通过遗传手段证明, 在 Kras 诱导的胰腺癌小鼠模型中, 的缺失完全阻断了肿瘤的发展。

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