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The Nestin progenitor lineage is the compartment of origin for pancreatic intraepithelial neoplasia

机译:Nestin祖细胞系是胰腺上皮内瘤变的起源部位

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摘要

To determine the cell compartment in which initial oncogenic mutations occur in pancreatic ductal adenocarcinoma (PDAC), we generated a mouse model in which endogenous expression of mutated Kras (KrasG12D) was initially directed to a population of pancreatic exocrine progenitors characterized by the expression of Nestin. Targeting of oncogenic Kras to such a restricted cell compartment was sufficient for the formation of pancreatic intraepithelial neoplasias (PanINs), putative precursors to PDAC. PanINs appeared with the same grade and frequency as observed when KrasG12D was targeted to the whole pancreas by a Pdx1-driven Cre recombinase strategy. Thus, the Nestin cell lineage is highly responsive to Kras oncogenic activation and may represent the elusive progenitor population in which PDAC arises.
机译:为了确定在胰腺导管腺癌(PDAC)中发生初始致癌突变的细胞区室,我们生成了小鼠模型,其中突变的Kras(KrasG12D)的内源表达最初针对以Nestin表达为特征的胰腺外分泌祖细胞群。将致癌性Kras靶向这种受限的细胞区隔足以形成胰腺上皮内瘤变(PanINs)(PDAC的假定前体)。 PanIns出现的等级和频率与通过Pdx1驱动的Cre重组酶策略将KrasG12D靶向整个胰腺时观察到的等级和频率相同。因此,巢蛋白细胞谱系对Kras致癌激活高度敏感,并且可以代表其中出现PDAC的难以捉摸的祖细胞群。

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