Direct Reprogramming of Hepatocytes Into JAK/Stat-Dependent LGR5+ Liver Cells Able to Initiate Intrahepatic Cholangiocarcinoma.

IF 4 2区 医学 Q2 BIOTECHNOLOGY & APPLIED MICROBIOLOGY STEM CELLS Pub Date : 2024-04-15 DOI:10.1093/stmcls/sxae006
Diana Chaker, Christophe Desterke, Nicolas Moniaux, Mohamed-Amine Bani, Noufissa Oudrhiri, Jamila Faivre, Ali G Turhan, Annelise Bennaceur-Griscelli, Frank Griscelli
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Abstract

Somatic cells that have been partially reprogrammed by the factors Oct4, Sox2, Klf4, and cMyc (OSKM) have been demonstrated to be potentially tumorigenic in vitro and in vivo due to the acquisition of cancer-associated genomic alterations and the absence of OSKM clearance over time. In the present study, we obtained partially reprogrammed, SSEA1-negative cells by transducing murine hepatocytes with Δ1Δ3-deleted adenoviruses that expressed the 4 OSKM factors. We observed that, under long-term 2D and 3D culture conditions, hepatocytes could be converted into LGR5-positive cells with self-renewal capacity that was dependent on 3 cross-signaling pathways: IL6/Jak/Stat3, LGR5/R-spondin, and Wnt/β-catenin. Following engraftment in syngeneic mice, LGR5-positive cells that expressed the cancer markers CD51, CD166, and CD73 were capable of forming invasive and metastatic tumors reminiscent of intrahepatic cholangiocarcinoma (ICC): they were positive for CK19 and CK7, featured associations of cord-like structures, and contained cuboidal and atypical cells with dissimilar degrees of pleomorphism and mitosis. The LGR5+-derived tumors exhibited a highly vascularized stroma with substantial fibrosis. In addition, we identified pro-angiogenic factors and signaling pathways involved in neo-angiogenesis and vascular development, which represent potential new targets for anti-angiogenic strategies to overcome tumor resistance to current ICC treatments.

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直接将肝细胞重编程为 JAK/Stat 依赖性 LGR5+肝细胞,从而引发肝内胆管癌。
经Oct4、Sox2、Klf4和cMyc(OSKM)因子部分重编程的体细胞已被证实在体外和体内具有潜在的致瘤性,因为它们会获得与癌症相关的基因组改变,而且随着时间的推移OSKM不会被清除。在本研究中,我们用表达四种OSKM因子的Δ1Δ3缺失腺病毒转导小鼠肝细胞,获得了部分重编程的SSEA1阴性细胞。我们观察到,在长期二维和三维培养条件下,肝细胞可转化为 LGR5 阳性细胞,其自我更新能力取决于三种交叉信号通路:IL6/Jak/Stat3、LGR5/R-spondin 和 Wnt/β-catenin。表达癌标志物 CD51、CD166 和 CD73 的 LGR5 阳性细胞在接种到合成小鼠体内后,能够形成令人联想到肝内胆管癌(ICC)的侵袭性和转移性肿瘤:它们的 CK19 和 CK7 阳性,具有条索状结构,含有多形性和有丝分裂程度不同的立方体和非典型细胞。LGR5+衍生肿瘤表现出高度血管化的基质,并伴有大量纤维化。此外,我们还发现了参与新血管生成和血管发育的促血管生成因子和信号通路,这些因子和通路是抗血管生成策略的潜在新靶点,可克服肿瘤对当前 ICC 治疗的耐药性。
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来源期刊
STEM CELLS
STEM CELLS 医学-生物工程与应用微生物
CiteScore
10.30
自引率
1.90%
发文量
104
审稿时长
3 months
期刊介绍: STEM CELLS, a peer reviewed journal published monthly, provides a forum for prompt publication of original investigative papers and concise reviews. STEM CELLS is read and written by clinical and basic scientists whose expertise encompasses the rapidly expanding fields of stem and progenitor cell biology. STEM CELLS covers: Cancer Stem Cells, Embryonic Stem Cells/Induced Pluripotent Stem (iPS) Cells, Regenerative Medicine, Stem Cell Technology: Epigenetics, Genomics, Proteomics, and Metabonomics, Tissue-Specific Stem Cells, Translational and Clinical Research.
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