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在表达易位的 hiPSC 来源的内皮细胞中重现血管肿瘤。

Vascular Tumor Recapitulated in Endothelial Cells from hiPSCs Engineered to Express the Translocation.

机构信息

Department of Pathology, Leiden University Medical Center, 2333 ZA Leiden, the Netherlands.

Central Laboratory Animal Facility, Leiden University Medical Center, 2333 ZA Leiden, the Netherlands.

出版信息

Cell Rep Med. 2020 Dec 22;1(9):100153. doi: 10.1016/j.xcrm.2020.100153.

Abstract

Chromosomal translocations are prevalent among soft tissue tumors, including those of the vasculature such as pseudomyogenic hemangioendothelioma (PHE). PHE shows endothelial cell (EC) features and has a tumor-specific t(7;19)(q22;q13) SERPINE1-FOSB translocation, but is difficult to study as no primary tumor cell lines have yet been derived. Here, we engineer the PHE chromosomal translocation into human induced pluripotent stem cells (hiPSCs) using CRISPR/Cas9 and differentiate these into ECs (hiPSC-ECs) to address this. Comparison of parental with PHE hiPSC-ECs shows (1) elevated expression of FOSB, (2) higher proliferation and more tube formation but lower endothelial barrier function, (3) invasive growth and abnormal vessel formation in mice after transplantation, and (4) specific transcriptome alterations reflecting PHE and indicating PI3K-Akt and MAPK signaling pathways as possible therapeutic targets. The modified hiPSC-ECs thus recapitulate functional features of PHE and demonstrate how these translocation models can be used to understand tumorigenic mechanisms and identify therapeutic targets.

摘要

染色体易位在软组织肿瘤中很常见,包括脉管系统的肿瘤,如假肌源性血管内皮细胞瘤(PHE)。PHE 表现出内皮细胞(EC)的特征,并且具有肿瘤特异性的 t(7;19)(q22;q13)SERPINE1-FOSB 易位,但由于尚未衍生出原发性肿瘤细胞系,因此难以研究。在这里,我们使用 CRISPR/Cas9 将 PHE 染色体易位工程引入人诱导多能干细胞(hiPSC)中,并将其分化为 EC(hiPSC-EC)来解决这个问题。与 PHE hiPSC-ECs 的亲本细胞相比,(1)FOSB 表达升高,(2)增殖和管状形成增加,但内皮屏障功能降低,(3)移植后在小鼠中侵袭性生长和异常血管形成,以及(4)反映 PHE 的特定转录组改变,并表明 PI3K-Akt 和 MAPK 信号通路可能是治疗靶点。因此,修饰后的 hiPSC-ECs 再现了 PHE 的功能特征,并展示了这些易位模型如何用于理解肿瘤发生机制和确定治疗靶点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/595f/7762773/236dd55eee21/fx1.jpg

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