Ganpat Maroussia M P, Morales-Rodriguez Francisco, Pham Nhung, Lijnzaad Philip, de Souza Terezinha, Derakhshan Sepide, Fumagalli Arianna, Zeller Peter, Balwierz Aleksandra, Ayyildiz Dilara, van den Heuvel-Eibrink Marry M, de Krijger Ronald R, van Oudenaarden Alexander, Margaritis Thanasis, Chuva de Sousa Lopes Susana M, Drost Jarno
Princess Máxima Center for Pediatric Oncology, Heidelberglaan 25, Utrecht 3584 CS, the Netherlands.
Oncode Institute, Jaarbeursplein 6, Utrecht 3521 AL, the Netherlands.
iScience. 2025 Mar 1;28(4):112122. doi: 10.1016/j.isci.2025.112122. eCollection 2025 Apr 18.
Translocation renal cell carcinoma (tRCC) is a rare, aggressive kidney cancer primarily occurring in children. They are genetically defined by translocations involving MiT/TFE gene family members or . The biology underlying tRCC development remains poorly understood, partly due to the lack of representative experimental models. We utilized human kidney organoids, or tubuloids, to engineer a tRCC model by expressing one of the most common MiT/TFE fusions, SFPQ-TFE3. Fusion-expressing tubuloids adopt a tRCC-like phenotype and gene expression signature and grow as clear cell RCC upon xenotransplantation in mice. Genome-wide binding analysis suggests that SFPQ-TFE3 reprograms gene expression signatures by widespread, aberrant DNA binding. Combining these analyses with single-cell mRNA readouts reveals a derailed epithelial differentiation trajectory that is at the root of transformation toward tRCC. Our study demonstrates that SFPQ-TFE3 expression is sufficient to transform kidney epithelial cells into tRCC and defines the trajectories underlying malignant transformation.
易位性肾细胞癌(tRCC)是一种罕见的侵袭性肾癌,主要发生于儿童。其遗传学特征为涉及MiT/TFE基因家族成员的易位。tRCC发生的生物学机制仍知之甚少,部分原因是缺乏具有代表性的实验模型。我们利用人肾类器官(即肾小管类器官),通过表达最常见的MiT/TFE融合蛋白之一SFPQ-TFE3构建了一个tRCC模型。表达融合蛋白的肾小管类器官呈现出tRCC样表型和基因表达特征,并在小鼠体内异种移植后以透明细胞肾细胞癌的形式生长。全基因组结合分析表明,SFPQ-TFE3通过广泛的异常DNA结合重编程基因表达特征。将这些分析与单细胞mRNA读数相结合,揭示了一条偏离轨道的上皮分化轨迹,这是向tRCC转变的根源。我们的研究表明,SFPQ-TFE3的表达足以将肾上皮细胞转化为tRCC,并确定了恶性转化的轨迹。
Zotero 插件