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肝癌多组学研究揭示多种蛋白激酶A破坏作用会共同导致纤维板层型肝细胞癌。

Liver cancer multiomics reveals diverse protein kinase A disruptions convergently produce fibrolamellar hepatocellular carcinoma.

作者信息

Requena David, Medico Jack A, Soto-Ugaldi Luis F, Shirani Mahsa, Saltsman James A, Torbenson Michael S, Coffino Philip, Simon Sanford M

机构信息

Laboratory of Cellular Biophysics, The Rockefeller University, New York, NY, USA.

Division of Anatomic Pathology, Mayo Clinic, Rochester, MN, USA.

出版信息

Nat Commun. 2024 Dec 30;15(1):10887. doi: 10.1038/s41467-024-55238-2.

Abstract

Fibrolamellar Hepatocellular Carcinoma (FLC) is a rare liver cancer characterized by a fusion oncokinase of the genes DNAJB1 and PRKACA, the catalytic subunit of protein kinase A (PKA). A few FLC-like tumors have been reported showing other alterations involving PKA. To better understand FLC pathogenesis and the relationships among FLC, FLC-like, and other liver tumors, we performed a massive multi-omics analysis. RNA-seq data of 1412 liver tumors from FLC, hepatocellular carcinoma, hepatoblastoma and intrahepatic cholangiocarcinoma are analyzed, obtaining transcriptomic signatures unrestricted by experimental processing methods. These signatures reveal which dysregulations are unique to specific tumors and which are common to all liver cancers. Moreover, the transcriptomic FLC signature identifies a unifying phenotype for all FLC tumors regardless of how PKA was activated. We study this signature at multi-omics and single-cell levels in the first spatial transcriptomic characterization of FLC, identifying the contribution of tumor, normal, stromal, and infiltrating immune cells. Additionally, we study FLC metastases, finding small differences from the primary tumors.

摘要

纤维板层型肝细胞癌(FLC)是一种罕见的肝癌,其特征是DNAJB1和PRKACA基因发生融合,PRKACA是蛋白激酶A(PKA)的催化亚基。已有报道称少数FLC样肿瘤存在涉及PKA的其他改变。为了更好地理解FLC的发病机制以及FLC、FLC样肿瘤和其他肝脏肿瘤之间的关系,我们进行了大规模的多组学分析。分析了来自FLC、肝细胞癌、肝母细胞瘤和肝内胆管癌的1412例肝脏肿瘤的RNA测序数据,获得不受实验处理方法限制的转录组特征。这些特征揭示了哪些失调是特定肿瘤所特有的,哪些是所有肝癌所共有的。此外,转录组FLC特征为所有FLC肿瘤确定了一个统一的表型,而不管PKA是如何被激活的。我们在FLC的首次空间转录组学特征研究中,在多组学和单细胞水平上研究了这一特征,确定了肿瘤细胞、正常细胞、基质细胞和浸润免疫细胞的贡献。此外,我们研究了FLC转移灶,发现其与原发肿瘤存在细微差异。

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