Multi-omic profiling of clear cell renal cell carcinoma identifies metabolic reprogramming associated with disease progression

Junyi Hu(Tongji Hospital), Shaogang Wang(Tongji Hospital), Yaxin Hou(Tongji Hospital), Zhaohui Chen(Union Hospital), Lilong Liu(Tongji Hospital), Ruizhi Li(Viva Biotech (China)), Nisha Li(Viva Biotech (China)), Lijie Zhou(First Affiliated Hospital of Zhengzhou University), Yu Yang(Indiana University School of Medicine), Liping Wang(Union Hospital), Liang Wang(Union Hospital), Xiong Yang(Union Hospital), Yichen Lei(Shanghai Jiao Tong University), Changqi Deng(Union Hospital), Yang Li(Tongji Hospital), Zhiyao Deng(Tongji Hospital), Yuhong Ding(Tongji Hospital), Yingchun Kuang(Tongji Hospital), Zhipeng Yao(Tongji Hospital), Yang Xun(Tongji Hospital), Fan Li(Tongji Hospital), Heng Li(Tongji Hospital), Jia Hu(Tongji Hospital), Zheng Liu(Tongji Hospital), Tao Wang(Tongji Hospital), Yi Hao(Huazhong University of Science and Technology), Xuanmao Jiao(Baruch S. Blumberg Institute), Wei Guan(Tongji Hospital), Zhen Tao(Tianjin Medical University Cancer Institute and Hospital), Shancheng Ren(Second Military Medical University), Ke Chen(Tongji Hospital)
Nature Genetics
February 15, 2024
Cited by 143Open Access
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Abstract

Clear cell renal cell carcinoma (ccRCC) is a complex disease with remarkable immune and metabolic heterogeneity. Here we perform genomic, transcriptomic, proteomic, metabolomic and spatial transcriptomic and metabolomic analyses on 100 patients with ccRCC from the Tongji Hospital RCC (TJ-RCC) cohort. Our analysis identifies four ccRCC subtypes including De-clear cell differentiated (DCCD)-ccRCC, a subtype with distinctive metabolic features. DCCD cancer cells are characterized by fewer lipid droplets, reduced metabolic activity, enhanced nutrient uptake capability and a high proliferation rate, leading to poor prognosis. Using single-cell and spatial trajectory analysis, we demonstrate that DCCD is a common mode of ccRCC progression. Even among stage I patients, DCCD is associated with worse outcomes and higher recurrence rate, suggesting that it cannot be cured by nephrectomy alone. Our study also suggests a treatment strategy based on subtype-specific immune cell infiltration that could guide the clinical management of ccRCC.


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