Pan-cancer analysis and experimental verification of its roles and clinical significance of SLC2A3 in kidney renal clear cell carcinoma
Zhaojie Lyu, Xueqi Zhang, Haichao Yuan, Qingshan Yang, Yu Yang, Zhengping Zhao, Guangsuo Wang, Liangkuan Bi

TL;DR
This study explores the role of SLC2A3 in kidney cancer, finding it promotes tumor growth and is linked to poor patient outcomes.
Contribution
The study identifies SLC2A3 as an oncogenic driver in KIRC through pan-cancer analysis and experimental validation.
Findings
SLC2A3 is upregulated in eight cancer types and linked to worse survival in several malignancies.
In KIRC, SLC2A3 is involved in hormone regulation, extracellular matrix remodeling, and pro-tumorigenic pathways.
SLC2A3 silencing reduced cell proliferation and migration in HK-2 and 786-O cell lines.
Abstract
Solute carrier family 2 member 3 (SLC2A3), a key glucose transporter, has been implicated in tumor metabolism and immune regulation, but its specific role in kidney renal clear cell carcinoma (KIRC) remains largely unclear. We conducted a comprehensive pan-cancer analysis of SLC2A3 using publicly available datasets. Its associations with patient prognosis, genomic heterogeneity, stemness features, immune-related genes, and immune cell infiltration were systematically explored. Functional enrichment and gene set enrichment analyses (GSEA) were conducted to explore the potential biological mechanisms in KIRC. Additionally, in vitro experiments using HK-2 and 786-O cell lines were carried out to validate the functional effects of SLC2A3. SLC2A3 expression was altered in multiple cancers, being upregulated in eight tumor types and downregulated in twenty. Elevated SLC2A3 levels were…
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Taxonomy
TopicsGenetic and Kidney Cyst Diseases · Renal cell carcinoma treatment · Ferroptosis and cancer prognosis
