Identification and subsequent validation of transcriptomic signature associated with metabolic status in endometrial cancer

被引:3
|
作者
Sidorkiewicz, Iwona [1 ]
Jozwik, Maciej [2 ]
Buczynska, Angelika [1 ]
Erol, Anna [1 ]
Jozwik, Marcin [3 ]
Moniuszko, Marcin [4 ,5 ]
Jarzabek, Katarzyna [6 ]
Niemira, Magdalena [1 ]
Kretowski, Adam [1 ,7 ]
机构
[1] Med Univ Bialystok, Clin Res Ctr, Marii Sklodowskiej Curie 24a, PL-15276 Bialystok, Poland
[2] Med Univ Bialystok, Dept Gynecol & Gynecol Oncol, PL-15276 Bialystok, Poland
[3] Univ Warmia & Mazury, Dept Gynecol & Obstet, Coll Med, PL-10045 Olsztyn, Poland
[4] Med Univ Bialystok, Dept Regenerat Med & Immune Regulat, PL-15269 Bialystok, Poland
[5] Med Univ Bialystok, Dept Allergol & Internal Med, PL-15276 Bialystok, Poland
[6] Maria Sklodowska Curie Bialystok Oncol Ctr, Lab Genet & Mol Diagnost, PL-15027 Bialystok, Poland
[7] Med Univ Bialystok, Dept Endocrinol Diabetol & Internal Med, PL-15276 Bialystok, Poland
关键词
AMINO-ACID TRANSPORTERS; THERAPEUTIC TARGET; PYRUVATE-KINASE; CYCLIN A1; PHASE-I; EXPRESSION; GLUTAMATE; REVEALS; RUNX1; GENE;
D O I
10.1038/s41598-023-40994-w
中图分类号
O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];
学科分类号
07 ; 0710 ; 09 ;
摘要
Aberrant metabolism has been identified as a main driver of cancer. Profiling of metabolism-related pathways in cancer furthers the understanding of tumor plasticity and identification of potential metabolic vulnerabilities. In this prospective controlled study, we established transcriptomic profiles of metabolism-related pathways in endometrial cancer (EC) using a novel method, NanoString nCounter Technology. Fifty-seven ECs and 30 normal endometrial specimens were studied using the NanoString Metabolic Panel, further validated by qRT-PCR with a very high similarity. Statistical analyses were by GraphPad PRISM and Weka software. The analysis identified 11 deregulated genes (FDR & LE; 0.05; |FC|& GE; 1.5) in EC: SLC7A11; SLC7A5; RUNX1; LAMA4; COL6A3; PDK1; CCNA1; ENO1; PKM; NR2F1; and NAALAD2. Gene ontology showed direct association of these genes with 'central carbon metabolism (CCM) in cancer'. Thus, 'CCM in cancer' appears to create one of the main metabolic axes in EC. Further, transcriptomic data were functionally validated with drug repurposing on three EC cell lines, with several drug candidates suggested. These results lay the foundation for personalized therapeutic strategies in this cancer. Metabolic plasticity represents a promising diagnostic and therapeutic option in EC.
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页数:14
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