- Mut, Melike;
- Adiguzel, Zelal;
- Cakir-Aktas, Canan;
- Hanalioğlu, Şahin;
- Gungor-Topcu, Gamze;
- Kiyga, Ezgi;
- Isikay, Ilkay;
- Sarac, Aydan;
- Soylemezoglu, Figen;
- Strobel, Thomas;
- Ampudia-Mesias, Elisabet;
- Cameron, Charles;
- Aslan, Tulay;
- Tekirdas, Eray;
- Hayran, Mutlu;
- Oguz, Kader;
- Henzler, Christine;
- Saydam, Nurten;
- Saydam, Okay
Glioblastoma is one of the most devastating neoplasms of the central nervous system. This study focused on the development of serum extracellular vesicle (EV)-based glioblastoma tumor marker panels that can be used in a clinic to diagnose glioblastomas and to monitor tumor burden, progression, and regression in response to treatment. RNA sequencing studies were performed using RNA isolated from serum EVs from both patients (n = 85) and control donors (n = 31). RNA sequencing results for preoperative glioblastoma EVs compared to control EVs revealed 569 differentially expressed genes (DEGs, 2XFC, FDR < 0.05). By using these DEGs, we developed serum-EV-based biomarker panels for the following glioblastomas: wild-type IDH1 (96% sensitivity/80% specificity), MGMT promoter methylation (91% sensitivity/73% specificity), p53 gene mutation (100% sensitivity/89% specificity), and TERT promoter mutation (89% sensitivity/100% specificity). This is the first study showing that serum-EV-based biomarker panels can be used to diagnose glioblastomas with a high sensitivity and specificity.