Is serum‐derived exosomal hTERT transcript a marker of oncogenic activity in primary brain tumors? An exploratory study

Author:

Uziel Orit123ORCID,Kanner Andrew A.34,Beery Einat1,Lev Sapir4,Lahav Meir123,Horn‐Fichman Suzana35,Nof Sagi Har34,Laviv Yuseph34,Yust‐Katz S.36,Amiel Alexandra36,Shkara Ramez Abu4,Siddeeq Mustafa37,Levy‐Barda Adva8,Raanani Pia123,Sela Yaron9,Cohen Zvi37,Siegal Tali610

Affiliation:

1. The Felsenstein Medical Research Center Petah Tikva Israel

2. Institute of Hematology Davidoff Cancer Center, Rabin Medical Center Petah Tikva Israel

3. Sackler School of Medicine Tel‐Aviv University Tel Aviv Israel

4. Department of Neurosurgery Rabin Medical Center Petah Tikva Israel

5. Neuropathology, Department of Pathology Rabin Medical Center Petah Tikva Israel

6. Neurooncology Unit Davidoff Cancer Center, Rabin Medical Center Petah Tikva Israel

7. Department of Neurosurgery Sheba Medical Center Ramat‐Gan Israel

8. Biobank, Department of Pathology Rabin Medical Center Petah Tikva Israel

9. The Center of Internet Psychology Reichman University Herzliya Israel

10. Hebrew University and Medical School Jerusalem Israel

Abstract

AbstractBackgroundIn order to proliferate indefinitely, all tumors require a telomere maintenance mechanism. The expression of human telomerase reverse transcriptase (hTERT) enables telomere maintenance and provides cancer cells with limitless replicative potential. As such, it may serve as an attractive biomarker for oncogenic activity. This study explored whether a liquid biopsy that analyses blood derived exosomal hTERT transcript (e‐hTERT‐trans) may serve as such a biomarker in gliomas and meningiomas when compared to healthy controls.MethodsExosomes were isolated from the pre‐operative sera of patients' samples stored in the biobank of both Rabin and Sheba Medical Centers. The levels of e‐hTERT‐trans were measured in 81 healthy controls, 117 meningiomas, 17 low‐grade gliomas, and 61 glioblastomas. Clinical parameters of the patients were collected retrospectively and compared to the levels of the e‐hTERT‐trans.ResultsThe upper normal limit of controls e‐hTERT‐trans was 1.85 relative quantitation (RQ). The rate of detection increased with rising tumor grade and correlated with tumor recurrence in meningiomas: mean RQ without recurrence (2.17 ± 11.7) versus with recurrence (3.59 ± 4.42; p = 0.002). In glioblastomas, preoperative measurements correlated with tumor volume and with the disease course on serial sampling.ConclusionsWe demonstrated for the first time that the expression of e‐hTERT‐trans transcript can be measured in the serum of primary brain tumors. This exosomal marker carries the potential to serve as a biomarker once used in conjunction with other clinical and radiological parameters. Future studies are required to investigate whether the sensitivity could be augmented and whether it can be implemented into routine patients care.

Publisher

Wiley

Subject

Cancer Research,Radiology, Nuclear Medicine and imaging,Oncology

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