Longitudinal evaluation of serum microRNAs as biomarkers for neuroblastoma burden and therapeutic p53 reactivation

Author:

Van Goethem Alan12,Deleu Jill12ORCID,Yigit Nurten12,Everaert Celine12,Moreno-Smith Myrthala3,Vasudevan Sanjeev A3,Zeka Fjoralba12,Demuynck Fleur12,Barbieri Eveline3,Speleman Frank24,Mestdagh Pieter12,Shohet Jason5,Vandesompele Jo12ORCID,Van Maerken Tom126

Affiliation:

1. OncoRNALab, Cancer Research Institute Ghent (CRIG) , Ghent, Belgium

2. Department of Biomolecular Medicine, Ghent University , Ghent, Belgium

3. Department of Pediatrics, Section of Hematology-Oncology, Texas Children's Cancer Center, Baylor College of Medicine , Houston, TX, USA

4. PPOL, Cancer Research Institute Ghent (CRIG) , Ghent, Belgium

5. Department of Pediatrics, Division of Pediatric Hematology-Oncology, University of Massachusetts Chan Medical School , Worcester, MA, USA

6. Department of Laboratory Medicine, AZ Groeninge , Kortrijk, Belgium

Abstract

Abstract Accurate assessment of treatment response and residual disease is indispensable for the evaluation of cancer treatment efficacy. However, performing tissue biopsies for longitudinal follow-up poses a major challenge in the management of solid tumours like neuroblastoma. In the present study, we evaluated whether circulating miRNAs are suitable to monitor neuroblastoma tumour burden and whether treatment-induced changes of miRNA abundance in the tumour are detectable in serum. We performed small RNA sequencing on longitudinally collected serum samples from mice carrying orthotopic neuroblastoma xenografts that were exposed to treatment with idasanutlin or temsirolimus. We identified 57 serum miRNAs to be differentially expressed upon xenograft tumour manifestation, out of which 21 were also found specifically expressed in the serum of human high-risk neuroblastoma patients. The murine serum levels of these 57 miRNAs correlated with tumour tissue expression and tumour volume, suggesting potential utility for monitoring tumour burden. In addition, we describe serum miRNAs that dynamically respond to p53 activation following treatment of engrafted mice with idasanutlin. We identified idasanutlin-induced serum miRNA expression changes upon one day and 11 days of treatment. By limiting to miRNAs with a tumour-related induction, we put forward hsa-miR-34a-5p as a potential pharmacodynamic biomarker of p53 activation in serum.

Funder

National Cancer Plan of the Belgian State

Kom op tegen Kanker

Bijzonder Onderzoeksfonds

Research Foundation Flanders

Publisher

Oxford University Press (OUP)

Subject

General Medicine

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