Detection of Circulating Tumor-specific DNA Methylation Markers in the Blood of Patients with Pituitary Tumors

Author:

Wells Michael,Asmaro Karam P.,Sabedot Thais S.,Malta Tathiane M.,Mosella Maritza S.,Nelson Kevin,Snyder James,deCarvalho Ana,Mukherjee Abir,Chitale Dhananjay,Robin Adam,Rosenblum Mark,Mikkelsen Thomas,Poisson Laila M.,Lee Ian Y.,Walbert Tobias,Bhan Arti,Kalkanis Steven,Rock Jack,Noushmehr Houtan,Castro Ana ValeriaORCID

Abstract

AbstractGenome-wide DNA methylation aberrations are pervasive and associated with clinicopathological features across pituitary tumors (PT) subtypes. The feasibility to detect CpG methylation abnormalities in circulating cell-free DNA (cfDNA) has been reported in central nervous system tumors other than PT. Here, we aimed to profile and identify methylome-based signatures in the serum of patients harboring PT (n =13). Our analysis indicated that serum cfDNA methylome from patients with PT are distinct from the counterparts in patients with other tumors (gliomas, meningiomas, colorectal carcinomas, n =134) and nontumor conditions (n = 4). Furthermore, the serum methylome patterns across PT was associated with functional status and adenohypophyseal cell lineage PT subtypes, recapitulating epigenetic features reported in PT-tissue. A machine learning algorithm using serum PT-specific signatures generated a score that distinguished PT from non-PT conditions with 100% accuracy in our validation set. These preliminary results underpin the potential clinical application of a liquid biopsy-based DNA methylation profiling as a noninvasive approach to identify clinically relevant epigenetic markers that can be used in the management of PT.

Publisher

Cold Spring Harbor Laboratory

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1. Cell-free DNA technologies for the analysis of brain cancer;British Journal of Cancer;2021-11-22

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