DNA methylation patterns facilitate tracing the origin of neuroendocrine neoplasms.

Goeppert, Benjamin; Bohn, Eva-Marie; Nazarov, Petr V; de Mestier, Louis; Apostolidis, Leonidas; Schrimpf, Daniel; Ji, Junfang; Cros, Jérôme; Toth, Reka; Vogel, Monika Nadja; Brobeil, Alexander; Albrecht, Thomas; von Deimling, Andreas; Chang, De-Hua; Roessler, Stephanie; Perren, Aurel; Zhang, Yue; Charbel, Alphonse; Tabbakh, Danial; Singer, Stephan

doi:10.1038/s41467-025-65227-8

TY  - JOUR
AU  - Goeppert, Benjamin
AU  - Charbel, Alphonse
AU  - Toth, Reka
AU  - Zhang, Yue
AU  - Tabbakh, Danial
AU  - Albrecht, Thomas
AU  - Schrimpf, Daniel
AU  - de Mestier, Louis
AU  - Cros, Jérôme
AU  - Vogel, Monika Nadja
AU  - Chang, De-Hua
AU  - Bohn, Eva-Marie
AU  - Brobeil, Alexander
AU  - Ji, Junfang
AU  - Singer, Stephan
AU  - Nazarov, Petr V
AU  - Perren, Aurel
AU  - Apostolidis, Leonidas
AU  - von Deimling, Andreas
AU  - Roessler, Stephanie
TI  - DNA methylation patterns facilitate tracing the origin of neuroendocrine neoplasms.
JO  - Nature Communications
VL  - 16
IS  - 1
SN  - 2041-1723
CY  - [London]
PB  - Springer Nature
M1  - DKFZ-2025-02222
SP  - 9477
PY  - 2025
AB  - Neuroendocrine neoplasms (NEN) are thought to originate from diffuse neuroendocrine networks and therefore most frequently arise in the gastrointestinal tract and lungs. The liver is a frequent site of metastasis of NEN but also the existence of primary hepatic NEN has been proposed. Due to the impact on disease management, it is urgently required to discriminate the origin of hepatic NEN metastases and to identify clinically relevant subgroups. Using a comprehensive set of NEN (N = 212) from two independent cohorts, we show that the DNA methylation profiles of NEN of distinct anatomical localizations differ significantly and primary tumor-metastasis pairs cluster together, enabling the identification of the tumor origin. Furthermore, the subgroup of hepatic NEN without clinically detectable primary tumor, thus classified as primary hepatic NEN, does not form a distinct cluster by DNA methylation analysis but colocalizes with various subgroups of extrahepatic NEN. Organ-specific subtyping of NEN delineates a foregut-like epigenetic profile for hepatic NEN with unknown primary. We propose a classifier with high prediction accuracy for each of the different organ sites. In conclusion, our results demonstrate that DNA methylation profiling enables precise prediction of NEN origin and suggests that a substantial proportion of presumed primary hepatic NEN may in fact represent misclassified secondary hepatic NEN of unknown primary.
KW  - Humans
KW  - DNA Methylation
KW  - Neuroendocrine Tumors: genetics
KW  - Neuroendocrine Tumors: pathology
KW  - Liver Neoplasms: genetics
KW  - Liver Neoplasms: secondary
KW  - Female
KW  - Male
KW  - Middle Aged
KW  - Aged
KW  - Epigenesis, Genetic
KW  - Adult
KW  - Neoplasms, Unknown Primary: genetics
KW  - Neoplasms, Unknown Primary: pathology
LB  - PUB:(DE-HGF)16
C6  - pmid:41145514
DO  - DOI:10.1038/s41467-025-65227-8
UR  - https://inrepo02.dkfz.de/record/305552
ER  -

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