Telomere content and genomics of myeloid neoplasia by whole-genome sequencing

Guarnera, Luca; Meggendorfer, Manja; Westermann, Frank; Pagliuca, Simona; Haferlach, Torsten; Kubota, Yasuo; Bravo-Perez, Carlos; Maciejewski, Jaroslaw P; Hutter, Stephan; Gurnari, Carmelo; Kern, Wolfgang; Huang, Yimin; Feuerbach, Lars; Walter, Wencke; Visconte, Valeria; Kawashima, Naomi; Stainczyk, Sabine; Williams, Nakisha; Wahida, Adam; Orland, Mark David; LaFramboise, Thomas; Durmaz, Arda

doi:10.1182/blood.2025028644

Journal Article

DKFZ-2025-01943

Telomere content and genomics of myeloid neoplasia by whole-genome sequencing

Guarnera, L. ; Wahida, A. ; Gurnari, C. ; Hutter, S. ; Stainczyk, S.DKFZ* ; Williams, N. ; Durmaz, A. ; Kubota, Y. ; Bravo-Perez, C. ; Kawashima, N. ; Orland, M. D. ; Pagliuca, S. ; Huang, Y. ; LaFramboise, T. ; Visconte, V. ; Walter, W. ; Meggendorfer, M. ; Kern, W. ; Westermann, F.DKFZ* ; Feuerbach, L.DKFZ* ; Haferlach, T. ; Maciejewski, J. P.

2026
American Society of Hematology Washington, DC

Blood 147(2), 197-208 (2026) [10.1182/blood.2025028644]

Abstract: Telomere length shortening has been associated with genomic instability and acquisition of molecular lesions, but these processes have not been systematically studied across large cohorts of myeloid neoplasia (MN). As proof of concept for a novel, cross-validated WGS-based method of telomere content (TC) determination combined with mutations, transcriptomics, and functional assays, we studied TC in correlation with specific molecular features of a large cohort (n=1804) of MN patients including acute myeloid leukemia (AML) and myelodysplastic syndrome. When compared to healthy subjects and patients with non-clonal diseases such as persistent polyclonal B cell lymphocytosis, both MN and non-malignant controls with clonal disease, such as paroxysmal nocturnal hemoglobinuria and aplastic anemia, exhibited decreased TC. Furthermore, we show that TC is lowered in adult MN abrogating correlation with age with considerable TC diversification among certain morphologic and molecular subtypes. For instance, AML harbored the lowest TC. Furthermore, MN originating from a more mature cell of origin (e.g., APL), and those characterized by hyperproliferative driver mutations (e.g., RAS pathway genes) had lower TC, possibly indicating a loss of telomere maintenance capacity. In contrast, MN subtypes arising in a context of profound genetic alterations, such as TP53 mutations and complex karyotype, exhibited a relatively higher/preserved TC compared to other mutations. This phenomenon did not involve alternative lengthening processes but was rather consistent with an increased TC due to preserved activity of the telomerase complex. Our results describe a common and genotype-specific telomeric make-up of a large cohort of patients with MN providing a molecular benchmark for future therapeutic targeting of the telomere machinery.

Classification:

ddc:610

Note: 2026 Jan 8;147(2):197-208

Contributing Institute(s):

Research Program(s):

312 - Funktionelle und strukturelle Genomforschung (POF4-312) (POF4-312)

Appears in the scientific report 2025

Database coverage:
Medline

; BIOSIS Previews ; Biological Abstracts ; Clarivate Analytics Master Journal List ; Current Contents - Clinical Medicine ; Current Contents - Life Sciences ; Ebsco Academic Search ; Essential Science Indicators ; IF >= 20 ; JCR ; SCOPUS ; Science Citation Index Expanded ; Web of Science Core Collection

Click to display QR Code for this record

The record appears in these collections:
Document types > Articles > Journal Article
Public records
Publications database

Record created 2025-09-24, last modified 2026-01-09

Similar records

Rate this document:

(Not yet reviewed)

Add to personal basket
Export as Author List with IDs BibTeX (UTF-8), EndNote XML, EndNote Text, RIS, MARC, Print MARC, MARCXML, DC,
Request correction
Submit fulltext

guest :: login DKFZ
		Search		Submit		Personalize Your alerts Your baskets Your searches		Help