Identification of Adult Patients With Classical Dyskeratosis Congenita or Cryptic Telomere Biology Disorder by Telomere Length Screening Using Age-modified Criteria

Overview

Journal Hemasphere

Publisher Wiley

Specialty Hematology

Date 2023 Apr 25

PMID 37096215

Authors

Mareike Tometten

Martin Kirschner

Robert Meyer

Matthias Begemann

Insa Halfmeyer

Margherita Vieri

Kim Kricheldorf

Angela Maurer

Uwe Platzbecker

Markus Radsak

Philippe Schafhausen

Selim Corbacioglu

Britta Hochsmann

C Matthias Wilk

Claas Hinze

Jorg Chromik

Michael Heuser

Michael Kreuter

Steffen Koschmieder

Jens Panse

Susanne Isfort

Ingo Kurth

Tim H Brummendorf

Fabian Beier

Affiliations

Soon will be listed here.

Abstract

Telomere biology disorders (TBD) result from premature telomere shortening due to pathogenic germline variants in telomere maintenance-associated genes. In adults, TBD are characterized by mono/oligosymptomatic clinical manifestations (cryptic TBD) contributing to severe underdiagnosis. We present a prospective multi-institutional cohort study where telomere length (TL) screening was performed in either newly diagnosed patients with aplastic anemia (AA) or if TBD was clinically suspected by the treating physician. TL of 262 samples was measured via flow-fluorescence in situ hybridization (FISH). TL was considered suspicious once below the 10th percentile of normal individuals (standard screening) or if below 6.5 kb in patients >40 years (extended screening). In cases with shortened TL, next generation sequencing (NGS) for TBD-associated genes was performed. The patients referred fell into 6 different screening categories: (1) AA/paroxysmal nocturnal hemoglobinuria, (2) unexplained cytopenia, (3) dyskeratosis congenita, (4) myelodysplastic syndrome/acute myeloid leukemia, (5) interstitial lung disease, and (6) others. Overall, TL was found to be shortened in 120 patients (n = 86 standard and n = 34 extended screening). In 17 of the 76 (22.4%) standard patients with sufficient material for NGS, a pathogenic/likely pathogenic TBD-associated gene variant was identified. Variants of uncertain significance were detected in 17 of 76 (22.4%) standard and 6 of 29 (20.7%) extended screened patients. Expectedly, mutations were mainly found in and . In conclusion, TL measured by flow-FISH represents a powerful functional in vivo screening for an underlying TBD and should be performed in every newly diagnosed patient with AA as well as other patients with clinical suspicion for an underlying TBD in both children and adults.

Citing Articles

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Clinical manifestations of telomere biology disorders in adults.

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