The implications of abnormal signal patterns of break-apart FISH probes used in the diagnosis of bone and soft tissue tumours

The implications of abnormal signal patterns of break-apart FISH probes used in the diagnosis of bone and soft tissue tumours

Many subtypes of bone and soft tissue tumours harbour specific chromosome translocations leading to chimeric fusion genes. The identification of these specific fusion genes is the basis of molecular diagnoses in such tumours. Break-apart FISH is a robust method that is commonly used to identify thes...

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Bibliographic Details
Main Authors: Hongtao Ye, Fitim Berisha, Evie Rowles, Emani Munasinghe, Christopher Davies, Akanksha Farswan, Nischalan Pillay
Format: Article
Language:English
Published: Frontiers Media S.A. 2025-07-01
Series:Pathology and Oncology Research
Subjects:
FISH
abnormal signal pattern
break-apart probe
bone and soft tissue tumour
gene rearrangement
translocation
Online Access:https://www.por-journal.com/articles/10.3389/pore.2025.1612142/full
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Summary:Many subtypes of bone and soft tissue tumours harbour specific chromosome translocations leading to chimeric fusion genes. The identification of these specific fusion genes is the basis of molecular diagnoses in such tumours. Break-apart FISH is a robust method that is commonly used to identify these translocations and provide diagnostic support to histological interpretations. The signal patterns of the break-apart probes are usually easily interpreted. However, some cases show abnormal signal patterns leading to equivocal and challenging interpretation. The incidence of these abnormal patterns is largely unknown. Using a retrospective cohort we explored the incidence of abnormal signal patterns across common bone and soft tissue tumour types to raise awareness of this occurrence and to aid in the interpretation. In total, 1,087 bone and soft tissue tumours tested by break-apart probes were examined. The abnormal signal patterns were classified as deletion, additional copy and amplification, which were found at highest frequency in low-grade fibromyxoid sarcoma (32%, 6/19), and at moderate frequencies in those from alveolar rhabdomyosarcoma (10%, 9/94), nodular fasciitis (9%, 18/209), synovial sarcoma (8%, 17/207) and Ewing sarcoma/round cell sarcoma with EWSR1-non-ETS fusions (6%, 29/497). The lowest frequency was found in clear cell sarcoma (1%, 1/61). Despite the equivocal results from the abnormal signal patterns, the specific fusion genes were confirmed by orthogonal molecular techniques such as FISH with fusion probes, RT-PCR or next-generation sequencing.
ISSN:1532-2807

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