Clinical relevance of NFYA splice variants in patients with acute myeloid leukaemia undergoing intensive chemotherapy

Author:

Yang Yi‐Tsung123ORCID,Yao Chi‐Yuan234ORCID,Kao Chein‐Jun3,Chiu Po‐Ju25,Lin Ming‐En23,Hou Hsin‐An3ORCID,Lin Chien‐Chin34ORCID,Chou Wen‐Chien34ORCID,Tien Hwei‐Fang36ORCID

Affiliation:

1. Division of Hematology, Department of Internal Medicine National Taiwan University Hospital Hsin‐Chu Branch Hsinchu Taiwan

2. Graduate Institute of Clinical Medicine College of Medicine, National Taiwan University Taipei Taiwan

3. Division of Hematology, Department of Internal Medicine National Taiwan University Hospital Taipei Taiwan

4. Department of Laboratory Medicine National Taiwan University Hospital Taipei Taiwan

5. Department of Hematological Oncology National Taiwan University Cancer Center Taipei Taiwan

6. Department of Internal Medicine Far‐Eastern Memorial Hospital New Taipei City Taiwan

Abstract

SummaryAberrant alternative splicing (AS) contributes to leukemogenesis, but reports on the clinical and biological implications of aberrant AS in acute myeloid leukaemia (AML) remain limited. Here, we used RNA‐seq to analyse AS in AML cells from 341 patients, comparing them to healthy CD34+ haematopoietic stem cells (HSCs). Our findings highlight distinct AS patterns in the nuclear transcription factor Y subunit alpha (NFYA) gene, with two main isoforms: NFYA‐L (Long) and NFYA‐S (Short), differing in exon 3 inclusion. Patients with lower NFYA‐L but higher NFYA‐S expression, termed NFYA‐S predominance, displayed more favourable characteristics and better outcomes following intensive chemotherapy, regardless of age and European LeukemiaNet risk classification, compared to those with higher NFYA‐L but lower NFYA‐S expression, termed NFYA‐L predominance. The prognostic effects were validated using The Cancer Genome Atlas cohort. Transcriptome analysis revealed upregulated cell cycle genes in NFYA‐S predominant cases, resembling those of active HSCs, demonstrating relative chemosensitivity. Conversely, NFYA‐L predominant cases, as observed in KMT2A‐rearranged leukaemia, were associated with relative chemoresistance. NFYA‐S overexpression in OCI‐AML3 cells promoted cell proliferation, S‐phase entry and increased cytarabine sensitivity, suggesting its clinical and therapeutic relevance in AML. Our study underscores NFYA AS as a potential prognostic biomarker in AML.

Funder

Ministry of Health and Welfare

Publisher

Wiley

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