1. EZH2 Protein Expression Is Decreased in MDS and MDS/MPN and Correlated with EZH2 Mutation Status, Chromosomal 7 Abnormalities and Clinical Outcome
- Author
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Jinming Song, Lynn C. Moscinski, Rami S. Komrokji, Daihui Qin, Kathy L. McGraw, Pearlie K. Epling-Burnette, Najla Alali, Alan F. List, Ling Zhang, Johnny Nguyen, Jeffrey E. Lancet, Eric Padron, and David A. Sallman
- Subjects
medicine.medical_specialty ,Pathology ,Myeloid ,Myelodysplastic syndromes ,Immunology ,Cancer ,macromolecular substances ,Cell Biology ,Hematology ,Gene mutation ,Biology ,medicine.disease ,Biochemistry ,Gastroenterology ,Lymphoma ,medicine.anatomical_structure ,hemic and lymphatic diseases ,Internal medicine ,Statistical significance ,medicine ,Allele frequency ,Myeloproliferative neoplasm - Abstract
Background: The EZH2 gene (Enhancer of Zester homolog 2), located on chromosome (chr) 7q, is mutated in ~10% of patients with myelodysplastic syndromes (MDS) or MDS/myeloproliferative neoplasm (MDS/MPN). EZH2 gene mutations are associated with negative clinical outcomes; however, the role of EZH2 protein in MDS or MDS/MPN is largely unknown. In contrast to lymphomas or solid tumors in which expression is upregulated, decreased EZH2 mRNA expression was recently reported in 47% of MDS patients compared to normal controls and was more prevalent in patients with chr7 abnormalities. Furthermore, patients with decreased EZH2 expression lacking chr7 abnormalities had better overall survival (OS) (Cabrero M et al 2016). This study aims to explore EZH2 protein expression by immunohistochemistry (IHC) in MDS and MDS/MPN and the relationship to gene mutation and clinical outcome. Methods: Retrospective analysis (Institutional Review Board approved) of MDS or MDS/MPN cases seen at Moffitt Cancer Center between 7/2013-5/2015 with myeloid targeted, next generation sequencing (NGS) panel was performed. Bone marrow biopsies corresponding to NGS date were used for IHC. Nuclear EZH2 expression was assessed semi-quantitatively using an IHC score calculated by multiplying signal strength (0-3+) with percent positivity in hematopoietic cells. OS was considered duration between date of diagnosis and date of death. P-values were determined using Chi-squared, student t-test, ANOVA, or log-rank analysis with p Results: EZH2 mutations were identified in 69/620 MDS and MDS/MPN patients (11.13%). Of these, IHC was performed on 44 patients with EZH2 mutations including 33 MDS and 11 MDS/MPN [median age 74 years (y), male to female (M: F) ratio 2:1], and on 25 EZH2 wild type (WT) patients (median age 70.5 y, M:F ratio 2.1:1, including 22 MDS and 3 MDS/MPN). While mean EZH2 IHC score was reduced in all MDS cases compared to hematologically normal, WT controls (n=5), more controls are required to reach statistical significance (MDS IHC score 77.60±8.09 control score 102.50±14.00, p=0.167). However, there was significantly decreased expression in EZH2 mutant compared to EZH2 WT cases (IHC score, 0.5716±0.09 vs 1.113±0.11, p Conclusion: EZH2 mutation is associated with reduced protein expression, chr7 abnormalities and inferior OS in MDS and MDS/MPN. Analysis of a larger cohort is warranted to explore the role of EZH2 protein in the pathogenesis and natural disease history of MDS and MDS/MPN. Figure OS of patients with MDS and MDS/MPN with or without EZH2 mutation Figure. OS of patients with MDS and MDS/MPN with or without EZH2 mutation Disclosures Komrokji: Novartis: Consultancy, Speakers Bureau; Celgene: Membership on an entity's Board of Directors or advisory committees, Research Funding.
- Published
- 2016
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