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   the prognostic impact of wt1 expression levels, mutations, and snp rs16754 in aml patients: a retrospective cohort study  
   
نویسنده rostami shahrbano ,kazemi ahmad ,chahardouli bahram ,mohammadi saeed ,nikbakht mohsen ,alizadeh nasrin ,mousavi asadollah ,alimoghaddam kamran ,teremmahi ardestani majid
منبع journal of advances in medical and biomedical research - 2021 - دوره : 29 - شماره : 133 - صفحه:109 -117
چکیده    Background and objective: the clinical outcomes and treatment options for acute myeloid leukemia (aml) patients are highly dependent upon molecular markers. in this study, wilms tumor (wt1) (exons 7 and 9) mutations, snp rs16754, and wt1 expression levels in 130 random aml patients were screened; fmslike tyrosine kinase3 internal tandem duplication (flt3itd), nucleophosmin (npm1), and ccaat/enhancerbinding protein alpha (cebpa) mutations were also evaluated. material and methods: overall, 130 aml patients were recruited for our study. wt1 mutations were determined by sanger sequencing, and expression levels were determined by realtime pcr. the kaplanmeier method was used to calculate overall survival (os) and diseasefree survival (dfs). results: the frequency of wt1 mutations in the study population was 5.4%, and it did not affect overall survival (os) (p=0.98), diseasefree survival (dfs) (p=0.97), or complete remission (cr) rates in aml patients. the major allele of snp rs16754 in the current study was a. no significant differences were found for os (p=0.52), dfs (p=0.42), or complete remission rates among all snp rs16754 genotypes. the overexpression of wt1 was observed in 83% of patients at diagnosis. no significant difference was found for os (p=0.84), dfs (p=0.82), or complete remission rates between aml patients with high and low wt1 expression levels. conclusion: the results of the current study do not support wt1 mutation, snp rs16754, or wt1 overexpression at diagnosis, as they were found to be poor prognostic markers in aml patients.
کلیدواژه aml ,wt1 mutations ,wt1 expression ,snp rs16754 ,outcomes
آدرس tehran university of medical sciences, cell therapy and hematopoietic stem cell transplantation research center, iran, iran university of medical sciences, school of allied medical sciences, department of hematology, iran, tehran university of medical sciences, cell therapy and hematopoietic stem cell transplantation research center, iran, tehran university of medical sciences, cell therapy and hematopoietic stem cell transplantation research center, iran, tehran university of medical sciences, cell therapy and hematopoietic stem cell transplantation research center, iran, tehran university of medical sciences, cell therapy and hematopoietic stem cell transplantation research center, iran, tehran university of medical sciences, cell therapy and hematopoietic stem cell transplantation research center, iran, tehran university of medical sciences, cell therapy and hematopoietic stem cell transplantation research center, iran, hormozgan university of medical sciences, school of allied medical sciences, department of medical technology, iran
پست الکترونیکی majidardestani50@gmail.com
 
     
   
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