| Literature DB >> 30252677 |
Aditi Shastri1, Gaurav Choudhary1, Margarida Teixeira1, Shanisha Gordon-Mitchell1, Nandini Ramachandra1, Lumie Bernard1, Sanchari Bhattacharyya1, Robert Lopez1, Kith Pradhan1, Orsolya Giricz1, Goutham Ravipati1, Li-Fan Wong1, Sally Cole1, Tushar D Bhagat1, Jonathan Feld1, Yosman Dhar1, Matthias Bartenstein1, Victor J Thiruthuvanathan1, Amittha Wickrema2, B Hilda Ye1, David A Frank3, Andrea Pellagatti4, Jacqueline Boultwood4, Tianyuan Zhou5, Youngsoo Kim5, A Robert MacLeod5, P K Epling-Burnette6, Minwei Ye7, Patricia McCoon7, Richard Woessner7, Ulrich Steidl1, Britta Will1, Amit Verma1.
Abstract
Acute myeloid leukemia (AML) and myelodysplastic syndromes (MDS) are associated with disease-initiating stem cells that are not eliminated by conventional therapies. Transcriptomic analysis of stem and progenitor populations in MDS and AML demonstrated overexpression of STAT3 that was validated in an independent cohort. STAT3 overexpression was predictive of a shorter survival and worse clinical features in a large MDS cohort. High STAT3 expression signature in MDS CD34+ cells was similar to known preleukemic gene signatures. Functionally, STAT3 inhibition by a clinical, antisense oligonucleotide, AZD9150, led to reduced viability and increased apoptosis in leukemic cell lines. AZD9150 was rapidly incorporated by primary MDS/AML stem and progenitor cells and led to increased hematopoietic differentiation. STAT3 knockdown also impaired leukemic growth in vivo and led to decreased expression of MCL1 and other oncogenic genes in malignant cells. These studies demonstrate that STAT3 is an adverse prognostic factor in MDS/AML and provide a preclinical rationale for studies using AZD9150 in these diseases.Entities:
Keywords: Hematology; Hematopoietic stem cells; Signal transduction; Stem cells
Mesh:
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Year: 2018 PMID: 30252677 PMCID: PMC6264739 DOI: 10.1172/JCI120156
Source DB: PubMed Journal: J Clin Invest ISSN: 0021-9738 Impact factor: 14.808