Proteomic and phosphoproteomic landscapes of acute myeloid leukemia

磷酸化 生物 髓系白血病 磷酸蛋白质组学 癌症研究 白血病 蛋白质磷酸化 计算生物学 医学 免疫学 细胞生物学 蛋白激酶A
作者
Michael H. Kramer,Qiang Zhang,Robert W. Sprung,Ryan B. Day,Petra Erdmann-Gilmore,Yang Li,Ziheng Xu,Nichole Helton,Daniel R. George,Yiling Mi,Peter Westervelt,Jacqueline E. Payton,Sai Mukund Ramakrishnan,Christopher A. Miller,Daniel C. Link,John F. DiPersio,Matthew J. Walter,R. Reid Townsend,Timothy J. Ley
出处
期刊:Blood [Elsevier BV]
卷期号:140 (13): 1533-1548 被引量:124
标识
DOI:10.1182/blood.2022016033
摘要

We have developed a deep-scale proteome and phosphoproteome database from 44 representative acute myeloid leukemia (AML) patients from the LAML TCGA dataset and 6 healthy bone marrow-derived controls. After confirming data quality, we orthogonally validated several previously undescribed features of AML revealed by the proteomic data. We identified examples of posttranscriptionally regulated proteins both globally (ie, in all AML samples) and also in patients with recurrent AML driver mutations. For example, samples with IDH1/2 mutations displayed elevated levels of the 2-oxoglutarate-dependent histone demethylases KDM4A/B/C, despite no changes in messenger RNA levels for these genes; we confirmed this finding in vitro. In samples with NPMc mutations, we identified several nuclear importins with posttranscriptionally increased protein abundance and showed that they interact with NPMc but not wild-type NPM1. We identified 2 cell surface proteins (CD180 and MRC1/CD206) expressed on AML blasts of many patients (but not healthy CD34+ stem/progenitor cells) that could represent novel targets for immunologic therapies and confirmed these targets via flow cytometry. Finally, we detected nearly 30 000 phosphosites in these samples; globally, AML samples were associated with the abnormal phosphorylation of specific residues in PTPN11, STAT3, AKT1, and PRKCD. FLT3-TKD samples were associated with increased phosphorylation of activating tyrosines on the cytoplasmic Src-family tyrosine kinases FGR and HCK and related signaling proteins. PML-RARA-initiated AML samples displayed a unique phosphorylation signature, and TP53-mutant samples showed abundant phosphorylation of serine-183 on TP53 itself. This publicly available database will serve as a foundation for further investigations of protein dysregulation in AML pathogenesis.
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