ATP Inhibits the Transcription Factor STAT5b

被引:6
|
作者
Berg, Angela [1 ]
Sperl, Bianca [2 ]
Berg, Thorsten [1 ]
机构
[1] Univ Leipzig, Inst Organ Chem, Johannisallee 29, D-04103 Leipzig, Germany
[2] Max Planck Inst Biochem, Dept Mol Biol, Klopferspitz 18, D-82152 Martinsried, Germany
来源
CHEMBIOCHEM | 2019年 / 20卷 / 17期
关键词
bioactive compounds; inhibitors; nucleotides; protein-protein interactions; SH2; domain; SIGNAL TRANSDUCER; SELECTIVE INHIBITORS; DISCOVERY; ACTIVATOR; CANCER; MODULATORS; DOMAINS; TARGETS; POTENT; ASSAY;
D O I
10.1002/cbic.201900173
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Although naturally occurring low-molecular-weight compounds have many known roles within the cell, these do not usually involve the direct inhibition of protein-protein interactions. Based on the results of high-throughput screening of a library of bioactive compounds and neurotransmitters, we report here that the four nucleoside triphosphates ATP, GTP, CTP and UTP inhibit the SH2 domain of the tumor-related transcription factor STAT5b. ATP and GTP are the most active nucleoside triphosphates and show specificity for STAT5b over STAT5a, STAT3, STAT6 and the p53-binding protein HDM2. As the inhibition constant of ATP against STAT5b is significantly lower than published values for the intracellular ATP concentration, our data suggest that ATP might inhibit the protein-protein interactions of STAT5b in living cells.
引用
收藏
页码:2227 / 2231
页数:5
相关论文
共 50 条
  • [21] Hypoxia upregulates Hsp90α expression via STAT5b in cancer cells
    Pak, Se Hyung
    Joung, Youn Hee
    Park, Jin Hee
    Lim, Eun Joung
    Darvin, Pramod
    Na, Yoon Mi
    Hong, Dae Young
    Lee, Boram
    Hwang, Tae Sook
    Park, Taegyu
    Ye, Sang-Kyu
    Moon, Eon-Soo
    Cho, Byung Wook
    Park, Kyung Do
    Lee, Hak Kyo
    Chung, Ill-Min
    Yang, Young Mok
    INTERNATIONAL JOURNAL OF ONCOLOGY, 2012, 41 (01) : 161 - 168
  • [22] A Novel Missense Mutation in the SH2 Domain of the STAT5B Gene Results in a Transcriptionally Inactive STAT5b Associated with Severe IGF-I Deficiency, Immune Dysfunction, and Lack of Pulmonary Disease
    Scaglia, Paula A.
    Martinez, Alicia S.
    Feigerlova, Eva
    Bezrodnik, Liliana
    Isabel Gaillard, Maria
    Di Giovanni, Daniela
    Gabriela Ballerini, Maria
    Jasper, Hector G.
    Heinrich, Juan J.
    Fang, Peng
    Domene, Horacio M.
    Rosenfeld, Ron G.
    Hwa, Vivian
    JOURNAL OF CLINICAL ENDOCRINOLOGY & METABOLISM, 2012, 97 (05) : E830 - E839
  • [23] The structural influence of the oncogenic driver mutation N642H in the STAT5B SH2 domain
    Haas-Neill, Liam
    Meneksedag-Erol, Deniz
    Chaudhry, Ayesha
    Novoselova, Masha
    Ashraf, Qirat F.
    de Araujo, Elvin D.
    Wilson, Derek J.
    Rauscher, Sarah
    PROTEIN SCIENCE, 2025, 34 (01)
  • [24] STAT3 and STAT5b polymorphism contributes to breast cancer risk and clinical outcomes
    Zhao, Ling
    Zhang, Qingyuan
    Luan, Xin
    Huang, Xu
    Zhao, Shu
    Zhao, Hong
    INTERNATIONAL JOURNAL OF CLINICAL AND EXPERIMENTAL PATHOLOGY, 2015, 8 (02): : 2033 - 2038
  • [25] Constitutively Active STAT5b Feminizes Mouse Liver Gene Expression
    Lau-Corona, Dana
    Ma, Hong
    Vergato, Cameron
    Sarmento-Cabral, Andre
    Del Rio-Moreno, Mercedes
    Kineman, Rhonda D.
    Waxman, David J.
    ENDOCRINOLOGY, 2022, 163 (05)
  • [26] STAT5B leukemic mutations, altering SH2 tyrosine 665, have opposing impacts on immune gene programs
    Lee, Hye Kyung
    Chen, Jichun
    Philips, Rachael L.
    Lee, Sung-Gwon
    Feng, Xingmin
    Wu, Zhijie
    Liu, Chengyu
    Schultz, Aaron B.
    Dalzell, Molly
    Meggendorfer, Manja
    Haferlach, Claudia
    Birnbaum, Foster
    Sexton, Joel A.
    Keating, Amy E.
    O'Shea, John J.
    Young, Neal S.
    Villarino, Alejandro V.
    Furth, Priscilla A.
    Hennighausen, Lothar
    LIFE SCIENCE ALLIANCE, 2025, 8 (07)
  • [27] A novel role for signal transducer and activator of transcription 5b (STAT5b) in β1-integrin-mediated human breast cancer cell migration
    Bernaciak, Teresa M.
    Zareno, Jessica
    Parsons, J. Thomas
    Silva, Corinne M.
    BREAST CANCER RESEARCH, 2009, 11 (04):
  • [28] Activating mutations of STAT5B and STAT3 in lymphomas derived from γδ-T or NK cells
    Kucuk, Can
    Jiang, Bei
    Hu, Xiaozhou
    Zhang, Wenyan
    Chan, John K. C.
    Xiao, Wenming
    Lack, Nathan
    Alkan, Can
    Williams, John C.
    Avery, Kendra N.
    Kavak, Pinar
    Scuto, Anna
    Sen, Emel
    Gaulard, Philippe
    Staudt, Lou
    Iqbal, Javeed
    Zhang, Weiwei
    Cornish, Adam
    Gong, Qiang
    Yang, Qunpei
    Sun, Hong
    d'Amore, Francesco
    Leppa, Sirpa
    Liu, Weiping
    Fu, Kai
    de Leval, Laurence
    McKeithan, Timothy
    Chan, Wing C.
    NATURE COMMUNICATIONS, 2015, 6
  • [29] Discovery of chromone-based inhibitors of the transcription factor STAT5
    Mueller, Judith
    Sperl, Bianca
    Reindl, Wolfgang
    Kiessling, Anke
    Berg, Thorsten
    CHEMBIOCHEM, 2008, 9 (05) : 723 - 727
  • [30] Transcription Factor Stat3 Stimulates Metastatic Behavior of Human Prostate Cancer Cells in Vivo, whereas Stat5b Has a Preferential Role in the Promotion of Prostate Cancer Cell Viability and Tumor Growth
    Gu, Lei
    Dagvadorj, Ayush
    Lutz, Jacqueline
    Leiby, Benjamin
    Bonuccelli, Gloria
    Lisanti, Michael P.
    Addya, Sankar
    Fortina, Paolo
    Dasgupta, Abhijit
    Hyslop, Terry
    Bubendorf, Lukas
    Nevalainen, Marja T.
    AMERICAN JOURNAL OF PATHOLOGY, 2010, 176 (04) : 1959 - 1972
12345