5ekn Citations

First comprehensive structural and biophysical analysis of MAPK13 inhibitors targeting DFG-in and DFG-out binding modes.

Yurtsever Z, Patel DA, Kober DL, Su A, Miller CA, Romero AG, Holtzman MJ, Brett TJ
Biochim Biophys Acta 1860 2335-2344 (2016)
Cited: 13 times
EuropePMC logo PMID: 27369736

Abstract

Background

P38 MAP kinases are centrally involved in mediating extracellular signaling in various diseases. While much attention has previously been focused on the ubiquitously expressed family member MAPK14 (p38α), recent studies indicate that family members such as MAPK13 (p38δ) display a more selective cellular and tissue expression and might therefore represent a specific kinase to target in certain diseases.

Methods

To facilitate the design of potent and specific inhibitors, we present here the structural, biophysical, and functional characterization of two new MAPK13-inhibitor complexes, as well as the first comprehensive structural, biophysical, and functional analysis of MAPK13 complexes with four different inhibitor compounds of greatly varying potency.

Results

These inhibitors display IC50 values either in the nanomolar range or micromolar range (>800-fold range). The nanomolar inhibitors exhibit much longer ligand-enzyme complex half-lives compared to the micromolar inhibitors as measured by biolayer interferometry. Crystal structures of the MAPK13 inhibitor complexes reveal that the nanomolar inhibitors engage MAPK13 in the DFG-out binding mode, while the micromolar inhibitors are in the DFG-in mode. Detailed structural and computational docking analyses suggest that this difference in binding mode engagement is driven by conformational restraints imposed by the chemical structure of the inhibitors, and may be fortified by an additional hydrogen bond to MAPK13 in the nanomolar inhibitors.

Conclusion

These studies provide a structural basis for understanding the differences in potency exhibited by these inhibitors.

Articles - 5ekn mentioned but not cited (4)

  1. First comprehensive structural and biophysical analysis of MAPK13 inhibitors targeting DFG-in and DFG-out binding modes. Yurtsever Z, Patel DA, Kober DL, Su A, Miller CA, Romero AG, Holtzman MJ, Brett TJ. Biochim Biophys Acta 1860 2335-2344 (2016)
  2. Profiling MAP kinase cysteines for targeted covalent inhibitor design. Liu R, Verma N, Henderson JA, Zhan S, Shen J. RSC Med Chem 13 54-63 (2022)
  3. RSK1 vs. RSK2 Inhibitory Activity of the Marine β-Carboline Alkaloid Manzamine A: A Biochemical, Cervical Cancer Protein Expression, and Computational Study. Mayer AMS, Hall ML, Lach J, Clifford J, Chandrasena K, Canton C, Kontoyianni M, Choo YM, Karan D, Hamann MT. Mar Drugs 19 506 (2021)
  4. New Antiproliferative Triflavanone from Thymelaea hirsuta-Isolation, Structure Elucidation and Molecular Docking Studies. Elhady SS, Abdelhameed RFA, El-Ayouty MM, Ibrahim AK, Habib ES, Elgawish MS, Hassanean HA, Safo MK, Nafie MS, Ahmed SA. Molecules 26 739 (2021)


Reviews citing this publication (6)

  1. p38γ and p38δ: From Spectators to Key Physiological Players. Cuenda A, Sanz-Ezquerro JJ. Trends Biochem Sci 42 431-442 (2017)
  2. The p38 MAPK Components and Modulators as Biomarkers and Molecular Targets in Cancer. García-Hernández L, García-Ortega MB, Ruiz-Alcalá G, Carrillo E, Marchal JA, García MÁ. Int J Mol Sci 23 370 (2021)
  3. Recent Advances in PROTACs for Drug Targeted Protein Research. Yao T, Xiao H, Wang H, Xu X. Int J Mol Sci 23 10328 (2022)
  4. A Special View of What Was Almost Forgotten: p38δ MAPK. Anton DB, Ducati RG, Timmers LFSM, Laufer S, Goettert MI. Cancers (Basel) 13 2077 (2021)
  5. Recent clinical findings on the role of kinase inhibitors in COVID-19 management. Malekinejad Z, Baghbanzadeh A, Nakhlband A, Baradaran B, Jafari S, Bagheri Y, Raei F, Montazersaheb S, Farahzadi R. Life Sci 306 120809 (2022)
  6. Synchrotron Big Data Science. Wang C, Steiner U, Sepe A. Small 14 e1802291 (2018)

Articles citing this publication (3)

  1. Differential PROTAC substrate specificity dictated by orientation of recruited E3 ligase. Smith BE, Wang SL, Jaime-Figueroa S, Harbin A, Wang J, Hamman BD, Crews CM. Nat Commun 10 131 (2019)
  2. circTNFRSF21, a newly identified circular RNA promotes endometrial carcinoma pathogenesis through regulating miR-1227-MAPK13/ATF2 axis. Liu Y, Chang Y, Cai Y. Aging (Albany NY) 12 6774-6792 (2020)
  3. MAPK13 stabilization via m6A mRNA modification limits anticancer efficacy of rapamycin. Kim J, Chun Y, Ramirez CB, Hoffner LA, Jung S, Jang KH, Rubtsova VI, Jang C, Lee G. J Biol Chem 299 105175 (2023)


Quick links