Identification of Novel Small Molecule Ligands for JAK2 Pseudokinase Domain

Anniina T. Virtanen; Teemu Haikarainen; Parthasarathy Sampathkumar; Maaria Palmroth; Sanna Liukkonen; Jianping Liu; Natalia Nekhotiaeva; Stevan R. Hubbard; Olli Silvennoinen

doi:10.3390/ph16010075

Identification of Novel Small Molecule Ligands for JAK2 Pseudokinase Domain

Anniina T. Virtanen^*
, Teemu Haikarainen
, Parthasarathy Sampathkumar
, Maaria Palmroth
, Sanna Liukkonen
, Jianping Liu
, Natalia Nekhotiaeva
, Stevan R. Hubbard
, Olli Silvennoinen^*

^*Tämän työn vastaava kirjoittaja

Kliinisen mikrobiologian yksikkö

Tutkimustuotos: Artikkeli › Tieteellinen › vertaisarvioitu

17 Sitaatiot (Scopus)

49 Lataukset (Pure)

Abstrakti

Hyperactive mutation V617F in the JAK2 regulatory pseudokinase domain (JH2) is prevalent in patients with myeloproliferative neoplasms. Here, we identified novel small molecules that target JH2 of JAK2 V617F and characterized binding via biochemical and structural approaches. Screening of 107,600 small molecules resulted in identification of 55 binders to the ATP-binding pocket of recombinant JAK2 JH2 V617F protein at a low hit rate of 0.05%, which indicates unique structural characteristics of the JAK2 JH2 ATP-binding pocket. Selected hits and structural analogs were further assessed for binding to JH2 and JH1 (kinase) domains of JAK family members (JAK1-3, TYK2) and for effects on MPN model cell viability. Crystal structures were determined with JAK2 JH2 wild-type and V617F. The JH2-selective binders were identified in diaminotriazole, diaminotriazine, and phenylpyrazolo-pyrimidone chemical entities, but they showed low-affinity, and no inhibition of MPN cells was detected, while compounds binding to both JAK2 JH1 and JH2 domains inhibited MPN cell viability. X-ray crystal structures of protein-ligand complexes indicated generally similar binding modes between the ligands and V617F or wild-type JAK2. Ligands of JAK2 JH2 V617F are applicable as probes in JAK-STAT research, and SAR optimization combined with structural insights may yield higher-affinity inhibitors with biological activity.

Alkuperäiskieli	Englanti
Artikkeli	75
Sivumäärä	17
Julkaisu	Pharmaceuticals
Vuosikerta	16
Numero	1
DOI - pysyväislinkit	https://doi.org/10.3390/ph16010075
Tila	Julkaistu - tammik. 2023
OKM-julkaisutyyppi	A1 Alkuperäisartikkeli tieteellisessä aikakauslehdessä

Rahoitus

This research was funded by Novo Nordisk Foundation, Academy of Finland, Sigrid Jusélius Foundation, Finnish Cancer Foundation, Jane and Aatos Erkko Foundation, Tampere Tuberculosis Foundation, Competitive State Research Financing of the Expert Responsibility area of Tampere University Hospital and Doctoral Programme of Medicine and Life Sciences at Tampere University. This study was supported by grants from Academy of Finland, Sigrid Jusélius Foundation, Jane and Aatos Erkko Foundation, Finnish Cancer Foundation, Tampere Tuberculosis Foundation, and Pirkanmaa hospital district competitive research funding. T.H. reports grant from Novo Nordisk Foundation. P.S. is currently an employee of Surrozen Inc. M.P. is currently an employee of MedEngine Oy. S.R.H. is a co-founder and scientific advisory board member of Ajax Therapeutics, Inc. O.S. reports lecture fees from Pfizer, Abbvie and Novartis, is a member of scientific advisory board of Ajax Therapeutics and chair of scientific advisory board of Finnish hematology registry and biobank. O.S. holds patents on JAK kinases, US Patent no. 5,728,536, US patent no. 8,841,078, AU 2011214254, CAN 2789186, and EPO 11741946.5, and reports royalties or licenses from St Jude Children’s Research Hospital and stock option for Ajax Therapeutics. A.T.V, S.L., J.L. and N.N. declare no competing interests.

Julkaisufoorumi-taso

Jufo-taso 1

!!ASJC Scopus subject areas

Molecular Medicine
Pharmaceutical Science
Drug Discovery

Pääsy asiakirjaan

10.3390/ph16010075Lisenssi: CC BY

pharmaceuticals-16-00075Final published version, 2,23 MBLisenssi: CC BY

https://urn.fi/URN:NBN:fi:tuni-202303293303Lisenssi: CC BY

Crystal structure of JAK2 JH2 (pseudokinase domain) in complex with Reversine
Virtanen, A. T. (Creator), Haikarainen, T. (Creator), Sampathkumar, P. (Creator), Palmroth, M. (Creator), Liukkonen, S. (Creator), Liu, J. (Creator), Nekhotiaeva, N. (Creator), Hubbard, S. R. (Creator) & Silvennoinen, O. (Creator), Protein Data Bank (PDB), 1 helmik. 2023
DOI - pysyväislinkki: 10.2210/pdb8EX1/pdb
Tietoaineisto: Dataset
Crystal structure of JAK2 JH2 (pseudokinase domain) in complex with CDK2-IV
Virtanen, A. T. (Creator), Haikarainen, T. (Creator), Sampathkumar, P. (Creator), Palmroth, M. (Creator), Liukkonen, S. (Creator), Liu, J. (Creator), Nekhotiaeva, N. (Creator), Hubbard, S. R. (Creator) & Silvennoinen, O. (Creator), Protein Data Bank (PDB), 1 helmik. 2023
DOI - pysyväislinkki: 10.2210/pdb8EX0/pdb
Tietoaineisto: Dataset
Crystal structure of JAK2 JH2-V617F in complex with JNJ-7706621
Virtanen, A. T. (Creator), Haikarainen, T. (Creator), Sampathkumar, P. (Creator), Palmroth, M. (Creator), Liukkonen, S. (Creator), Liu, J. (Creator), Nekhotiaeva, N. (Creator), Hubbard, S. R. (Creator) & Silvennoinen, O. (Creator), Protein Data Bank (PDB), 1 helmik. 2023
DOI - pysyväislinkki: 10.2210/pdb8B99/pdb
Tietoaineisto: Dataset

Siteeraa tätä

@article{2d67f1f3f8a547e8bc7b94fd91dd1543,

title = "Identification of Novel Small Molecule Ligands for JAK2 Pseudokinase Domain",

abstract = "Hyperactive mutation V617F in the JAK2 regulatory pseudokinase domain (JH2) is prevalent in patients with myeloproliferative neoplasms. Here, we identified novel small molecules that target JH2 of JAK2 V617F and characterized binding via biochemical and structural approaches. Screening of 107,600 small molecules resulted in identification of 55 binders to the ATP-binding pocket of recombinant JAK2 JH2 V617F protein at a low hit rate of 0.05\%, which indicates unique structural characteristics of the JAK2 JH2 ATP-binding pocket. Selected hits and structural analogs were further assessed for binding to JH2 and JH1 (kinase) domains of JAK family members (JAK1-3, TYK2) and for effects on MPN model cell viability. Crystal structures were determined with JAK2 JH2 wild-type and V617F. The JH2-selective binders were identified in diaminotriazole, diaminotriazine, and phenylpyrazolo-pyrimidone chemical entities, but they showed low-affinity, and no inhibition of MPN cells was detected, while compounds binding to both JAK2 JH1 and JH2 domains inhibited MPN cell viability. X-ray crystal structures of protein-ligand complexes indicated generally similar binding modes between the ligands and V617F or wild-type JAK2. Ligands of JAK2 JH2 V617F are applicable as probes in JAK-STAT research, and SAR optimization combined with structural insights may yield higher-affinity inhibitors with biological activity.",

keywords = "cytokine signaling, JAK inhibitor, JAK2 V617F, myeloproliferative neoplasm, pseudokinase",

author = "Virtanen, \{Anniina T.\} and Teemu Haikarainen and Parthasarathy Sampathkumar and Maaria Palmroth and Sanna Liukkonen and Jianping Liu and Natalia Nekhotiaeva and Hubbard, \{Stevan R.\} and Olli Silvennoinen",

note = "Funding Information: This research was funded by Novo Nordisk Foundation, Academy of Finland, Sigrid Jus{\'e}lius Foundation, Finnish Cancer Foundation, Jane and Aatos Erkko Foundation, Tampere Tuberculosis Foundation, Competitive State Research Financing of the Expert Responsibility area of Tampere University Hospital and Doctoral Programme of Medicine and Life Sciences at Tampere University. Funding Information: This study was supported by grants from Academy of Finland, Sigrid Jus{\'e}lius Foundation, Jane and Aatos Erkko Foundation, Finnish Cancer Foundation, Tampere Tuberculosis Foundation, and Pirkanmaa hospital district competitive research funding. T.H. reports grant from Novo Nordisk Foundation. P.S. is currently an employee of Surrozen Inc. M.P. is currently an employee of MedEngine Oy. S.R.H. is a co-founder and scientific advisory board member of Ajax Therapeutics, Inc. O.S. reports lecture fees from Pfizer, Abbvie and Novartis, is a member of scientific advisory board of Ajax Therapeutics and chair of scientific advisory board of Finnish hematology registry and biobank. O.S. holds patents on JAK kinases, US Patent no. 5,728,536, US patent no. 8,841,078, AU 2011214254, CAN 2789186, and EPO 11741946.5, and reports royalties or licenses from St Jude Children{\textquoteright}s Research Hospital and stock option for Ajax Therapeutics. A.T.V, S.L., J.L. and N.N. declare no competing interests. Publisher Copyright: {\textcopyright} 2023 by the authors.",

year = "2023",

month = jan,

doi = "10.3390/ph16010075",

language = "English",

volume = "16",

journal = "Pharmaceuticals",

issn = "1424-8247",

publisher = "Multidisciplinary Digital Publishing Institute (MDPI)",

number = "1",

}

TY - JOUR

T1 - Identification of Novel Small Molecule Ligands for JAK2 Pseudokinase Domain

AU - Virtanen, Anniina T.

AU - Haikarainen, Teemu

AU - Sampathkumar, Parthasarathy

AU - Palmroth, Maaria

AU - Liukkonen, Sanna

AU - Liu, Jianping

AU - Nekhotiaeva, Natalia

AU - Hubbard, Stevan R.

AU - Silvennoinen, Olli

N1 - Funding Information: This research was funded by Novo Nordisk Foundation, Academy of Finland, Sigrid Jusélius Foundation, Finnish Cancer Foundation, Jane and Aatos Erkko Foundation, Tampere Tuberculosis Foundation, Competitive State Research Financing of the Expert Responsibility area of Tampere University Hospital and Doctoral Programme of Medicine and Life Sciences at Tampere University. Funding Information: This study was supported by grants from Academy of Finland, Sigrid Jusélius Foundation, Jane and Aatos Erkko Foundation, Finnish Cancer Foundation, Tampere Tuberculosis Foundation, and Pirkanmaa hospital district competitive research funding. T.H. reports grant from Novo Nordisk Foundation. P.S. is currently an employee of Surrozen Inc. M.P. is currently an employee of MedEngine Oy. S.R.H. is a co-founder and scientific advisory board member of Ajax Therapeutics, Inc. O.S. reports lecture fees from Pfizer, Abbvie and Novartis, is a member of scientific advisory board of Ajax Therapeutics and chair of scientific advisory board of Finnish hematology registry and biobank. O.S. holds patents on JAK kinases, US Patent no. 5,728,536, US patent no. 8,841,078, AU 2011214254, CAN 2789186, and EPO 11741946.5, and reports royalties or licenses from St Jude Children’s Research Hospital and stock option for Ajax Therapeutics. A.T.V, S.L., J.L. and N.N. declare no competing interests. Publisher Copyright: © 2023 by the authors.

PY - 2023/1

Y1 - 2023/1

N2 - Hyperactive mutation V617F in the JAK2 regulatory pseudokinase domain (JH2) is prevalent in patients with myeloproliferative neoplasms. Here, we identified novel small molecules that target JH2 of JAK2 V617F and characterized binding via biochemical and structural approaches. Screening of 107,600 small molecules resulted in identification of 55 binders to the ATP-binding pocket of recombinant JAK2 JH2 V617F protein at a low hit rate of 0.05%, which indicates unique structural characteristics of the JAK2 JH2 ATP-binding pocket. Selected hits and structural analogs were further assessed for binding to JH2 and JH1 (kinase) domains of JAK family members (JAK1-3, TYK2) and for effects on MPN model cell viability. Crystal structures were determined with JAK2 JH2 wild-type and V617F. The JH2-selective binders were identified in diaminotriazole, diaminotriazine, and phenylpyrazolo-pyrimidone chemical entities, but they showed low-affinity, and no inhibition of MPN cells was detected, while compounds binding to both JAK2 JH1 and JH2 domains inhibited MPN cell viability. X-ray crystal structures of protein-ligand complexes indicated generally similar binding modes between the ligands and V617F or wild-type JAK2. Ligands of JAK2 JH2 V617F are applicable as probes in JAK-STAT research, and SAR optimization combined with structural insights may yield higher-affinity inhibitors with biological activity.

AB - Hyperactive mutation V617F in the JAK2 regulatory pseudokinase domain (JH2) is prevalent in patients with myeloproliferative neoplasms. Here, we identified novel small molecules that target JH2 of JAK2 V617F and characterized binding via biochemical and structural approaches. Screening of 107,600 small molecules resulted in identification of 55 binders to the ATP-binding pocket of recombinant JAK2 JH2 V617F protein at a low hit rate of 0.05%, which indicates unique structural characteristics of the JAK2 JH2 ATP-binding pocket. Selected hits and structural analogs were further assessed for binding to JH2 and JH1 (kinase) domains of JAK family members (JAK1-3, TYK2) and for effects on MPN model cell viability. Crystal structures were determined with JAK2 JH2 wild-type and V617F. The JH2-selective binders were identified in diaminotriazole, diaminotriazine, and phenylpyrazolo-pyrimidone chemical entities, but they showed low-affinity, and no inhibition of MPN cells was detected, while compounds binding to both JAK2 JH1 and JH2 domains inhibited MPN cell viability. X-ray crystal structures of protein-ligand complexes indicated generally similar binding modes between the ligands and V617F or wild-type JAK2. Ligands of JAK2 JH2 V617F are applicable as probes in JAK-STAT research, and SAR optimization combined with structural insights may yield higher-affinity inhibitors with biological activity.

KW - cytokine signaling

KW - JAK inhibitor

KW - JAK2 V617F

KW - myeloproliferative neoplasm

KW - pseudokinase

U2 - 10.3390/ph16010075

DO - 10.3390/ph16010075

M3 - Article

AN - SCOPUS:85146766468

SN - 1424-8247

VL - 16

JO - Pharmaceuticals

JF - Pharmaceuticals

IS - 1

M1 - 75

ER -

Identification of Novel Small Molecule Ligands for JAK2 Pseudokinase Domain

Abstrakti

Rahoitus

Julkaisufoorumi-taso

!!ASJC Scopus subject areas

Pääsy asiakirjaan

Sormenjälki

Tietoaineistot

Crystal structure of JAK2 JH2 (pseudokinase domain) in complex with Reversine

Crystal structure of JAK2 JH2 (pseudokinase domain) in complex with CDK2-IV

Crystal structure of JAK2 JH2-V617F in complex with JNJ-7706621

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