Discovery of a Potent, Selective, and In Vivo Efficacious Covalent Inhibitor for Lysine Methyltransferase SETD8

He Chen; Rudra Prasad Dutta; Zhizhong Li; Yue Zhong; Anqi Ma; Kwang Su Park; Jithesh Kottur; Alison Park; Nicolas Babault; Ke Wang; Dandan Wang; Yan Xiong; H. Ümit Kaniskan; Minkui Luo; Samir Parekh; Jian Jin

doi:10.1021/acs.jmedchem.5c02958

Discovery of a Potent, Selective, and In Vivo Efficacious Covalent Inhibitor for Lysine Methyltransferase SETD8

He Chen
, Rudra Prasad Dutta
, Zhizhong Li
, Yue Zhong
, Anqi Ma
, Kwang Su Park
, Jithesh Kottur
, Alison Park
, Nicolas Babault
, Ke Wang
, Dandan Wang
, Yan Xiong
, H. Ümit Kaniskan
, Minkui Luo
, Samir Parekh
, Jian Jin

Research output: Contribution to journal › Article › peer-review

Abstract

Dysregulated signaling of SET domain-containing protein 8 (SETD8) has been implicated in tumorigenesis, yet most SETD8 inhibitors exhibited limited cellular efficacy. Herein, we developed a potent and selective SETD8 covalent inhibitor, MS2928 (3), featuring a propiolamide covalent warhead. Compound 3 potently and selectively inhibited SETD8 methyltransferase activity. The covalent inhibition mechanism of 3 was confirmed by mass spectrometry and X-ray crystallography. Moreover, 3 significantly reduced the histone H4 lysine 20 monomethylation (H4K20me1) levels in cells and robustly inhibited the proliferation of SETD8-overexpressing multiple myeloma (MM) cell lines with no significant antiproliferative effect on SETD8-low expressing MM cells and normal cells. Importantly, 3 effectively inhibited tumor growth in vivo in two xenograft mouse models of SETD8-overexpressing MM cell lines. Collectively, our results establish 3 as a valuable chemical tool for exploring the biological functions of SETD8 and pave the way for further development of novel epigenetic therapies for MM.

Original language	English
Pages (from-to)	4255-4269
Number of pages	15
Journal	Journal of Medicinal Chemistry
Volume	69
Issue number	4
DOIs	https://doi.org/10.1021/acs.jmedchem.5c02958
State	Published - 26 Feb 2026

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Chen, H., Dutta, R. P., Li, Z., Zhong, Y., Ma, A., Park, K. S., Kottur, J., Park, A., Babault, N., Wang, K., Wang, D., Xiong, Y., Kaniskan, H. Ü., Luo, M., Parekh, S., & Jin, J. (2026). Discovery of a Potent, Selective, and In Vivo Efficacious Covalent Inhibitor for Lysine Methyltransferase SETD8. Journal of Medicinal Chemistry, 69(4), 4255-4269. https://doi.org/10.1021/acs.jmedchem.5c02958

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title = "Discovery of a Potent, Selective, and In Vivo Efficacious Covalent Inhibitor for Lysine Methyltransferase SETD8",

abstract = "Dysregulated signaling of SET domain-containing protein 8 (SETD8) has been implicated in tumorigenesis, yet most SETD8 inhibitors exhibited limited cellular efficacy. Herein, we developed a potent and selective SETD8 covalent inhibitor, MS2928 (3), featuring a propiolamide covalent warhead. Compound 3 potently and selectively inhibited SETD8 methyltransferase activity. The covalent inhibition mechanism of 3 was confirmed by mass spectrometry and X-ray crystallography. Moreover, 3 significantly reduced the histone H4 lysine 20 monomethylation (H4K20me1) levels in cells and robustly inhibited the proliferation of SETD8-overexpressing multiple myeloma (MM) cell lines with no significant antiproliferative effect on SETD8-low expressing MM cells and normal cells. Importantly, 3 effectively inhibited tumor growth in vivo in two xenograft mouse models of SETD8-overexpressing MM cell lines. Collectively, our results establish 3 as a valuable chemical tool for exploring the biological functions of SETD8 and pave the way for further development of novel epigenetic therapies for MM.",

author = "He Chen and Dutta, \{Rudra Prasad\} and Zhizhong Li and Yue Zhong and Anqi Ma and Park, \{Kwang Su\} and Jithesh Kottur and Alison Park and Nicolas Babault and Ke Wang and Dandan Wang and Yan Xiong and Kaniskan, \{H. {\"U}mit\} and Minkui Luo and Samir Parekh and Jian Jin",

note = "Publisher Copyright: {\textcopyright} 2026 The Authors. Published by American Chemical Society",

year = "2026",

month = feb,

day = "26",

doi = "10.1021/acs.jmedchem.5c02958",

language = "English",

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Chen, H, Dutta, RP, Li, Z, Zhong, Y, Ma, A, Park, KS, Kottur, J, Park, A, Babault, N, Wang, K, Wang, D, Xiong, Y, Kaniskan, HÜ, Luo, M, Parekh, S & Jin, J 2026, 'Discovery of a Potent, Selective, and In Vivo Efficacious Covalent Inhibitor for Lysine Methyltransferase SETD8', Journal of Medicinal Chemistry, vol. 69, no. 4, pp. 4255-4269. https://doi.org/10.1021/acs.jmedchem.5c02958

TY - JOUR

T1 - Discovery of a Potent, Selective, and In Vivo Efficacious Covalent Inhibitor for Lysine Methyltransferase SETD8

AU - Chen, He

AU - Dutta, Rudra Prasad

AU - Li, Zhizhong

AU - Zhong, Yue

AU - Ma, Anqi

AU - Park, Kwang Su

AU - Kottur, Jithesh

AU - Park, Alison

AU - Babault, Nicolas

AU - Wang, Ke

AU - Wang, Dandan

AU - Xiong, Yan

AU - Kaniskan, H. Ümit

AU - Luo, Minkui

AU - Parekh, Samir

AU - Jin, Jian

PY - 2026/2/26

Y1 - 2026/2/26

N2 - Dysregulated signaling of SET domain-containing protein 8 (SETD8) has been implicated in tumorigenesis, yet most SETD8 inhibitors exhibited limited cellular efficacy. Herein, we developed a potent and selective SETD8 covalent inhibitor, MS2928 (3), featuring a propiolamide covalent warhead. Compound 3 potently and selectively inhibited SETD8 methyltransferase activity. The covalent inhibition mechanism of 3 was confirmed by mass spectrometry and X-ray crystallography. Moreover, 3 significantly reduced the histone H4 lysine 20 monomethylation (H4K20me1) levels in cells and robustly inhibited the proliferation of SETD8-overexpressing multiple myeloma (MM) cell lines with no significant antiproliferative effect on SETD8-low expressing MM cells and normal cells. Importantly, 3 effectively inhibited tumor growth in vivo in two xenograft mouse models of SETD8-overexpressing MM cell lines. Collectively, our results establish 3 as a valuable chemical tool for exploring the biological functions of SETD8 and pave the way for further development of novel epigenetic therapies for MM.

AB - Dysregulated signaling of SET domain-containing protein 8 (SETD8) has been implicated in tumorigenesis, yet most SETD8 inhibitors exhibited limited cellular efficacy. Herein, we developed a potent and selective SETD8 covalent inhibitor, MS2928 (3), featuring a propiolamide covalent warhead. Compound 3 potently and selectively inhibited SETD8 methyltransferase activity. The covalent inhibition mechanism of 3 was confirmed by mass spectrometry and X-ray crystallography. Moreover, 3 significantly reduced the histone H4 lysine 20 monomethylation (H4K20me1) levels in cells and robustly inhibited the proliferation of SETD8-overexpressing multiple myeloma (MM) cell lines with no significant antiproliferative effect on SETD8-low expressing MM cells and normal cells. Importantly, 3 effectively inhibited tumor growth in vivo in two xenograft mouse models of SETD8-overexpressing MM cell lines. Collectively, our results establish 3 as a valuable chemical tool for exploring the biological functions of SETD8 and pave the way for further development of novel epigenetic therapies for MM.

UR - https://www.scopus.com/pages/publications/105031246754

U2 - 10.1021/acs.jmedchem.5c02958

DO - 10.1021/acs.jmedchem.5c02958

M3 - Article

C2 - 41693203

AN - SCOPUS:105031246754

SN - 0022-2623

VL - 69

SP - 4255

EP - 4269

JO - Journal of Medicinal Chemistry

JF - Journal of Medicinal Chemistry

IS - 4

ER -

Discovery of a Potent, Selective, and In Vivo Efficacious Covalent Inhibitor for Lysine Methyltransferase SETD8

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