AGR2-Dependent Nuclear Import of RNA Polymerase II Constitutes a Specific Target of Pancreatic Ductal Adenocarcinoma in the Context of Wild-Type p53

Zhiheng Zhang; Hongzhen Li; Yibin Deng; Kathleen Schuck; Susanne Raulefs; Nadja Maeritz; Yuanyuan Yu; Torsten Hechler; Andreas Pahl; Vanesa Fernández-Sáiz; Yuan Wan; Guosheng Wang; Thomas Engleitner; Rupert Öllinger; Roland Rad; Maximilian Reichert; Kalliope N. Diakopoulos; Verena Weber; Jingjing Li; Shanshan Shen; Xiaoping Zou; Jörg Kleeff; Andre Mihaljevic; Christoph W. Michalski; Hana Algül; Helmut Friess; Bo Kong

doi:10.1053/j.gastro.2021.07.030

AGR2-Dependent Nuclear Import of RNA Polymerase II Constitutes a Specific Target of Pancreatic Ductal Adenocarcinoma in the Context of Wild-Type p53

Zhiheng Zhang, Hongzhen Li, Yibin Deng, Kathleen Schuck, Susanne Raulefs, Nadja Maeritz, Yuanyuan Yu, Torsten Hechler, Andreas Pahl, Vanesa Fernández-Sáiz, Yuan Wan, Guosheng Wang, Thomas Engleitner, Rupert Öllinger, Roland Rad, Maximilian Reichert, Kalliope N. Diakopoulos, Verena Weber, Jingjing Li, Shanshan ShenXiaoping Zou, Jörg Kleeff, Andre Mihaljevic, Christoph W. Michalski, Hana Algül, Helmut Friess, Bo Kong

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

17 Scopus citations

Abstract

Background & Aims: Promoted by pancreatitis, oncogenic Kras^G12D triggers acinar cells’ neoplastic transformation through acinar-to-ductal metaplasia (ADM) and pancreatic intraepithelial neoplasia. Anterior gradient 2 (Agr2), a known inhibitor of p53, is detected at early stage of pancreatic ductal adenocarcinoma (PDAC) development. RNA polymerase II (RNAPII) is a key nuclear enzyme; regulation of its nuclear localization in mammalian cells represents a potential therapeutic target. Methods: A mouse model of inflammation-accelerated Kras^G12D-driven ADM and pancreatic intraepithelial neoplasia development was used. Pancreas-specific Agr2 ablation was performed to access its role in pancreatic carcinogenesis. Hydrophobic hexapeptides loaded in liposomes were developed to disrupt Agr2–RNAPII complex. Results: We found that Agr2 is up-regulated in ADM-to-pancreatic intraepithelial neoplasia transition in inflammation and Kras^G12D-driven early pancreatic carcinogenesis. Genetic ablation of Agr2 specifically blocks this metaplastic-to-neoplastic process. Mechanistically, Agr2 directs the nuclear import of RNAPII via its C-terminal nuclear localization signal, undermining the ATR-dependent p53 activation in ADM lesions. Because Agr2 binds to the largest subunit of RNAPII in a peptide motif-dependent manner, we developed a hexapeptide to interfere with the nuclear import of RNAPII by competitively disrupting the Agr2-RNAPII complex. This novel hexapeptide leads to dysfunction of RNAPII with concomitant activation of DNA damage response in early neoplastic lesions; hence, it dramatically compromises PDAC initiation in vivo. Moreover, the hexapeptide sensitizes PDAC cells and patient-derived organoids harboring wild-type p53 to RNAPII inhibitors and first-line chemotherapeutic agents in vivo. Of note, this therapeutic effect is efficient across various cancer types. Conclusions: Agr2 is identified as a novel adaptor protein for nuclear import of RNAPII in mammalian cells. Also, we provide genetic evidence defining Agr2-dependent nuclear import of RNAPII as a pharmaceutically accessible target for prevention and treatment in PDAC in the context of wild-type p53.

Original language	English
Pages (from-to)	1601-1614.e23
Journal	Gastroenterology
Volume	161
Issue number	5
DOIs	https://doi.org/10.1053/j.gastro.2021.07.030
State	Published - Nov 2021

Keywords

Agr2
Hexapeptide
Metaplastic
Neoplastic
Pancreatic Cancer

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10.1053/j.gastro.2021.07.030

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Zhang, Z., Li, H., Deng, Y., Schuck, K., Raulefs, S., Maeritz, N., Yu, Y., Hechler, T., Pahl, A., Fernández-Sáiz, V., Wan, Y., Wang, G., Engleitner, T., Öllinger, R., Rad, R., Reichert, M., Diakopoulos, K. N., Weber, V., Li, J., ... Kong, B. (2021). AGR2-Dependent Nuclear Import of RNA Polymerase II Constitutes a Specific Target of Pancreatic Ductal Adenocarcinoma in the Context of Wild-Type p53. Gastroenterology, 161(5), 1601-1614.e23. https://doi.org/10.1053/j.gastro.2021.07.030

@article{b97370f84d674a55a88559e1ef0e3a57,

title = "AGR2-Dependent Nuclear Import of RNA Polymerase II Constitutes a Specific Target of Pancreatic Ductal Adenocarcinoma in the Context of Wild-Type p53",

abstract = "Background & Aims: Promoted by pancreatitis, oncogenic KrasG12D triggers acinar cells{\textquoteright} neoplastic transformation through acinar-to-ductal metaplasia (ADM) and pancreatic intraepithelial neoplasia. Anterior gradient 2 (Agr2), a known inhibitor of p53, is detected at early stage of pancreatic ductal adenocarcinoma (PDAC) development. RNA polymerase II (RNAPII) is a key nuclear enzyme; regulation of its nuclear localization in mammalian cells represents a potential therapeutic target. Methods: A mouse model of inflammation-accelerated KrasG12D-driven ADM and pancreatic intraepithelial neoplasia development was used. Pancreas-specific Agr2 ablation was performed to access its role in pancreatic carcinogenesis. Hydrophobic hexapeptides loaded in liposomes were developed to disrupt Agr2–RNAPII complex. Results: We found that Agr2 is up-regulated in ADM-to-pancreatic intraepithelial neoplasia transition in inflammation and KrasG12D-driven early pancreatic carcinogenesis. Genetic ablation of Agr2 specifically blocks this metaplastic-to-neoplastic process. Mechanistically, Agr2 directs the nuclear import of RNAPII via its C-terminal nuclear localization signal, undermining the ATR-dependent p53 activation in ADM lesions. Because Agr2 binds to the largest subunit of RNAPII in a peptide motif-dependent manner, we developed a hexapeptide to interfere with the nuclear import of RNAPII by competitively disrupting the Agr2-RNAPII complex. This novel hexapeptide leads to dysfunction of RNAPII with concomitant activation of DNA damage response in early neoplastic lesions; hence, it dramatically compromises PDAC initiation in vivo. Moreover, the hexapeptide sensitizes PDAC cells and patient-derived organoids harboring wild-type p53 to RNAPII inhibitors and first-line chemotherapeutic agents in vivo. Of note, this therapeutic effect is efficient across various cancer types. Conclusions: Agr2 is identified as a novel adaptor protein for nuclear import of RNAPII in mammalian cells. Also, we provide genetic evidence defining Agr2-dependent nuclear import of RNAPII as a pharmaceutically accessible target for prevention and treatment in PDAC in the context of wild-type p53.",

keywords = "Agr2, Hexapeptide, Metaplastic, Neoplastic, Pancreatic Cancer",

author = "Zhiheng Zhang and Hongzhen Li and Yibin Deng and Kathleen Schuck and Susanne Raulefs and Nadja Maeritz and Yuanyuan Yu and Torsten Hechler and Andreas Pahl and Vanesa Fern{\'a}ndez-S{\'a}iz and Yuan Wan and Guosheng Wang and Thomas Engleitner and Rupert {\"O}llinger and Roland Rad and Maximilian Reichert and Diakopoulos, {Kalliope N.} and Verena Weber and Jingjing Li and Shanshan Shen and Xiaoping Zou and J{\"o}rg Kleeff and Andre Mihaljevic and Michalski, {Christoph W.} and Hana Alg{\"u}l and Helmut Friess and Bo Kong",

note = "Publisher Copyright: {\textcopyright} 2021 AGA Institute",

year = "2021",

month = nov,

doi = "10.1053/j.gastro.2021.07.030",

language = "English",

volume = "161",

pages = "1601--1614.e23",

journal = "Gastroenterology",

issn = "0016-5085",

publisher = "W.B. Saunders",

number = "5",

}

Zhang, Z, Li, H, Deng, Y, Schuck, K, Raulefs, S, Maeritz, N, Yu, Y, Hechler, T, Pahl, A, Fernández-Sáiz, V, Wan, Y, Wang, G, Engleitner, T, Öllinger, R, Rad, R , Reichert, M, Diakopoulos, KN, Weber, V, Li, J, Shen, S, Zou, X, Kleeff, J, Mihaljevic, A, Michalski, CW, Algül, H , Friess, H & Kong, B 2021, 'AGR2-Dependent Nuclear Import of RNA Polymerase II Constitutes a Specific Target of Pancreatic Ductal Adenocarcinoma in the Context of Wild-Type p53', Gastroenterology, vol. 161, no. 5, pp. 1601-1614.e23. https://doi.org/10.1053/j.gastro.2021.07.030

TY - JOUR

T1 - AGR2-Dependent Nuclear Import of RNA Polymerase II Constitutes a Specific Target of Pancreatic Ductal Adenocarcinoma in the Context of Wild-Type p53

AU - Zhang, Zhiheng

AU - Li, Hongzhen

AU - Deng, Yibin

AU - Schuck, Kathleen

AU - Raulefs, Susanne

AU - Maeritz, Nadja

AU - Yu, Yuanyuan

AU - Hechler, Torsten

AU - Pahl, Andreas

AU - Fernández-Sáiz, Vanesa

AU - Wan, Yuan

AU - Wang, Guosheng

AU - Engleitner, Thomas

AU - Öllinger, Rupert

AU - Rad, Roland

AU - Reichert, Maximilian

AU - Diakopoulos, Kalliope N.

AU - Weber, Verena

AU - Li, Jingjing

AU - Shen, Shanshan

AU - Zou, Xiaoping

AU - Kleeff, Jörg

AU - Mihaljevic, Andre

AU - Michalski, Christoph W.

AU - Algül, Hana

AU - Friess, Helmut

AU - Kong, Bo

PY - 2021/11

Y1 - 2021/11

N2 - Background & Aims: Promoted by pancreatitis, oncogenic KrasG12D triggers acinar cells’ neoplastic transformation through acinar-to-ductal metaplasia (ADM) and pancreatic intraepithelial neoplasia. Anterior gradient 2 (Agr2), a known inhibitor of p53, is detected at early stage of pancreatic ductal adenocarcinoma (PDAC) development. RNA polymerase II (RNAPII) is a key nuclear enzyme; regulation of its nuclear localization in mammalian cells represents a potential therapeutic target. Methods: A mouse model of inflammation-accelerated KrasG12D-driven ADM and pancreatic intraepithelial neoplasia development was used. Pancreas-specific Agr2 ablation was performed to access its role in pancreatic carcinogenesis. Hydrophobic hexapeptides loaded in liposomes were developed to disrupt Agr2–RNAPII complex. Results: We found that Agr2 is up-regulated in ADM-to-pancreatic intraepithelial neoplasia transition in inflammation and KrasG12D-driven early pancreatic carcinogenesis. Genetic ablation of Agr2 specifically blocks this metaplastic-to-neoplastic process. Mechanistically, Agr2 directs the nuclear import of RNAPII via its C-terminal nuclear localization signal, undermining the ATR-dependent p53 activation in ADM lesions. Because Agr2 binds to the largest subunit of RNAPII in a peptide motif-dependent manner, we developed a hexapeptide to interfere with the nuclear import of RNAPII by competitively disrupting the Agr2-RNAPII complex. This novel hexapeptide leads to dysfunction of RNAPII with concomitant activation of DNA damage response in early neoplastic lesions; hence, it dramatically compromises PDAC initiation in vivo. Moreover, the hexapeptide sensitizes PDAC cells and patient-derived organoids harboring wild-type p53 to RNAPII inhibitors and first-line chemotherapeutic agents in vivo. Of note, this therapeutic effect is efficient across various cancer types. Conclusions: Agr2 is identified as a novel adaptor protein for nuclear import of RNAPII in mammalian cells. Also, we provide genetic evidence defining Agr2-dependent nuclear import of RNAPII as a pharmaceutically accessible target for prevention and treatment in PDAC in the context of wild-type p53.

AB - Background & Aims: Promoted by pancreatitis, oncogenic KrasG12D triggers acinar cells’ neoplastic transformation through acinar-to-ductal metaplasia (ADM) and pancreatic intraepithelial neoplasia. Anterior gradient 2 (Agr2), a known inhibitor of p53, is detected at early stage of pancreatic ductal adenocarcinoma (PDAC) development. RNA polymerase II (RNAPII) is a key nuclear enzyme; regulation of its nuclear localization in mammalian cells represents a potential therapeutic target. Methods: A mouse model of inflammation-accelerated KrasG12D-driven ADM and pancreatic intraepithelial neoplasia development was used. Pancreas-specific Agr2 ablation was performed to access its role in pancreatic carcinogenesis. Hydrophobic hexapeptides loaded in liposomes were developed to disrupt Agr2–RNAPII complex. Results: We found that Agr2 is up-regulated in ADM-to-pancreatic intraepithelial neoplasia transition in inflammation and KrasG12D-driven early pancreatic carcinogenesis. Genetic ablation of Agr2 specifically blocks this metaplastic-to-neoplastic process. Mechanistically, Agr2 directs the nuclear import of RNAPII via its C-terminal nuclear localization signal, undermining the ATR-dependent p53 activation in ADM lesions. Because Agr2 binds to the largest subunit of RNAPII in a peptide motif-dependent manner, we developed a hexapeptide to interfere with the nuclear import of RNAPII by competitively disrupting the Agr2-RNAPII complex. This novel hexapeptide leads to dysfunction of RNAPII with concomitant activation of DNA damage response in early neoplastic lesions; hence, it dramatically compromises PDAC initiation in vivo. Moreover, the hexapeptide sensitizes PDAC cells and patient-derived organoids harboring wild-type p53 to RNAPII inhibitors and first-line chemotherapeutic agents in vivo. Of note, this therapeutic effect is efficient across various cancer types. Conclusions: Agr2 is identified as a novel adaptor protein for nuclear import of RNAPII in mammalian cells. Also, we provide genetic evidence defining Agr2-dependent nuclear import of RNAPII as a pharmaceutically accessible target for prevention and treatment in PDAC in the context of wild-type p53.

KW - Agr2

KW - Hexapeptide

KW - Metaplastic

KW - Neoplastic

KW - Pancreatic Cancer

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U2 - 10.1053/j.gastro.2021.07.030

DO - 10.1053/j.gastro.2021.07.030

M3 - Article

C2 - 34303658

AN - SCOPUS:85115791011

SN - 0016-5085

VL - 161

SP - 1601-1614.e23

JO - Gastroenterology

JF - Gastroenterology

IS - 5

ER -

AGR2-Dependent Nuclear Import of RNA Polymerase II Constitutes a Specific Target of Pancreatic Ductal Adenocarcinoma in the Context of Wild-Type p53

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