5′-triphosphate-siRNA: Turning gene silencing and Rig-I activation against melanoma

Hendrik Poeck; Robert Besch; Cornelius Maihoefer; Marcel Renn; Damia Tormo; Svetlana Shulga Morskaya; Susanne Kirschnek; Evelyn Gaffal; Jennifer Landsberg; Johannes Hellmuth; Andreas Schmidt; David Anz; Michael Bscheider; Tobias Schwerd; Carola Berking; Carole Bourquin; Ulrich Kalinke; Elisabeth Kremmer; Hiroki Kato; Shizuo Akira; Rachel Meyers; Georg Häcker; Michael Neuenhahn; Dirk Busch; Jürgen Ruland; Simon Rothenfusser; Marco Prinz; Veit Hornung; Stefan Endres; Thomas Tüting; Gunther Hartmann

doi:10.1038/nm.1887

5′-triphosphate-siRNA: Turning gene silencing and Rig-I activation against melanoma

Hendrik Poeck, Robert Besch, Cornelius Maihoefer, Marcel Renn, Damia Tormo, Svetlana Shulga Morskaya, Susanne Kirschnek, Evelyn Gaffal, Jennifer Landsberg, Johannes Hellmuth, Andreas Schmidt, David Anz, Michael Bscheider, Tobias Schwerd, Carola Berking, Carole Bourquin, Ulrich Kalinke, Elisabeth Kremmer, Hiroki Kato, Shizuo AkiraRachel Meyers, Georg Häcker, Michael Neuenhahn, Dirk Busch, Jürgen Ruland, Simon Rothenfusser, Marco Prinz, Veit Hornung, Stefan Endres, Thomas Tüting, Gunther Hartmann

Chair of Medical Microbiology, Immunology and Hygiene

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

349 Scopus citations

Abstract

Genetic and epigenetic plasticity allows tumors to evade single-targeted treatments. Here we direct Bcl2-specific short interfering RNA (siRNA) with 5′-triphosphate ends (3p-siRNA) against melanoma. Recognition of 5′-triphosphate by the cytosolic antiviral helicase retinoic acid-induced protein I (Rig-I, encoded by Ddx58) activated innate immune cells such as dendritic cells and directly induced expression of interferons (IFNs) and apoptosis in tumor cells. These Rig-I-mediated activities synergized with siRNA-mediated Bcl2 silencing to provoke massive apoptosis of tumor cells in lung metastases in vivo. The therapeutic activity required natural killer cells and IFN, as well as silencing of Bcl2, as evidenced by rescue with a mutated Bcl2 target, by site-specific cleavage of Bcl2 messenger RNA in lung metastases and downregulation of Bcl-2 protein in tumor cells in vivo. Together, 3p-siRNA represents a single molecule-based approach in which Rig-I activation on both the immune- and tumor cell level corrects immune ignorance and in which gene silencing corrects key molecular events that govern tumor cell survival.

Original language	English
Pages (from-to)	1256-1263
Number of pages	8
Journal	Nature Medicine
Volume	14
Issue number	11
DOIs	https://doi.org/10.1038/nm.1887
State	Published - Nov 2008

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Poeck, H., Besch, R., Maihoefer, C., Renn, M., Tormo, D., Morskaya, S. S., Kirschnek, S., Gaffal, E., Landsberg, J., Hellmuth, J., Schmidt, A., Anz, D., Bscheider, M., Schwerd, T., Berking, C., Bourquin, C., Kalinke, U., Kremmer, E., Kato, H., ... Hartmann, G. (2008). 5′-triphosphate-siRNA: Turning gene silencing and Rig-I activation against melanoma. Nature Medicine, 14(11), 1256-1263. https://doi.org/10.1038/nm.1887

@article{d99a421bd44d4e7aaf1305eb3a42109c,

title = "5′-triphosphate-siRNA: Turning gene silencing and Rig-I activation against melanoma",

abstract = "Genetic and epigenetic plasticity allows tumors to evade single-targeted treatments. Here we direct Bcl2-specific short interfering RNA (siRNA) with 5′-triphosphate ends (3p-siRNA) against melanoma. Recognition of 5′-triphosphate by the cytosolic antiviral helicase retinoic acid-induced protein I (Rig-I, encoded by Ddx58) activated innate immune cells such as dendritic cells and directly induced expression of interferons (IFNs) and apoptosis in tumor cells. These Rig-I-mediated activities synergized with siRNA-mediated Bcl2 silencing to provoke massive apoptosis of tumor cells in lung metastases in vivo. The therapeutic activity required natural killer cells and IFN, as well as silencing of Bcl2, as evidenced by rescue with a mutated Bcl2 target, by site-specific cleavage of Bcl2 messenger RNA in lung metastases and downregulation of Bcl-2 protein in tumor cells in vivo. Together, 3p-siRNA represents a single molecule-based approach in which Rig-I activation on both the immune- and tumor cell level corrects immune ignorance and in which gene silencing corrects key molecular events that govern tumor cell survival.",

author = "Hendrik Poeck and Robert Besch and Cornelius Maihoefer and Marcel Renn and Damia Tormo and Morskaya, {Svetlana Shulga} and Susanne Kirschnek and Evelyn Gaffal and Jennifer Landsberg and Johannes Hellmuth and Andreas Schmidt and David Anz and Michael Bscheider and Tobias Schwerd and Carola Berking and Carole Bourquin and Ulrich Kalinke and Elisabeth Kremmer and Hiroki Kato and Shizuo Akira and Rachel Meyers and Georg H{\"a}cker and Michael Neuenhahn and Dirk Busch and J{\"u}rgen Ruland and Simon Rothenfusser and Marco Prinz and Veit Hornung and Stefan Endres and Thomas T{\"u}ting and Gunther Hartmann",

year = "2008",

month = nov,

doi = "10.1038/nm.1887",

language = "English",

volume = "14",

pages = "1256--1263",

journal = "Nature Medicine",

issn = "1078-8956",

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Poeck, H, Besch, R, Maihoefer, C, Renn, M, Tormo, D, Morskaya, SS, Kirschnek, S, Gaffal, E, Landsberg, J, Hellmuth, J, Schmidt, A, Anz, D, Bscheider, M, Schwerd, T, Berking, C, Bourquin, C, Kalinke, U, Kremmer, E, Kato, H, Akira, S, Meyers, R, Häcker, G, Neuenhahn, M, Busch, D, Ruland, J, Rothenfusser, S, Prinz, M, Hornung, V, Endres, S, Tüting, T & Hartmann, G 2008, '5′-triphosphate-siRNA: Turning gene silencing and Rig-I activation against melanoma', Nature Medicine, vol. 14, no. 11, pp. 1256-1263. https://doi.org/10.1038/nm.1887

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T2 - Turning gene silencing and Rig-I activation against melanoma

AU - Poeck, Hendrik

AU - Besch, Robert

AU - Maihoefer, Cornelius

AU - Renn, Marcel

AU - Tormo, Damia

AU - Morskaya, Svetlana Shulga

AU - Kirschnek, Susanne

AU - Gaffal, Evelyn

AU - Landsberg, Jennifer

AU - Hellmuth, Johannes

AU - Schmidt, Andreas

AU - Anz, David

AU - Bscheider, Michael

AU - Schwerd, Tobias

AU - Berking, Carola

AU - Bourquin, Carole

AU - Kalinke, Ulrich

AU - Kremmer, Elisabeth

AU - Kato, Hiroki

AU - Akira, Shizuo

AU - Meyers, Rachel

AU - Häcker, Georg

AU - Neuenhahn, Michael

AU - Busch, Dirk

AU - Ruland, Jürgen

AU - Rothenfusser, Simon

AU - Prinz, Marco

AU - Hornung, Veit

AU - Endres, Stefan

AU - Tüting, Thomas

AU - Hartmann, Gunther

PY - 2008/11

Y1 - 2008/11

N2 - Genetic and epigenetic plasticity allows tumors to evade single-targeted treatments. Here we direct Bcl2-specific short interfering RNA (siRNA) with 5′-triphosphate ends (3p-siRNA) against melanoma. Recognition of 5′-triphosphate by the cytosolic antiviral helicase retinoic acid-induced protein I (Rig-I, encoded by Ddx58) activated innate immune cells such as dendritic cells and directly induced expression of interferons (IFNs) and apoptosis in tumor cells. These Rig-I-mediated activities synergized with siRNA-mediated Bcl2 silencing to provoke massive apoptosis of tumor cells in lung metastases in vivo. The therapeutic activity required natural killer cells and IFN, as well as silencing of Bcl2, as evidenced by rescue with a mutated Bcl2 target, by site-specific cleavage of Bcl2 messenger RNA in lung metastases and downregulation of Bcl-2 protein in tumor cells in vivo. Together, 3p-siRNA represents a single molecule-based approach in which Rig-I activation on both the immune- and tumor cell level corrects immune ignorance and in which gene silencing corrects key molecular events that govern tumor cell survival.

AB - Genetic and epigenetic plasticity allows tumors to evade single-targeted treatments. Here we direct Bcl2-specific short interfering RNA (siRNA) with 5′-triphosphate ends (3p-siRNA) against melanoma. Recognition of 5′-triphosphate by the cytosolic antiviral helicase retinoic acid-induced protein I (Rig-I, encoded by Ddx58) activated innate immune cells such as dendritic cells and directly induced expression of interferons (IFNs) and apoptosis in tumor cells. These Rig-I-mediated activities synergized with siRNA-mediated Bcl2 silencing to provoke massive apoptosis of tumor cells in lung metastases in vivo. The therapeutic activity required natural killer cells and IFN, as well as silencing of Bcl2, as evidenced by rescue with a mutated Bcl2 target, by site-specific cleavage of Bcl2 messenger RNA in lung metastases and downregulation of Bcl-2 protein in tumor cells in vivo. Together, 3p-siRNA represents a single molecule-based approach in which Rig-I activation on both the immune- and tumor cell level corrects immune ignorance and in which gene silencing corrects key molecular events that govern tumor cell survival.

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DO - 10.1038/nm.1887

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VL - 14

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JO - Nature Medicine

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ER -

5′-triphosphate-siRNA: Turning gene silencing and Rig-I activation against melanoma

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