Iron Chelation Therapy Elicits Innate Immune Control of Metastatic Ovarian Cancer

Tito A. Sandoval; Camilla Salvagno; Chang Suk Chae; Deepika Awasthi; Paolo Giovanelli; Matias Marin Falco; Sung Min Hwang; Eli Teran-Cabanillas; Lasse Suominen; Takahiro Yamazaki; Hui Hsuan Kuo; Jenna E. Moyer; M. Laura Martin; Jyothi Manohar; Kihwan Kim; Maria A. Sierra; Yusibeska Ramos; Chen Tan; Alexander Emmanuelli; Minkyung Song; Diana K. Morales; Dmitriy Zamarin; Melissa K. Frey; Evelyn Cantillo; Eloise Chapman-Davis; Kevin Holcomb; Christopher E. Mason; Lorenzo Galluzzi; Zhen Ni Zhou; Anna Vähärautio; Suzanne M. Cloonan; Juan R. Cubillos-Ruiz

doi:10.1158/2159-8290.CD-23-1451

Iron Chelation Therapy Elicits Innate Immune Control of Metastatic Ovarian Cancer

Tito A. Sandoval, Camilla Salvagno, Chang Suk Chae, Deepika Awasthi, Paolo Giovanelli, Matias Marin Falco, Sung Min Hwang, Eli Teran-Cabanillas, Lasse Suominen, Takahiro Yamazaki, Hui Hsuan Kuo, Jenna E. Moyer, M. Laura Martin, Jyothi Manohar, Kihwan Kim, Maria A. Sierra, Yusibeska Ramos, Chen Tan, Alexander Emmanuelli, Minkyung SongDiana K. Morales, Dmitriy Zamarin, Melissa K. Frey, Evelyn Cantillo, Eloise Chapman-Davis, Kevin Holcomb, Christopher E. Mason, Lorenzo Galluzzi, Zhen Ni Zhou, Anna Vähärautio, Suzanne M. Cloonan, Juan R. Cubillos-Ruiz

Tutkimustuotos: Artikkelijulkaisu › Artikkeli › Tieteellinen › vertaisarvioitu

Abstrakti

Iron accumulation in tumors contributes to disease progression and chemoresistance. Although targeting this process can influence various hallmarks of cancer, the immunomodulatory effects of iron chelation in the tumor microenvironment are unknown. Here, we report that treatment with deferiprone, an FDA-approved iron chelator, unleashes innate immune responses that restrain ovarian cancer. Deferiprone reprogrammed ovarian cancer cells toward an immunostimulatory state characterized by the production of type-I IFN and overexpression of molecules that activate NK cells. Mechanistically, these effects were driven by innate sensing of mitochondrial DNA in the cytosol and concomitant activation of nuclear DNA damage responses triggered upon iron chelation. Deferiprone synergized with chemotherapy and prolonged the survival of mice with ovarian cancer by bolstering type-I IFN responses that drove NK cell-dependent control of metastatic disease. Hence, iron chelation may represent an alternative immunotherapeutic strategy for malignancies that are refractory to current T-cell-centric modalities. Significance: This study uncovers that targeting dysregulated iron accumulation in ovarian tumors represents a major therapeutic opportunity. Iron chelation therapy using an FDA-approved agent causes immunogenic stress responses in ovarian cancer cells that delay metastatic disease progression and enhance the effects of first-line chemotherapy. See related commentary by Bell and Zou, p. 1771.

Alkuperäiskieli	englanti
Lehti	Cancer Discovery
Vuosikerta	14
Numero	10
Sivut	1901-1921
Sivumäärä	21
ISSN	2159-8290
DOI - pysyväislinkit	https://doi.org/10.1158/2159-8290.CD-23-1451
Tila	Julkaistu - 4 lokak. 2024
OKM-julkaisutyyppi	A1 Alkuperäisartikkeli tieteellisessä aikakauslehdessä, vertaisarvioitu

Lisätietoja

Publisher Copyright:
©2024 American Association for Cancer Research.

Tieteenalat

3122 Syöpätaudit

Pääsy asiakirjaan

10.1158/2159-8290.CD-23-1451Lisenssi: CC BY

https://www.researchsquare.com/article/rs-3399219/v1Lisenssi: CC BY

Siteeraa tätä

Sandoval, T. A., Salvagno, C., Chae, C. S., Awasthi, D., Giovanelli, P., Marin Falco, M., Hwang, S. M., Teran-Cabanillas, E., Suominen, L., Yamazaki, T., Kuo, H. H., Moyer, J. E., Martin, M. L., Manohar, J., Kim, K., Sierra, M. A., Ramos, Y., Tan, C., Emmanuelli, A., ... Cubillos-Ruiz, J. R. (2024). Iron Chelation Therapy Elicits Innate Immune Control of Metastatic Ovarian Cancer. Cancer Discovery, 14(10), 1901-1921. https://doi.org/10.1158/2159-8290.CD-23-1451

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title = "Iron Chelation Therapy Elicits Innate Immune Control of Metastatic Ovarian Cancer",

abstract = "Iron accumulation in tumors contributes to disease progression and chemoresistance. Although targeting this process can influence various hallmarks of cancer, the immunomodulatory effects of iron chelation in the tumor microenvironment are unknown. Here, we report that treatment with deferiprone, an FDA-approved iron chelator, unleashes innate immune responses that restrain ovarian cancer. Deferiprone reprogrammed ovarian cancer cells toward an immunostimulatory state characterized by the production of type-I IFN and overexpression of molecules that activate NK cells. Mechanistically, these effects were driven by innate sensing of mitochondrial DNA in the cytosol and concomitant activation of nuclear DNA damage responses triggered upon iron chelation. Deferiprone synergized with chemotherapy and prolonged the survival of mice with ovarian cancer by bolstering type-I IFN responses that drove NK cell-dependent control of metastatic disease. Hence, iron chelation may represent an alternative immunotherapeutic strategy for malignancies that are refractory to current T-cell-centric modalities. Significance: This study uncovers that targeting dysregulated iron accumulation in ovarian tumors represents a major therapeutic opportunity. Iron chelation therapy using an FDA-approved agent causes immunogenic stress responses in ovarian cancer cells that delay metastatic disease progression and enhance the effects of first-line chemotherapy. See related commentary by Bell and Zou, p. 1771.",

keywords = "3122 Cancers",

author = "Sandoval, {Tito A.} and Camilla Salvagno and Chae, {Chang Suk} and Deepika Awasthi and Paolo Giovanelli and {Marin Falco}, Matias and Hwang, {Sung Min} and Eli Teran-Cabanillas and Lasse Suominen and Takahiro Yamazaki and Kuo, {Hui Hsuan} and Moyer, {Jenna E.} and Martin, {M. Laura} and Jyothi Manohar and Kihwan Kim and Sierra, {Maria A.} and Yusibeska Ramos and Chen Tan and Alexander Emmanuelli and Minkyung Song and Morales, {Diana K.} and Dmitriy Zamarin and Frey, {Melissa K.} and Evelyn Cantillo and Eloise Chapman-Davis and Kevin Holcomb and Mason, {Christopher E.} and Lorenzo Galluzzi and {Ni Zhou}, Zhen and Anna V{\"a}h{\"a}rautio and Cloonan, {Suzanne M.} and Cubillos-Ruiz, {Juan R.}",

note = "Publisher Copyright: {\textcopyright}2024 American Association for Cancer Research.",

year = "2024",

month = oct,

day = "4",

doi = "10.1158/2159-8290.CD-23-1451",

language = "English",

volume = "14",

pages = "1901--1921",

journal = "Cancer Discovery",

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Sandoval, TA, Salvagno, C, Chae, CS, Awasthi, D, Giovanelli, P, Marin Falco, M, Hwang, SM, Teran-Cabanillas, E, Suominen, L, Yamazaki, T, Kuo, HH, Moyer, JE, Martin, ML, Manohar, J, Kim, K, Sierra, MA, Ramos, Y, Tan, C, Emmanuelli, A, Song, M, Morales, DK, Zamarin, D, Frey, MK, Cantillo, E, Chapman-Davis, E, Holcomb, K, Mason, CE, Galluzzi, L, Ni Zhou, Z, Vähärautio, A, Cloonan, SM & Cubillos-Ruiz, JR 2024, 'Iron Chelation Therapy Elicits Innate Immune Control of Metastatic Ovarian Cancer', Cancer Discovery, Vuosikerta 14, Nro 10, Sivut 1901-1921. https://doi.org/10.1158/2159-8290.CD-23-1451

TY - JOUR

T1 - Iron Chelation Therapy Elicits Innate Immune Control of Metastatic Ovarian Cancer

AU - Sandoval, Tito A.

AU - Salvagno, Camilla

AU - Chae, Chang Suk

AU - Awasthi, Deepika

AU - Giovanelli, Paolo

AU - Marin Falco, Matias

AU - Hwang, Sung Min

AU - Teran-Cabanillas, Eli

AU - Suominen, Lasse

AU - Yamazaki, Takahiro

AU - Kuo, Hui Hsuan

AU - Moyer, Jenna E.

AU - Martin, M. Laura

AU - Manohar, Jyothi

AU - Kim, Kihwan

AU - Sierra, Maria A.

AU - Ramos, Yusibeska

AU - Tan, Chen

AU - Emmanuelli, Alexander

AU - Song, Minkyung

AU - Morales, Diana K.

AU - Zamarin, Dmitriy

AU - Frey, Melissa K.

AU - Cantillo, Evelyn

AU - Chapman-Davis, Eloise

AU - Holcomb, Kevin

AU - Mason, Christopher E.

AU - Galluzzi, Lorenzo

AU - Ni Zhou, Zhen

AU - Vähärautio, Anna

AU - Cloonan, Suzanne M.

AU - Cubillos-Ruiz, Juan R.

PY - 2024/10/4

Y1 - 2024/10/4

N2 - Iron accumulation in tumors contributes to disease progression and chemoresistance. Although targeting this process can influence various hallmarks of cancer, the immunomodulatory effects of iron chelation in the tumor microenvironment are unknown. Here, we report that treatment with deferiprone, an FDA-approved iron chelator, unleashes innate immune responses that restrain ovarian cancer. Deferiprone reprogrammed ovarian cancer cells toward an immunostimulatory state characterized by the production of type-I IFN and overexpression of molecules that activate NK cells. Mechanistically, these effects were driven by innate sensing of mitochondrial DNA in the cytosol and concomitant activation of nuclear DNA damage responses triggered upon iron chelation. Deferiprone synergized with chemotherapy and prolonged the survival of mice with ovarian cancer by bolstering type-I IFN responses that drove NK cell-dependent control of metastatic disease. Hence, iron chelation may represent an alternative immunotherapeutic strategy for malignancies that are refractory to current T-cell-centric modalities. Significance: This study uncovers that targeting dysregulated iron accumulation in ovarian tumors represents a major therapeutic opportunity. Iron chelation therapy using an FDA-approved agent causes immunogenic stress responses in ovarian cancer cells that delay metastatic disease progression and enhance the effects of first-line chemotherapy. See related commentary by Bell and Zou, p. 1771.

AB - Iron accumulation in tumors contributes to disease progression and chemoresistance. Although targeting this process can influence various hallmarks of cancer, the immunomodulatory effects of iron chelation in the tumor microenvironment are unknown. Here, we report that treatment with deferiprone, an FDA-approved iron chelator, unleashes innate immune responses that restrain ovarian cancer. Deferiprone reprogrammed ovarian cancer cells toward an immunostimulatory state characterized by the production of type-I IFN and overexpression of molecules that activate NK cells. Mechanistically, these effects were driven by innate sensing of mitochondrial DNA in the cytosol and concomitant activation of nuclear DNA damage responses triggered upon iron chelation. Deferiprone synergized with chemotherapy and prolonged the survival of mice with ovarian cancer by bolstering type-I IFN responses that drove NK cell-dependent control of metastatic disease. Hence, iron chelation may represent an alternative immunotherapeutic strategy for malignancies that are refractory to current T-cell-centric modalities. Significance: This study uncovers that targeting dysregulated iron accumulation in ovarian tumors represents a major therapeutic opportunity. Iron chelation therapy using an FDA-approved agent causes immunogenic stress responses in ovarian cancer cells that delay metastatic disease progression and enhance the effects of first-line chemotherapy. See related commentary by Bell and Zou, p. 1771.

KW - 3122 Cancers

U2 - 10.1158/2159-8290.CD-23-1451

DO - 10.1158/2159-8290.CD-23-1451

M3 - Article

C2 - 39073085

AN - SCOPUS:85205741247

SN - 2159-8290

VL - 14

SP - 1901

EP - 1921

JO - Cancer Discovery

JF - Cancer Discovery

IS - 10

ER -