Antigen-Specific antitumor responses induced by OX40 agonist are enhanced by the ido inhibitor indoximod

Zuzana Berrong; Mikayel Mkrtichyan; Shamim Ahmad; Mason Webb; Eslam Mohamed; Grigori Okoev; Adelaida Matevosyan; Rajeev Shrimali; Rasha Abu Eid; Scott Hammond; John E. Janik; Samir N. Khleif

doi:10.1158/2326-6066.CIR-17-0223

Antigen-Specific antitumor responses induced by OX40 agonist are enhanced by the ido inhibitor indoximod

Zuzana Berrong, Mikayel Mkrtichyan, Shamim Ahmad, Mason Webb, Eslam Mohamed, Grigori Okoev, Adelaida Matevosyan, Rajeev Shrimali, Rasha Abu Eid, Scott Hammond, John E. Janik, Samir N. Khleif

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

12 Scopus citations

Abstract

Although an immune response to tumors may be generated using vaccines, so far, this approach has only shown minimal clinical success. This is attributed to the tendency of cancer to escape immune surveillance via multiple immune suppressive mechanisms. Successful cancer immunotherapy requires targeting these inhibitory mechanisms along with enhancement of antigen-specific immune responses to promote sustained tumor-specific immunity. Here, we evaluated the effect of indoximod, an inhibitor of the immunosuppressive indoleamine-(2,3)-dioxygenase (IDO) pathway, on antitumor efficacy of anti-OX40 agonist in the context of vaccine in the IDO TC-1 tumor model. We demonstrate that although the addition of anti-OX40 to the vaccine moderately enhances therapeutic efficacy, incorporation of indoximod into this treatment leads to enhanced tumor regression and cure of established tumors in 60% of treated mice. We show that the mechanisms by which the IDO inhibitor leads to this therapeutic potency include (i) an increment of vaccine-induced tumor-infiltrating effector T cells that is facilitated by anti-OX40 and (ii) a decrease of IDO enzyme activity produced by nontumor cells within the tumor microenvironment that results in enhancement of the specificity and the functionality of vaccine-induced effector T cells. Our findings suggest a translatable strategy to enhance the overall efficacy of cancer immunotherapy.

Original language	English (US)
Pages (from-to)	201-208
Number of pages	8
Journal	Cancer Immunology Research
Volume	6
Issue number	2
DOIs	https://doi.org/10.1158/2326-6066.CIR-17-0223
State	Published - Feb 2018
Externally published	Yes

Bibliographical note

Funding Information:
M. Mkrtichyan is a scientist at FivePrime Therapeutics Inc. J.E. Janik is executive director at Incyte. S.N. Khleif reports receiving a commercial research grant from MedImmune and is a consultant/advisory board member for New-Link. No potential conflicts of interest were disclosed by the other authors.

Publisher Copyright:
© 2018 American Association for Cancer Research.

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title = "Antigen-Specific antitumor responses induced by OX40 agonist are enhanced by the ido inhibitor indoximod",

abstract = "Although an immune response to tumors may be generated using vaccines, so far, this approach has only shown minimal clinical success. This is attributed to the tendency of cancer to escape immune surveillance via multiple immune suppressive mechanisms. Successful cancer immunotherapy requires targeting these inhibitory mechanisms along with enhancement of antigen-specific immune responses to promote sustained tumor-specific immunity. Here, we evaluated the effect of indoximod, an inhibitor of the immunosuppressive indoleamine-(2,3)-dioxygenase (IDO) pathway, on antitumor efficacy of anti-OX40 agonist in the context of vaccine in the IDO TC-1 tumor model. We demonstrate that although the addition of anti-OX40 to the vaccine moderately enhances therapeutic efficacy, incorporation of indoximod into this treatment leads to enhanced tumor regression and cure of established tumors in 60% of treated mice. We show that the mechanisms by which the IDO inhibitor leads to this therapeutic potency include (i) an increment of vaccine-induced tumor-infiltrating effector T cells that is facilitated by anti-OX40 and (ii) a decrease of IDO enzyme activity produced by nontumor cells within the tumor microenvironment that results in enhancement of the specificity and the functionality of vaccine-induced effector T cells. Our findings suggest a translatable strategy to enhance the overall efficacy of cancer immunotherapy.",

author = "Zuzana Berrong and Mikayel Mkrtichyan and Shamim Ahmad and Mason Webb and Eslam Mohamed and Grigori Okoev and Adelaida Matevosyan and Rajeev Shrimali and Eid, {Rasha Abu} and Scott Hammond and Janik, {John E.} and Khleif, {Samir N.}",

note = "Funding Information: M. Mkrtichyan is a scientist at FivePrime Therapeutics Inc. J.E. Janik is executive director at Incyte. S.N. Khleif reports receiving a commercial research grant from MedImmune and is a consultant/advisory board member for New-Link. No potential conflicts of interest were disclosed by the other authors. Publisher Copyright: {\textcopyright} 2018 American Association for Cancer Research.",

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AU - Berrong, Zuzana

AU - Mkrtichyan, Mikayel

AU - Ahmad, Shamim

AU - Webb, Mason

AU - Mohamed, Eslam

AU - Okoev, Grigori

AU - Matevosyan, Adelaida

AU - Shrimali, Rajeev

AU - Eid, Rasha Abu

AU - Hammond, Scott

AU - Janik, John E.

AU - Khleif, Samir N.

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N2 - Although an immune response to tumors may be generated using vaccines, so far, this approach has only shown minimal clinical success. This is attributed to the tendency of cancer to escape immune surveillance via multiple immune suppressive mechanisms. Successful cancer immunotherapy requires targeting these inhibitory mechanisms along with enhancement of antigen-specific immune responses to promote sustained tumor-specific immunity. Here, we evaluated the effect of indoximod, an inhibitor of the immunosuppressive indoleamine-(2,3)-dioxygenase (IDO) pathway, on antitumor efficacy of anti-OX40 agonist in the context of vaccine in the IDO TC-1 tumor model. We demonstrate that although the addition of anti-OX40 to the vaccine moderately enhances therapeutic efficacy, incorporation of indoximod into this treatment leads to enhanced tumor regression and cure of established tumors in 60% of treated mice. We show that the mechanisms by which the IDO inhibitor leads to this therapeutic potency include (i) an increment of vaccine-induced tumor-infiltrating effector T cells that is facilitated by anti-OX40 and (ii) a decrease of IDO enzyme activity produced by nontumor cells within the tumor microenvironment that results in enhancement of the specificity and the functionality of vaccine-induced effector T cells. Our findings suggest a translatable strategy to enhance the overall efficacy of cancer immunotherapy.

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Antigen-Specific antitumor responses induced by OX40 agonist are enhanced by the ido inhibitor indoximod

Abstract

Bibliographical note

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