2018
DOI: 10.1158/2326-6066.cir-17-0223
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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 immunosuppres… Show more

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Cited by 16 publications
(9 citation statements)
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“…To determine whether intra-tumoral T cells changed with D-1MT treatment, we used the pan T cell marker CD3. Similar to prior results in a syngeneic murine model of lung cancer 22 , we found no change in CD3 pos T cell frequency or absolute number with D-1MT treatment (Fig. 1D).…”
Section: Ido1 Pathway Inhibition Decreases Tumor Infiltrating B Cellssupporting
confidence: 91%
See 1 more Smart Citation
“…To determine whether intra-tumoral T cells changed with D-1MT treatment, we used the pan T cell marker CD3. Similar to prior results in a syngeneic murine model of lung cancer 22 , we found no change in CD3 pos T cell frequency or absolute number with D-1MT treatment (Fig. 1D).…”
Section: Ido1 Pathway Inhibition Decreases Tumor Infiltrating B Cellssupporting
confidence: 91%
“…C57BL/6 mice (The Jackson Laboratory) were housed in a pathogen-free environment, and experimental protocols were approved by the Johns Hopkins Institutional Animal Care and Use Committee. Similar to others studying the role of IDO1 in cancer 21,22 , female mice were used.…”
Section: Mice and Cell Linesmentioning
confidence: 99%
“…Administering indoximod with the PD-1 antibody pembrolizumab (Keytruda) led to a 61% overall response rate, including 10 complete responses (20%) and 21 partial responses (41%), in patients with advanced melanoma. The median progression-free survival under combinatorial treatment was 12.9 months, with a 1-year rate of 56%, suggesting a synergistic antitumor therapeutic effect [ 71 ].…”
Section: Ido1 Inhibitors In Preclinical Development and Clinical Triamentioning
confidence: 99%
“…The addition of IDO inhibitors is required to induce anticancer effects in several models of cancer. For example, HPV16-E6-E7/HRAS-driven lung epithelial cancer was suppressed by only the combination of HPV16 E7 vaccines, OX40 agonists, and IDO inhibitors 63 . Furthermore, Berrong et al 63 showed that while the addition of anti-OX40 to an antigen-specific cancer vaccine moderately enhanced therapeutic efficacy, it was the addition of an IDO inhibitor to this treatment that eventually led to complete regression of established tumors in 60% of treated mice.…”
Section: Downstream Of Ido Ahr Is Activated By Viral Infectionmentioning
confidence: 99%
“…For example, HPV16-E6-E7/HRAS-driven lung epithelial cancer was suppressed by only the combination of HPV16 E7 vaccines, OX40 agonists, and IDO inhibitors 63 . Furthermore, Berrong et al 63 showed that while the addition of anti-OX40 to an antigen-specific cancer vaccine moderately enhanced therapeutic efficacy, it was the addition of an IDO inhibitor to this treatment that eventually led to complete regression of established tumors in 60% of treated mice. Additionally, in agreement with our data, Sagiv-Barfi and colleagues combined intratumoral delivery of an adenovirusrelated TLR9 ligand with OX40 activation to increase anticancer T cell responses 64 .…”
Section: Downstream Of Ido Ahr Is Activated By Viral Infectionmentioning
confidence: 99%