Growth differentiation factor-15 slows the growth of murine prostate cancer by stimulating tumor immunity.

Growth differentiation factor-15 slows the growth of murine prostate cancer by stimulating tumor immunity.

Growth Differentiation Factor-15 (GDF15) is a divergent TGF-beta superfamily cytokine that is overexpressed by most cancers and is induced by anticancer therapy. Transgenic and induced animal models suggest that it protects from cancer development but the mechanisms are uncertain. We investigated th...

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Main Authors: Yasmin Husaini, Vicky Wang-Wei Tsai, Rakesh Manandhar, Hong Ping Zhang, Ka Ki Michelle Lee-Ng, Hélène Lebhar, Christopher P Marquis, David A Brown, Samuel N Breit
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2020-01-01
Series:PLoS ONE
Online Access:https://doi.org/10.1371/journal.pone.0233846
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spelling doaj-c03491e8a640495c96e487c633b150be2021-03-03T21:49:09ZengPublic Library of Science (PLoS)PLoS ONE1932-62032020-01-01156e023384610.1371/journal.pone.0233846Growth differentiation factor-15 slows the growth of murine prostate cancer by stimulating tumor immunity.Yasmin HusainiVicky Wang-Wei TsaiRakesh ManandharHong Ping ZhangKa Ki Michelle Lee-NgHélène LebharChristopher P MarquisDavid A BrownSamuel N BreitGrowth Differentiation Factor-15 (GDF15) is a divergent TGF-beta superfamily cytokine that is overexpressed by most cancers and is induced by anticancer therapy. Transgenic and induced animal models suggest that it protects from cancer development but the mechanisms are uncertain. We investigated the role of immunity in GDF15 induced reduction in prostate cancer (PCa) growth. The C57BL/6 transgenic TRAMP prostate cancer prone mice were bred with mice that were immunodeficient and/or systemically overexpressed GDF15. We developed a novel orthotopic TRAMP PCa model in which primary TRAMP tumor cells were implanted into prostates of mice to reduce the study time. These mice were administered recombinant mouse GDF15, antibody to CD8, PD1 or their respective controls. We found that GDF15 induced protection from tumor growth was reversed by lack of adaptive immunity. Flow cytometric evaluation of lymphocytes within these orthotopic tumors showed that GDF15 overexpression was associated with increased CD8 T cell numbers and an increased number and proportion of recently activated CD8+CD11c+ T cells and a reduced proportion of "exhausted" CD8+PD1+ T cells. Further, depletion of CD8 T cells in tumor bearing mice abolished the GDF15 induced protection from tumor growth. Infusion of GDF15 into mice bearing orthotopic TRAMP tumor, substantially reduced tumor growth that was further reduced by concurrent PD1 antibody administration. GDF15 overexpression or recombinant protein protects from TRAMP tumor growth by modulating CD8 T cell mediated antitumor immunity and augments the positive effects of anti-PD1 blockers.https://doi.org/10.1371/journal.pone.0233846
collection DOAJ
language English
format Article
sources DOAJ
author Yasmin Husaini
Vicky Wang-Wei Tsai
Rakesh Manandhar
Hong Ping Zhang
Ka Ki Michelle Lee-Ng
Hélène Lebhar
Christopher P Marquis
David A Brown
Samuel N Breit
spellingShingle Yasmin Husaini
Vicky Wang-Wei Tsai
Rakesh Manandhar
Hong Ping Zhang
Ka Ki Michelle Lee-Ng
Hélène Lebhar
Christopher P Marquis
David A Brown
Samuel N Breit
Growth differentiation factor-15 slows the growth of murine prostate cancer by stimulating tumor immunity.
PLoS ONE
author_facet Yasmin Husaini
Vicky Wang-Wei Tsai
Rakesh Manandhar
Hong Ping Zhang
Ka Ki Michelle Lee-Ng
Hélène Lebhar
Christopher P Marquis
David A Brown
Samuel N Breit
author_sort Yasmin Husaini
title Growth differentiation factor-15 slows the growth of murine prostate cancer by stimulating tumor immunity.
title_short Growth differentiation factor-15 slows the growth of murine prostate cancer by stimulating tumor immunity.
title_full Growth differentiation factor-15 slows the growth of murine prostate cancer by stimulating tumor immunity.
title_fullStr Growth differentiation factor-15 slows the growth of murine prostate cancer by stimulating tumor immunity.
title_full_unstemmed Growth differentiation factor-15 slows the growth of murine prostate cancer by stimulating tumor immunity.
title_sort growth differentiation factor-15 slows the growth of murine prostate cancer by stimulating tumor immunity.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2020-01-01
description Growth Differentiation Factor-15 (GDF15) is a divergent TGF-beta superfamily cytokine that is overexpressed by most cancers and is induced by anticancer therapy. Transgenic and induced animal models suggest that it protects from cancer development but the mechanisms are uncertain. We investigated the role of immunity in GDF15 induced reduction in prostate cancer (PCa) growth. The C57BL/6 transgenic TRAMP prostate cancer prone mice were bred with mice that were immunodeficient and/or systemically overexpressed GDF15. We developed a novel orthotopic TRAMP PCa model in which primary TRAMP tumor cells were implanted into prostates of mice to reduce the study time. These mice were administered recombinant mouse GDF15, antibody to CD8, PD1 or their respective controls. We found that GDF15 induced protection from tumor growth was reversed by lack of adaptive immunity. Flow cytometric evaluation of lymphocytes within these orthotopic tumors showed that GDF15 overexpression was associated with increased CD8 T cell numbers and an increased number and proportion of recently activated CD8+CD11c+ T cells and a reduced proportion of "exhausted" CD8+PD1+ T cells. Further, depletion of CD8 T cells in tumor bearing mice abolished the GDF15 induced protection from tumor growth. Infusion of GDF15 into mice bearing orthotopic TRAMP tumor, substantially reduced tumor growth that was further reduced by concurrent PD1 antibody administration. GDF15 overexpression or recombinant protein protects from TRAMP tumor growth by modulating CD8 T cell mediated antitumor immunity and augments the positive effects of anti-PD1 blockers.
url https://doi.org/10.1371/journal.pone.0233846
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