Age-related tumor growth in mice is related to integrin α 4 in CD8+ T cells
Juhyun Oh, Angela Magnuson, Christophe Benoist, Mikael J. Pittet, Ralph Weissleder
Juhyun Oh, Angela Magnuson, Christophe Benoist, Mikael J. Pittet, Ralph Weissleder
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Research Article Aging Immunology

Age-related tumor growth in mice is related to integrin α 4 in CD8+ T cells

Abstract

Cancer incidence increases with age, but paradoxically, cancers have been found to grow more quickly in young mice compared with aged ones. The cause of differential tumor growth has been debated and, over time, attributed to faster tumor cell proliferation, decreased tumor cell apoptosis, and/or increased angiogenesis in young animals. Despite major advances in our understanding of tumor immunity over the past 2 decades, little attention has been paid to comparing immune cell populations in young and aged mice. Using mouse colon adenocarcinoma model MC38 implanted in young and mature mice, we show that age substantially influences the number of tumor-infiltrating cytotoxic CD8+ T cells, which control cancer progression. The different tumor growth pace in young and mature mice was abrogated in RAG1null mice, which lack mature T and B lymphocytes, and upon selective depletion of endogenous CD8+ cells. Transcriptome analysis further indicated that young mice have decreased levels of the Itga4 gene (CD49d, VLA-4) in tumor-infiltrating lymphocytes when compared with mature mice. Hypothesizing that VLA-4 can have a tumor-protective effect, we depleted the protein, which resulted in accelerated tumor growth in mature mice. These observations may explain the paradoxical growth rates observed in murine cancers, point to the central role of VLA-4 in controlling tumor growth, and open new venues to therapeutic manipulation.

Authors

Juhyun Oh, Angela Magnuson, Christophe Benoist, Mikael J. Pittet, Ralph Weissleder

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Figure 4

Tumor-infiltrating CD49dhiCD8+ T cells show higher cytotoxic and effector status than CD49dlo cells.

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Tumor-infiltrating CD49dhiCD8+ T cells show higher cytotoxic and effecto...
S.c. MC38 tumors were harvested on day 14 after implantation and assessed for expression levels of (A) granzyme B (n = 10), (B) IFN-γ (n = 6), (C) CD44 (n = 10), and (D) Ki-67 (n = 7) in tumor-infiltrating CD49d+ and CD49dCD8+ T cells of mature mice by flow cytometry. IFN-γ level was measured after restimulation in vitro. Histograms were presented in comparison with unstained controls for granzyme B, CD44, and Ki-67 or with unstimulated control for IFN-γ (gray lines). Each line of before-after graphs represents individual tumors of mature mice. P values were calculated based on the 2-tailed paired t test between CD49d+ and CD49dCD8+ T cell subsets in each tumor. (E) Linear regression model shows positive correlation between the frequency of CD49d+CD8+ T cells and the number of infiltrating CD8+ T cells. (F) Linear regression analysis between the frequency of CD49d+CD8+ T cells and the frequency of Ki-67–expressing CD8+ T cells. Each dot in E and F represents individual tumor samples of mature mice.