Mitigating age-related immune dysfunction heightens the efficacy of tumor immunotherapy in aged mice.

نویسندگان

  • Vincent Hurez
  • Benjamin J Daniel
  • Lishi Sun
  • Ai-Jie Liu
  • Sara M Ludwig
  • Mark J Kious
  • Suzanne R Thibodeaux
  • Srilakshmi Pandeswara
  • Kruthi Murthy
  • Carolina B Livi
  • Shawna Wall
  • Michael J Brumlik
  • Tahiro Shin
  • Bin Zhang
  • Tyler J Curiel
چکیده

Although cancer tends to affect the elderly, most preclinical studies are carried out in young subjects. In this study, we developed a melanoma-specific cancer immunotherapy that shows efficacy in aged but not young hosts by mitigating age-specific tumor-associated immune dysfunction. Both young and aged CD4(+)CD25(hi) regulatory T cells (Treg) exhibited equivalent in vitro T-cell suppression and tumor-associated augmentation in numbers. However, denileukin diftitox (DT)-mediated Treg depletion improved tumor-specific immunity and was clinically effective only in young mice. DT-mediated Treg depletion significantly increased myeloid-derived suppressor cell (MDSC) numbers in aged but not young mice, and MDSC depletion improved tumor-specific immunity and reduced tumor growth in aged mice. Combining Treg depletion with anti-Gr-1 antibody was immunologically and clinically more efficacious than anti-Gr-1 antibody alone in aged B16-bearing mice, similar to Treg depletion alone in young mice. In contrast, DT increased MDSCs in young and aged mice following MC-38 tumor challenge, although effects were greater in aged mice. Anti-Gr-1 boosted DT effects in young but not aged mice. Aged antitumor immune effector cells are therefore competent to combat tumor when underlying tumor-associated immune dysfunction is appropriately mitigated, but this dysfunction varies with tumor, thus also varying responses to immunotherapy. By tailoring immunotherapy to account for age-related tumor-associated immune dysfunctions, cancer immunotherapy for aged patients with specific tumors can be remarkably improved.

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عنوان ژورنال:
  • Cancer research

دوره 72 8  شماره 

صفحات  -

تاریخ انتشار 2012