Prevalence of regulatory T cells is increased in peripheral blood and tumor microenvironment of patients with pancreas or breast adenocarcinoma
- PMID: 12193750
- DOI: 10.4049/jimmunol.169.5.2756
Prevalence of regulatory T cells is increased in peripheral blood and tumor microenvironment of patients with pancreas or breast adenocarcinoma
Abstract
Regulatory T cells (T(reg)) that prevent autoimmune diseases by suppression of self-reactive T cells may also suppress the immune response against cancer. In mice, depletion of T(reg) by Ab therapy leads to more efficient tumor rejection. T(reg)-mediated suppression of antitumor immune responses may partly explain the poor clinical response to vaccine-based immunotherapy for human cancer. In this study, we measured the prevalence of T(reg) that coexpress CD4 and CD25 in the PBLs, tumor-infiltrating lymphocytes, and regional lymph node lymphocytes from 65 patients with either pancreas or breast cancer. In breast cancer patients (n = 35), pancreas cancer patients (n = 30), and normal donors (n = 35), the prevalence of T(reg) were 16. 6% (SE 1. 22), 13. 2% (SE 1. 13), and 8. 6% (SE 0. 71) of the total CD4(+) cells, respectively VSports手机版. The prevalence of T(reg) were significantly higher in breast cancer patients (p < 0. 01) and pancreas cancer patients (p < 0. 01) when compared with normal donors. In tumor-infiltrating lymphocytes and lymph node lymphocytes, the T(reg) prevalence were 20. 2% (SE 3. 93) and 20. 1% (SE 4. 3), respectively. T(reg) constitutively coexpressed CTLA-4 and CD45RO markers, and secreted TGF-beta and IL-10 but did not secrete IFN-gamma. When cocultured with activated CD8(+) cells or CD4(+)25(-) cells, T(reg) potently suppressed their proliferation and secretion of IFN-gamma. We conclude that the prevalence of T(reg) is increased in the peripheral blood as well as in the tumor microenvironment of patients with invasive breast or pancreas cancers. These T(reg) may mitigate the immune response against cancer, and may partly explain the poor immune response against tumor Ags. .
Publication types
- V体育安卓版 - Actions
- Actions (V体育安卓版)
MeSH terms
- Actions (VSports最新版本)
- "V体育2025版" Actions
- "V体育安卓版" Actions
- "VSports" Actions
- "VSports" Actions
- Actions (VSports)
- Actions (V体育2025版)
- Actions (V体育平台登录)
- "V体育2025版" Actions
- Actions (VSports在线直播)
- "VSports手机版" Actions
- V体育官网 - Actions
- Actions (VSports app下载)
- "V体育平台登录" Actions
- "VSports" Actions
- "V体育平台登录" Actions
- Actions (VSports在线直播)
- Actions (VSports手机版)
- "VSports app下载" Actions
- "VSports注册入口" Actions
- "V体育2025版" Actions
- VSports最新版本 - Actions
- "V体育ios版" Actions
- "VSports app下载" Actions
- V体育安卓版 - Actions
- "VSports注册入口" Actions
- V体育ios版 - Actions
- VSports app下载 - Actions
- V体育ios版 - Actions
Substances
- Actions (VSports在线直播)
- "VSports最新版本" Actions
- "V体育安卓版" Actions
- "V体育ios版" Actions
Grants and funding (VSports app下载)
VSports注册入口 - LinkOut - more resources
Full Text Sources
Other Literature Sources
Medical
Research Materials
