Article

The prognostic value of FoxP3+ tumor-infiltrating lymphocytes in cancer: a critical review of the literature.

Trev and Joyce Deeley Research Centre, British Columbia Cancer Agency, University of Victoria, Victoria, Canada.
Clinical Cancer Research (impact factor: 7.74). 04/2012; 18(11):3022-9. DOI:10.1158/1078-0432.CCR-11-3216
Source: PubMed

ABSTRACT CD8+ tumor-infiltrating lymphocytes (TIL) are associated with survival in a variety of cancers. A second subpopulation of TIL, defined by forkhead box protein P3 (FoxP3) expression, has been reported to inhibit tumor immunity, resulting in decreased patient survival. On the basis of this premise, several groups are attempting to deplete FoxP3+ T cells to enhance tumor immunity. However, recent studies have challenged this paradigm by showing that FoxP3+ T cells exhibit heterogeneous phenotypes and, in some cohorts, are associated with favorable prognosis. These discrepant results could arise from differences in study methodologies or the biologic properties of specific cancer types. Here, we conduct the first systematic review of the prognostic significance of FoxP3+ T cells across nonlymphoid cancers (58 studies from 16 cancers). We assessed antibody specificity, cell-scoring strategy, multivariate modeling, use of single compared with multiple markers, and tumor site. Two factors proved important. First, when FoxP3 was combined with one additional marker, double-positive T cells were generally associated with poor prognosis. Second, tumor site had a major influence. FoxP3+ T cells were associated with poor prognosis in hepatocellular cancer and generally good prognosis in colorectal cancer, whereas other cancer types were inconsistent or understudied. We conclude that FoxP3+ T cells have heterogeneous properties that can be discerned by the use of additional markers. Furthermore, the net biologic effects of FoxP3+ T cells seem to depend on the tumor site, perhaps reflecting microenvironmental differences. Thus, depletion of FoxP3+ T cells might enhance tumor immunity in some patient groups but be detrimental in others.

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Keywords

16 cancers
 
additional marker
 
additional markers
 
antibody specificity
 
CD8+ tumor-infiltrating lymphocytes
 
cell-scoring strategy
 
double-positive T cells
 
favorable prognosis
 
first systematic review
 
good prognosis
 
multiple markers
 
multivariate modeling
 
net biologic effects
 
nonlymphoid cancers
 
patient survival
 
poor prognosis
 
prognostic significance
 
second subpopulation
 
specific cancer types
 
tumor immunity
 

Ron J Deleeuw