Neuropilin‐1 expression identifies a subset of regulatory T cells in human lymph nodes that is modulated by preoperative chemoradiation therapy in cervical cancer

Abstract: Neuropilin-1 expression identifies a subset of regulatory T cells in human lymph nodes that is modulated by preoperative chemoradiation therapy in cervical cancer Introduction CD4 + T cells that constitutively express the interleukin-2 (IL-2) receptor a-chain CD25 (regulatory T cells, Treg) and the master regulator Foxp3 transcription factor play a central and prominent role in maintaining self-tolerance and in regulating responses to infectious agents, transplantation antigens and tumour antigens. SummaryWe … Show more

“…11,14,15) This result suggests that, to assess the response to induction CRT not only reduced tumor size or metabolic status of the tumor shown on CT or 18 F-deoxyglucose positron emission tomography but patient's immune response to the therapy also can be employed. Low tumor-infiltrating FOXP3+ Treg density was associated with favorable prognosis, although the difference was not statistically significant, as expected from its strong correlation with the pathological response and the impact of the pathological response on prognosis, suggesting that Tregs may be a possible target for adjunct immunotherapy.…”

“…In breast cancer patients treated with neoadjuvant chemotherapy, low infiltration of FOXP3+ Tregs with or without high CD8+ T cells was reported to be highly associated with good pathological response 11) or favorable prognosis. 12,13) Low FOXP3+ Treg density in the tumor stroma of ovarian cancer patients treated with neoadjuvant chemotherapy 14) or in the tumor-draining lymph nodes of patients with cervical cancer who underwent induction CRT 15) was also shown to be a favorable prognostic factor. To date, the effects of CRT on tumor-infiltrating T cells in patients with NSCLC are largely unknown.…”

Density of Tumor-Infiltrating FOXP3+ T Cells as a Response Marker for Induction Chemoradiotherapy and a Potential Prognostic Factor in Patients Treated with Trimodality Therapy for Locally Advanced Non-Small Cell Lung Cancer

“…11,14,15) This result suggests that, to assess the response to induction CRT not only reduced tumor size or metabolic status of the tumor shown on CT or 18 F-deoxyglucose positron emission tomography but patient's immune response to the therapy also can be employed. Low tumor-infiltrating FOXP3+ Treg density was associated with favorable prognosis, although the difference was not statistically significant, as expected from its strong correlation with the pathological response and the impact of the pathological response on prognosis, suggesting that Tregs may be a possible target for adjunct immunotherapy.…”

“…In breast cancer patients treated with neoadjuvant chemotherapy, low infiltration of FOXP3+ Tregs with or without high CD8+ T cells was reported to be highly associated with good pathological response 11) or favorable prognosis. 12,13) Low FOXP3+ Treg density in the tumor stroma of ovarian cancer patients treated with neoadjuvant chemotherapy 14) or in the tumor-draining lymph nodes of patients with cervical cancer who underwent induction CRT 15) was also shown to be a favorable prognostic factor. To date, the effects of CRT on tumor-infiltrating T cells in patients with NSCLC are largely unknown.…”

Density of Tumor-Infiltrating FOXP3+ T Cells as a Response Marker for Induction Chemoradiotherapy and a Potential Prognostic Factor in Patients Treated with Trimodality Therapy for Locally Advanced Non-Small Cell Lung Cancer

“…Since two previous reports had identified Nrp-1-expressing T cells in human tonsils [14] and lymph nodes [15], we further analyzed our data focusing on such subsets. Nrp-1-expressing T cells were variably abundant in secondary lymphoid organs, but consistently rare in peripheral blood ( Fig.…”

Neuropilin‐1 is not a marker of human Foxp3⁺ Treg

“…This finding indicates that HCV_G1_p7_794 induces the conversion of conventional CD4 + FoxP3 -T cells to T reg cells, i.e., infectious tolerance, a suggestion supported by studies demonstrating the inability of nT reg cells to proliferate in response to their cognate antigen in vitro [34]. Furthermore, in contrast to Ab + VL + PBMCs cultured in medium alone, only a minority of CD3 + CD4 + FoxP3 + cells cultured in the presence of HCV_G1_p7_794 expressed CD304 (neuropilin), which is expressed by a subset of FoxP3 + T reg cells in humans and associated specifically with nT reg cells in mice [21,22]. While it has been suggested alternatively that the expanded T reg cell population in chronic, HCV infected patients is composed of cells phenotypically similar to nT reg or iT reg cells [11,20], our results concur with the consensus that the expanded T reg cell population in chronic HCV-infected patients is heterogeneous, composed of both T reg cell subsets.…”

“…CD304 (neuropilin-1) is expressed by a subset of FoxP3 + T reg cells in humans [21]. In mice, CD304 expression differentiates natural (CD304 + ), from inducible (CD304 -), T reg cells [22].…”

HCV epitope, homologous to multiple human protein sequences, induces a regulatory T cell response in infected patients