T Cell Costimulatory and Inhibitory Receptors as Therapeutic Targets for Inducing Anti-Tumor Immunity

Foell, Jeurgen; Hewes, Becker

doi:10.2174/156800907780006841

Cited by 26 publications

(25 citation statements)

References 139 publications

(175 reference statements)

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“…Signal transduction through the TCR pathway is recognized as an essential event required for resting T cells to enter the cell cycle and proliferate [22]. A second signal provided by ligation through the CD28 receptor protein augments TCR signaling and enables maximal T cell activation and proliferation [22]. Thus, our findings revealing a spectrum of toxicity profiles that correlate with the activation status and proliferative capacity of the cell supports the hypothesis that ZnO NP preferentially target rapidly dividing cells.…”

Section: Discussionsupporting

confidence: 78%

“…This hypothesis is further supported by studies comparing responses in healthy primary resting T cells to identical cultures in which cells were either activated through the T cell receptor signaling pathway or via both TCR and CD28 costimulation pathways (figure 1). Signal transduction through the TCR pathway is recognized as an essential event required for resting T cells to enter the cell cycle and proliferate [22]. A second signal provided by ligation through the CD28 receptor protein augments TCR signaling and enables maximal T cell activation and proliferation [22].…”

Section: Discussionmentioning

confidence: 99%

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Preferential killing of cancer cells and activated human T cells using ZnO nanoparticles

Hanley¹,

Cory²,

Layne³

et al. 2008

Nanotechnology

579

382

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Nanoparticles are increasingly being recognized for their potential utility in biological applications including nanomedicine. Here we examine the response of normal human cells to ZnO nanoparticles under different signaling environments and compare it to the response of cancerous cells. ZnO nanoparticles exhibit a strong preferential ability to kill cancerous T cells (∼28-35×) compared to normal cells. Interestingly, the activation state of the cell contributes toward nanoparticle toxicity, as resting T cells display a relative resistance while cells stimulated through the T cell receptor and CD28 costimulatory pathway show greater toxicity in direct relation to the level of activation. Mechanisms of toxicity appear to involve the generation of reactive oxygen species, with cancerous T cells producing higher inducible levels than normal T cells. In addition, nanoparticles were found to induce apoptosis and the inhibition of reactive oxygen species was found to be protective against nanoparticle induced cell death. The novel findings of cell selective toxicity, towards potential disease causing cells, indicate a potential utility of ZnO nanoparticles in the treatment of cancer and/ or autoimmunity.

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Section: Discussionsupporting

confidence: 78%

Section: Discussionmentioning

confidence: 99%

Preferential killing of cancer cells and activated human T cells using ZnO nanoparticles

Hanley¹,

Cory²,

Layne³

et al. 2008

Nanotechnology

579

382

View full text Add to dashboard Cite

show abstract

“…PD-1 is expressed by B cells, T lymphocytes (activated but not resting), and myeloid cells, in contrast to the more restricted expression of CD28 and CD152. PD-1 is also expressed in the thymus primarily on CD4 – CD8 – T cells, during this transition from double negative to double positive [17]. B7-H1 binds its receptor PD-1 along with another ligand, B7-DC.…”

Section: Introductionmentioning

confidence: 99%

Stimulation of Human CD4+ T Lymphocytes via TLR3, TLR5 and TLR7/8 Up-Regulates Expression of Costimulatory and Modulates Proliferation

Simone¹,

Floriani²,

Saverino³

2009

TOMICROJ

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The cells of innate and adaptive immunity, although activated by different ligands, engage in cross talk to ensure a successful immune outcome. Toll-like receptors (TLRs) are key components of the innate immune system and have the ability to detect microbial infection and trigger host defence responses. Otherwise, human T lymphocytes are able to produce most TLRs. Thus, we analyze the capability of some TLR ligands to modulate the function of highly-purified CD4+ T cells. We found that agents acting via TLRs (poly I:C, a TLR3 ligand; flagellin, a TLR5 ligand; and R848, a TLR7/8 ligand) are able to regulate the expression of costimulatory molecules both on purified antigen presenting cells and on purified T lymphocytes. Moreover, the activation mediated by TLRs determines a kinetic expression of B7-family members such as through an inhibition of T lymphocytes delayed proliferation. These findings suggest a functional role of some invading microorganisms in regulating acquired immunity.

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“…Cells of the MNP, e.g. present antigens to B-and T lymphocytes as well as co-regulate lymphocytes via direct interaction of CD80 ⁄ 86 to CD28 on lymphocytes [3]. Furthermore, these cells secrete cytokines and other substances, e.g.…”

Section: Introductionmentioning

confidence: 99%

Co‐culture of Head and Neck Squamous Cell Carcinoma Spheroids with Autologous Monocytes Predicts Prognosis

et al. 2008

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Co‐culture of monocytes with autologous fragment (F) spheroids originating from malignant (M) tumour or benign (B) control mucosa of head and neck squamous cell carcinoma (HNSCC) yields interleukin (IL)‐6 and monocyte chemo‐attractant protein (MCP)‐1 secretion. This study investigates the association between this cytokine co‐culture response and prognosis. Analysis of IL‐6 and MCP‐1 content of supernatants from monocytes in vitro co‐culture with autologous MF‐ or BF‐spheroids was investigated in a cohort of HNSCC patients (n = 65) diagnosed between 1998 and 2005, all of whom were treated with curative intent by primary surgery. The IL‐6 response was expressed as a fraction of the lipopolysaccharid response of the same batch of monocytes. Recurrence, survival and causes of death were then established following the second part of 2005. MCP‐1 levels did not predict prognosis. We found that increased levels of IL‐6 from autologous monocytes in co‐culture with MF‐spheroids predicted recurrence with a hazard ratio (HR) of 1.5 [confidence interval (CI): 1.01–2.60; P = 0.05] and co‐culture with BF‐spheroids and monocytes predicted recurrence (HR = 4.17; CI: 1.54–11.29; P = 0.005). The same results where obtained in addition with TNM stage of the patients. Simultaneous analysis of BF‐ and MF‐spheroid co‐culture IL‐6 responses as well as adjustment for age and TNM stage of the patients allowed prediction of total survival (HR = 3.1; CI: 1.11–8.56; P = 0.03) based on BF co‐culture levels. IL‐6 secreted upon in vitro co‐culture with monocytes and BF‐spheroids predicts recurrence and prognosis, whereas co‐culture with monocytes and MF‐spheroids predicts recurrence.

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T Cell Costimulatory and Inhibitory Receptors as Therapeutic Targets for Inducing Anti-Tumor Immunity

Cited by 26 publications

References 139 publications

Preferential killing of cancer cells and activated human T cells using ZnO nanoparticles

Preferential killing of cancer cells and activated human T cells using ZnO nanoparticles

Stimulation of Human CD4+ T Lymphocytes via TLR3, TLR5 and TLR7/8 Up-Regulates Expression of Costimulatory and Modulates Proliferation

Co‐culture of Head and Neck Squamous Cell Carcinoma Spheroids with Autologous Monocytes Predicts Prognosis

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