ΔPK oncolytic activity includes modulation of the tumour cell milieu

Bollino, Dominique; Nghiem, Paul; Li, Baiquan; Aurelian, Laure

doi:10.1099/jgv.0.000353

Cited by 28 publications

(29 citation statements)

References 75 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…46 Simultaneously, ΔPK could activate JNK protein activity to suppress the expression of IL-10, which is an immunosuppressive factor. 47 On the basis of these results, we believe that FSTL1 plays a critical role in immune regulation by increasing the antigen presentation ability of DCs and T lymphocytes through altering NF-κb and JNK expression.…”

Section: Discussionmentioning

confidence: 83%

Follistatin‐like protein 1 contributes to dendritic cell and T‐lymphocyte activation in nasopharyngeal carcinoma patients by altering nuclear factor κb and Jun N‐terminal kinase expression

Wang

Huang

et al. 2016

Cell Biochemistry & Function

View full text Add to dashboard Cite

Follistatin‐like protein 1 (FSTL1) is a newly characterized protein that can regulate the immune response in various ways. Dendritic cells (DCs) are central to immune regulation. In this study, we explored the impact of FSTL1 on DC activity in nasopharyngeal carcinoma (NPC) patients. The surface expression of CD40, CD86, and HLA‐DR on DCs was analyzed and showed significantly elevated expression levels, indicating DC maturity. After FSTL1 was added to DCs collected from NPC patients (n = 50), controls (n = 47), and healthy donors (n = 10), interferon γ secretion and T‐cell receptor expression in cytotoxic T lymphocytes were also investigated. In the experimental groups, the expression of the critical immune protein nuclear factor (NF)‐κb was upregulated, whereas Jun N‐terminal kinase (JNK) was downregulated. Our findings demonstrate that FSTL1 plays a critical role in immune regulation, enhancing the antigen presentation ability of DCs by up‐regulating NF‐κb expression and down‐regulating JNK expression.

show abstract

Section: Discussionmentioning

confidence: 83%

Follistatin‐like protein 1 contributes to dendritic cell and T‐lymphocyte activation in nasopharyngeal carcinoma patients by altering nuclear factor κb and Jun N‐terminal kinase expression

Wang

Huang

et al. 2016

Cell Biochemistry & Function

View full text Add to dashboard Cite

show abstract

“…MICA induction resulted from virus replication and JNK/c-Jun-dependent inhibition of secretion of the immunosuppressive cytokine IL-10 by melanoma cells. 51 Further studies are needed to better understand the relative contribution of different death pathways, including ICD, to the OV clinical efficacy.…”

Section: Ovs As Antitumor Vaccines: the Icd Connectionmentioning

confidence: 99%

“…However, OVs that naturally induce the secretion of multiple inflammatory cytokines (without genetic modification) ( Table 3 ) are desirable, particularly if they simultaneously inhibit tumor-promoting immunosuppressive functions, as we have recently shown for the HSV-2 OV, ΔPK. 51 Additional studies are needed in order to better understand these contributions, particularly within the context of different tumor types.…”

Section: Transgene Arming Enhances the Ov Antitumor Activitymentioning

confidence: 99%

Oncolytic viruses as immunotherapy: progress and remaining challenges

Aurelian

2016

OTT

Self Cite

View full text Add to dashboard Cite

Oncolytic viruses (OVs) comprise an emerging cancer therapeutic modality whose activity involves both direct tumor cell lysis and the induction of immunogenic cell death (ICD). Cellular proteins released from the OV-lysed tumor cells, known as damage-associated molecular patterns and tumor-associated antigens, activate dendritic cells and elicit adaptive antitumor immunity. Interaction with the innate immune system and the development of long-lasting immune memory also contribute to OV-induced cell death. The degree to which the ICD component contributes to the clinical efficacy of OV therapy is still unclear. Modulation of a range of immune interactions may be beneficial or detrimental in nature and the interactions depend on the specific tumor, the site and extent of the disease, the immunosuppressive tumor microenvironment, the OV platform, the dose, time, and delivery conditions, as well as individual patient responses. To enhance the contribution of ICD, OVs have been engineered to express immunostimulatory genes and strategies have been developed to combine OV therapy with chemo- and immune-based therapeutic regimens. However, these approaches carry the risk that they may also be tolerogenic depending on their levels and the presence of other cytokines, their direct antiviral effects, and the timing and conditions of their expression. The contribution of autophagy to adaptive immunity, the ability of the OVs to kill cancer stem cells, and the patient’s baseline immune status are additional considerations. This review focuses on the complex and as yet poorly understood balancing act that dictates the outcome of OV therapy. We summarize current understanding of the OVs’ function in eliciting antitumor immunity and its relationship to therapeutic efficacy. Also discussed are the criteria involved in restraining antiviral immune responses and minimizing pathology while promoting antitumor immunity to override immune tolerance.

show abstract

“…A HSV-2 mutant lacking part of the R1 N-terminal domain (ICP10ΔPK) replicated less efficiently in serum-starved cells and exhibited reduced virulence in animals, despite still being able to complex with R2 and catalyze dNTP synthesis ( 210 , 211 ). This virus is being tested as a candidate vaccine against genital herpes ( 212 ) but can also control the growth of human melanoma xenografts in nude mice ( 213 , 214 ). A similar version of this virus, called FusOn-H2, also exhibited growth restriction in serum-starved cells and controlled growth of xenografted human MDA-MB-435 melanomas ( 168 ) and EC9706 esophageal tumors ( 215 ) in nude mice.…”

Section: Herpes Simplex Virusesmentioning

confidence: 99%

Targeting Nucleotide Biosynthesis: A Strategy for Improving the Oncolytic Potential of DNA Viruses

2017

View full text Add to dashboard Cite

The rapid growth of tumors depends upon elevated levels of dNTPs, and while dNTP concentrations are tightly regulated in normal cells, this control is often lost in transformed cells. This feature of cancer cells has been used to advantage to develop oncolytic DNA viruses. DNA viruses employ many different mechanisms to increase dNTP levels in infected cells, because the low concentration of dNTPs found in non-cycling cells can inhibit virus replication. By disrupting the virus-encoded gene(s) that normally promote dNTP biosynthesis, one can assemble oncolytic versions of these agents that replicate selectively in cancer cells. This review covers the pathways involved in dNTP production, how they are dysregulated in cancer cells, and the various approaches that have been used to exploit this biology to improve the tumor specificity of oncolytic viruses. In particular, we compare and contrast the ways that the different types of oncolytic virus candidates can directly modulate these processes. We limit our review to the large DNA viruses that naturally encode homologs of the cellular enzymes that catalyze dNTP biogenesis. Lastly, we consider how this knowledge might guide future development of oncolytic viruses.

show abstract

ΔPK oncolytic activity includes modulation of the tumour cell milieu

Cited by 28 publications

References 75 publications

Follistatin‐like protein 1 contributes to dendritic cell and T‐lymphocyte activation in nasopharyngeal carcinoma patients by altering nuclear factor κb and Jun N‐terminal kinase expression

Follistatin‐like protein 1 contributes to dendritic cell and T‐lymphocyte activation in nasopharyngeal carcinoma patients by altering nuclear factor κb and Jun N‐terminal kinase expression

Oncolytic viruses as immunotherapy: progress and remaining challenges

Targeting Nucleotide Biosynthesis: A Strategy for Improving the Oncolytic Potential of DNA Viruses

Contact Info

Product

Resources

About