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1. Investigating the effect of reduced temperatures on the efficacy of rhabdovirus-based viral vector platforms.

2. Recombinant Newcastle disease viruses expressing immunological checkpoint inhibitors induce a pro-inflammatory state and enhance tumor-specific immune responses in two murine models of cancer.

3. A promoterless AAV6.2FF-based lung gene editing platform for the correction of surfactant protein B deficiency.

4. Kinetic analysis of oncolytic OrfV-induced innate and adaptive immune responses in a murine model of late-stage ovarian cancer.

5. Multiplex flow cytometry-based assay for quantifying tumor- and virus-associated antibodies induced by immunotherapies.

6. The Role of Neutrophils in Oncolytic Orf Virus-Mediated Cancer Immunotherapy.

7. Oncolytic Orf virus licenses NK cells via cDC1 to activate innate and adaptive antitumor mechanisms and extends survival in a murine model of late-stage ovarian cancer.

8. AAV-Vectored Expression of the Vascular Normalizing Agents 3TSR and Fc3TSR, and the Anti-Angiogenic Bevacizumab Extends Survival in a Murine Model of End-Stage Epithelial Ovarian Carcinoma.

9. Using a Prime-Boost Vaccination Strategy That Proved Effective for High Resolution Epitope Mapping to Characterize the Elusive Immunogenicity of Survivin.

10. Production and purification of high-titer OrfV for preclinical studies in vaccinology and cancer therapy.

11. Mechanisms that allow vaccination against an oncolytic vesicular stomatitis virus-encoded transgene to enhance safety without abrogating oncolysis.

12. Combining vanadyl sulfate with Newcastle disease virus potentiates rapid innate immune-mediated regression with curative potential in murine cancer models.

13. Tumour vasculature: Friend or foe of oncolytic viruses?

14. A lung tropic AAV vector improves survival in a mouse model of surfactant B deficiency.

15. Optimized Pre-Clinical Grade Production of Two Novel Lentiviral Vector Pseudotypes for Lung Gene Delivery.

16. Quantifying Antibody Responses Induced by Antigen-Agnostic Immunotherapies.

17. Combining Vascular Normalization with an Oncolytic Virus Enhances Immunotherapy in a Preclinical Model of Advanced-Stage Ovarian Cancer.

18. Myeloid Cells during Viral Infections and Inflammation.

19. Quantifying Antigen-Specific T Cell Responses When Using Antigen-Agnostic Immunotherapies.

20. Use of Precision-Cut Lung Slices as an Ex Vivo Tool for Evaluating Viruses and Viral Vectors for Gene and Oncolytic Therapy.

21. Critical Interactions between Immunogenic Cancer Cell Death, Oncolytic Viruses, and the Immune System Define the Rational Design of Combination Immunotherapies.

22. Immune responses in the thyroid cancer microenvironment: making immunotherapy a possible mission.

23. Enhancing Immune Responses to Cancer Vaccines Using Multi-Site Injections.

24. Truncation of the enzootic nasal tumor virus envelope protein cytoplasmic tail increases Env-mediated fusion and infectivity.

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