2021
DOI: 10.3390/bioengineering8070090
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Reengineering Tumor Microenvironment with Sequential Interleukin Delivery

Abstract: Some cytokines can reengineer anti-tumor immunity to modify the tumor micro-environment. Interleukin-27 (IL-27) can partially reduce tumor growth in several animal models, including prostate cancer. We hypothesized that addition of IL-18, which can induce the proliferation of several immune effector cells through inducing IFNγ could synergize with IL-27 to enhance tumor growth control. We describe our findings on the effects of IL-27 gene delivery on prostate cancer cells and how sequential therapy with IL-18 … Show more

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Cited by 8 publications
(9 citation statements)
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“…As expected, upregulated genes in response to IL27 treatment were positively co-expressed with IL27 in both human prostate cancer (GSE32448; FDR = 0.014, NES = 1.47; Figure 4D) and human melanoma cancer (TCGA-SKCM; FDR = 0.000, NES = 3.33; Figure 4E), further supporting IL27 as a driver gene. Moreover, tumor volume for the control group was observed to be significantly larger than that in IL27 overexpressing group in a previously reported study (23). Altogether, these combined analyses suggest that IL27 acts as a driver gene and has an anti-tumor effect.…”
Section: Validation Of Biological Function Of Il27supporting
confidence: 62%
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“…As expected, upregulated genes in response to IL27 treatment were positively co-expressed with IL27 in both human prostate cancer (GSE32448; FDR = 0.014, NES = 1.47; Figure 4D) and human melanoma cancer (TCGA-SKCM; FDR = 0.000, NES = 3.33; Figure 4E), further supporting IL27 as a driver gene. Moreover, tumor volume for the control group was observed to be significantly larger than that in IL27 overexpressing group in a previously reported study (23). Altogether, these combined analyses suggest that IL27 acts as a driver gene and has an anti-tumor effect.…”
Section: Validation Of Biological Function Of Il27supporting
confidence: 62%
“…Although we have observed that IL27 was linked to enhanced immune response as described above, it remained unclear whether IL27 was a driver of the immune response or simply a passenger. To further validate the effects of IL27 on the biological function of tumors in vivo , we searched and found an ideal dataset (GSE178142) ( 23 ), including RNA-seq data from control mice (GSM5380810 and GSM5380811) and IL27 overexpressing mice treated intramuscularly with plasmids containing IL27 (GSM5380806 and GSM5380807). We downloaded RNA-seq data for control mice and experimental mice, and converted the ensemble ID to gene symbol.…”
Section: Resultsmentioning
confidence: 99%
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“…We have also shown a role of IL-27 in impacting bone-cell differentiation and proliferation [ 6 ]. We previously examined a first-generation IL-27 targeted at the C-terminus with a short ‘peptide L’ (pepL, LSLITRL), which binds the interleukin 6 receptor α (IL-6Rα) that is upregulated in tumor cells [ 7 ] in order to reduce prostate tumor growth (IL-27pepL or 27pepL) [ 4 , 8 , 9 ].…”
Section: Introductionmentioning
confidence: 99%
“…IL-27 can also serve as an effective bone-normalization agent due to its impact on pro-osteogenic-gene changes in both osteoblasts and osteoclasts [ 6 ]. Additionally, IL-27 exhibits immunomodulatory activity capable of promoting the accumulation of tumor-clearing effector cells at the site of prostate-cancer bone metastases [ 4 , 9 ].…”
Section: Introductionmentioning
confidence: 99%