Introduction About 50% of human prostate cancers (PC) overexpress an ETS gene due to a translocation downstream of promoters of genes highly expressed in prostate. Half of 10 month-old transgenic mice with prostate overexpression of the ETS gene ETV4 (ETV4 mice) develop low-grade prostatic intraepithelial neoplasia. In comparison, almost all mice carrying both ETV4 overexpression and heterozygote Pten deletion (ETV4-Pten+/- mice) develop PC at 7 months, suggesting an oncogenic cooperation between these two common genetic alterations. Inflammatory and immune tumor-infiltrating cells may have a major role in tumor development. We are investigating if differences in the subsets of tumor-infiltrating cells may have a role in the above model of PC progression. Material and Methods ETV4 mice and mice with heterozygote Pten deletion were crossed to obtain mice with 4 different genotypes: WT, ETV4, Pten+/-, ETV4-Pten+/-. Tumor-infiltrating cells were characterized in 10 and 14 month-old mice. A single-cell suspension was obtained from shredded prostate tissues by using collagenase/hyaluronidase enzymes: inflammatory and immune infiltrating cells were identified by flow cytometry using an anti-CD45+ moAb, and further subtyped by appropriate antibodies in lymphoid (B-, T-, T-helper, T-suppressor lymphocytes and dendritic cells) and in myeloid (macrophages and neutrophils) cells. ? Results and discussion We analyzed 28 ten-month-old mice (>=6 for genotype) and 61 fourteen-month-old mice (>=13 for genotype). We found no differences in the frequency of prostate lymphoid infiltrating-cells at any age. In contrast, at any ages we found an increase of neutrophils in Pten-deleted mice, increase that was particularly high and significant in ETV4-Pten+/- mice. Furthermore, we investigated pro-inflammatory (M1) and anti-inflammatory (M2) activated macrophages. We found a higher percentage of M2 macrophages in both Pten+/- and ETV4-Pten+/- compared to WT and ETV4 mice. ? Conclusion The high frequency of anti-inflammatory activated macrophages (M2) in mice with Pten deletion suggests a role of Pten in macrophage regulation. The particularly high increase of neutrophils in mice with both ETV4 overexpression and Pten deletion (ETV4-Pten+/- mice) developing early PC, is in keeping with the high neutrophil/lymphocyte ratio found associated with poor prognosis in several cancers. The direct or indirect role of these genetic alterations in the increase of neutrophils needs to be investigated.
Myeloid tumor infiltrating cells in a mouse model of prostate cancer progression
De Angioletti Maria
2023
Abstract
Introduction About 50% of human prostate cancers (PC) overexpress an ETS gene due to a translocation downstream of promoters of genes highly expressed in prostate. Half of 10 month-old transgenic mice with prostate overexpression of the ETS gene ETV4 (ETV4 mice) develop low-grade prostatic intraepithelial neoplasia. In comparison, almost all mice carrying both ETV4 overexpression and heterozygote Pten deletion (ETV4-Pten+/- mice) develop PC at 7 months, suggesting an oncogenic cooperation between these two common genetic alterations. Inflammatory and immune tumor-infiltrating cells may have a major role in tumor development. We are investigating if differences in the subsets of tumor-infiltrating cells may have a role in the above model of PC progression. Material and Methods ETV4 mice and mice with heterozygote Pten deletion were crossed to obtain mice with 4 different genotypes: WT, ETV4, Pten+/-, ETV4-Pten+/-. Tumor-infiltrating cells were characterized in 10 and 14 month-old mice. A single-cell suspension was obtained from shredded prostate tissues by using collagenase/hyaluronidase enzymes: inflammatory and immune infiltrating cells were identified by flow cytometry using an anti-CD45+ moAb, and further subtyped by appropriate antibodies in lymphoid (B-, T-, T-helper, T-suppressor lymphocytes and dendritic cells) and in myeloid (macrophages and neutrophils) cells. ? Results and discussion We analyzed 28 ten-month-old mice (>=6 for genotype) and 61 fourteen-month-old mice (>=13 for genotype). We found no differences in the frequency of prostate lymphoid infiltrating-cells at any age. In contrast, at any ages we found an increase of neutrophils in Pten-deleted mice, increase that was particularly high and significant in ETV4-Pten+/- mice. Furthermore, we investigated pro-inflammatory (M1) and anti-inflammatory (M2) activated macrophages. We found a higher percentage of M2 macrophages in both Pten+/- and ETV4-Pten+/- compared to WT and ETV4 mice. ? Conclusion The high frequency of anti-inflammatory activated macrophages (M2) in mice with Pten deletion suggests a role of Pten in macrophage regulation. The particularly high increase of neutrophils in mice with both ETV4 overexpression and Pten deletion (ETV4-Pten+/- mice) developing early PC, is in keeping with the high neutrophil/lymphocyte ratio found associated with poor prognosis in several cancers. The direct or indirect role of these genetic alterations in the increase of neutrophils needs to be investigated.I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.
