microRNAs in the Antitumor Immune Response and in Bone Metastasis of Breast Cancer: From Biological Mechanisms to Therapeutics

Maroni, Paola; Banfi, Giuseppe; Lombardi, Giovanni

doi:10.3390/ijms21082805

Cited by 18 publications

(16 citation statements)

References 156 publications

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“…Our results suggest that cell-free miR200b and miR200c might be possible players of this process in ovarian cancer due to their supposed delivery to neighboring cells. It is interesting to mention that these miRNAs were able to affect the phenotype of several cell types in previous studies that favored tumor growth as well as cancer immune escape [ 67 , 68 , 69 , 70 ]. It is important to note that the presence of cell lysis or apoptosis was ruled out during the tested conditions, which suggests the active secretion of these miRNAs to the extracellular environment, a process which was also suggested by others [ 71 ].…”

Section: Discussionmentioning

confidence: 99%

The Cell-Free Expression of MiR200 Family Members Correlates with Estrogen Sensitivity in Human Epithelial Ovarian Cells

Márton

Varga

Széles

et al. 2020

IJMS

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Exposure to physiological estrogens or xenoestrogens (e.g., zearalenone or bisphenol A) increases the risk for cancer. However, little information is available on their significance in ovarian cancer. We present a comprehensive study on the effect of estradiol, zearalenone and bisphenol A on the phenotype, mRNA, intracellular and cell-free miRNA expression of human epithelial ovarian cell lines. Estrogens induced a comparable effect on the rate of cell proliferation and migration as well as on the expression of estrogen-responsive genes (GREB1, CA12, DEPTOR, RBBP8) in the estrogen receptor α (ERα)-expressing PEO1 cell line, which was not observable in the absence of this receptor (in A2780 cells). The basal intracellular and cell-free expression of miR200s and miR203a was higher in PEO1, which was accompanied with low ZEB1 and high E-cadherin expression. These miRNAs showed a rapid but intermittent upregulation in response to estrogens that was diminished by an ERα-specific antagonist. The role of ERα in the regulation of the MIR200B-MIR200A-MIR429 locus was further supported by publicly available ChIP-seq data. MiRNA expression of cell lysates correlated well with cell-free miRNA expression. We conclude that cell-free miR200s might be promising biomarkers to assess estrogen sensitivity of ovarian cells.

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Section: Discussionmentioning

confidence: 99%

The Cell-Free Expression of MiR200 Family Members Correlates with Estrogen Sensitivity in Human Epithelial Ovarian Cells

Márton

Varga

Széles

et al. 2020

IJMS

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“…We have also discussed the way that miRNA modulates immunogenic cells in the microenvironment of tumours. Therefore, miRNA emerges as a potential future therapeutic tool against cancer treatment [ 187 ]. Currently, two broad categories of microRNA, i.e., miRNA mimics and miRNA inhibitory therapy, are being explored to determine their role as an immunotherapeutic agent in managing and treating cancer.…”

Section: Effect Of Mirnas On Cancer Immunotherapymentioning

confidence: 99%

miRNAs in the Regulation of Cancer Immune Response: Effect of miRNAs on Cancer Immunotherapy

Pottoo

Iqubal

et al. 2021

Cancers

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In the last few decades, carcinogenesis has been extensively explored and substantial research has identified immunogenic involvement in various types of cancers. As a result, immune checkpoint blockers and other immune-based therapies were developed as novel immunotherapeutic strategies. However, despite being a promising therapeutic option, immunotherapy has significant constraints such as a high cost of treatment, unpredictable toxicity, and clinical outcomes. miRNAs are non-coding, small RNAs actively involved in modulating the immune system’s multiple signalling pathways by binding to the 3′-UTR of target genes. miRNAs possess a unique advantage in modulating multiple targets of either the same or different signalling pathways. Therefore, miRNA follows a ‘one drug multiple target’ hypothesis. Attempts are made to explore the therapeutic promise of miRNAs in cancer so that it can be transported from bench to bedside for successful immunotherapeutic results. Therefore, in the current manuscript, we discussed, in detail, the mechanism and role of miRNAs in different types of cancers relating to the immune system, its diagnostic and therapeutic aspect, the effect on immune escape, immune-checkpoint molecules, and the tumour microenvironment. We have also discussed the existing limitations, clinical success and the prospective use of miRNAs in cancer.

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“…Cancer cells with malignant potential develop various strategies to reach secondary growth sites: they escape immunosurveillance [ 5 , 6 ], degrade the basement membrane and the extra cellular matrix (ECM), invade the surrounding microenvironment (local invasion), and enter the bloodstream and/or the lymphatic system, ultimately reaching sites where they will give rise to metastatic growth [ 3 , 7 , 8 ]. Bone metastasis differs in aspect depending on the interactions between the cancer cells and the complex tissue microenvironment.…”

Section: Bone Metastasis From Breast and Prostate Carcinomas: Ostementioning

confidence: 99%

Bone, a Secondary Growth Site of Breast and Prostate Carcinomas: Role of Osteocytes

Maroni

Bendinelli

2020

Cancers

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Bone is the primarily preferred site for breast and prostate cancer to metastasize. Bone metastases are responsible for most deaths related to breast and prostate cancer. The bone’s particular microenvironment makes it conducive for the growth of cancer cells. Studies on bone metastasis have focused on the interaction between cancer cells and the bone microenvironment. Osteocytes, the most common cell type of bone tissue, have received little attention in bone metastasis, although they are master signal sensors, integrators, and skeleton transducers. They play an important role in regulating bone mass by acting on both osteoblasts and osteoclasts, through the release of proteins such as sclerostin, Dickkopf-1 (DKK-1), and fibroblast growth factor 23 (FGF23). Osteocytes have been extensively re-evaluated, in light of their multiple functions: with different experimental approaches, it has been shown that, indeed, osteocytes are actively involved in the colonization of bone tissue by cancer cells. The present review focuses on recent research on the role that osteocytes play in bone metastasis of breast and prostate cancers. Moreover, the studies here summarized open up perspectives for new therapeutic approaches focused on modulating the activity of osteocytes to improve the condition of the bone metastatic patients. A better understanding of the complex interactions between cancer cells and bone-resident cells is indispensable for identifying potential therapeutic targets to stop tumor progression and prevent bone metastases.

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microRNAs in the Antitumor Immune Response and in Bone Metastasis of Breast Cancer: From Biological Mechanisms to Therapeutics

Cited by 18 publications

References 156 publications

The Cell-Free Expression of MiR200 Family Members Correlates with Estrogen Sensitivity in Human Epithelial Ovarian Cells

The Cell-Free Expression of MiR200 Family Members Correlates with Estrogen Sensitivity in Human Epithelial Ovarian Cells

miRNAs in the Regulation of Cancer Immune Response: Effect of miRNAs on Cancer Immunotherapy

Bone, a Secondary Growth Site of Breast and Prostate Carcinomas: Role of Osteocytes

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