Biological and clinical impact of imbalanced progesterone receptor isoform ratios in breast cancer

Lamb, Caroline A.; Fabris, Victoria; Jacobsen, Britta M.; Molinolo, Alfredo A.; Lanari, Claudia

doi:10.1530/erc-18-0179

Cited by 24 publications

(17 citation statements)

References 131 publications

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“…Both ER and PR expression varies widely in luminal breast cancer. LOH of the PGR gene locus occurs with high frequency in breast cancer, as does loss of ER (23). Thus, while approximately 70% of newly diagnosed luminal type breast tumors are ER+/PR+, about 40% and 25% of these tumors exhibit loss of heterozygosity (LOH) at either the PGR or ESR1 gene locus, respectively (5); ER and PR LOH are positively correlated.…”

Section: Pr Mutationsmentioning

confidence: 99%

Progesterone and Breast Cancer: an NCI Workshop Report

Sathyamoorthy

Lange

2020

HORM CANC

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Section: Pr Mutationsmentioning

confidence: 99%

Progesterone and Breast Cancer: an NCI Workshop Report

Sathyamoorthy

Lange

2020

HORM CANC

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“…In this region, it has acted as AF2; mediates transcriptional activation [20]. AF-2 is needed for recruitment of hormonedependent, dimerized coactivators and interactions with companion proteins in an inactive state then transcription modulation and proliferation of breast cancer cells are disrupted [21] [22]. Additionally, all bonds that occur are not on the binding site PR-Progesterone ARG766 [23].…”

Section: Methodsmentioning

confidence: 99%

Virtual Inhibition Analysis of Bioactive Compound Brazilin (Caesalpinia sappan L.) Toward Progesterone Receptor or Lonaprisan in Breast Cancer Proliferation

Harnis

Hasan²,

Janah³

et al. 2020

Biotropika

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Breast cancer is one of the leading causes of death worldwide. The pathway of breast cancer in KEGG shows that the most effective pathway is through the progesterone receptor (PR). Brazilin is a bioactive compound of secang (Caesalpinia sappan L.) used to inhibit breast cancer through survivin and Bcl-2 pathway but the interaction with PR route is unknown. This research was conducted to determine the virtual interaction between brazilin and PR and its comparison with lonaprisan, so the potential of breast cancer drugs that can overcome through three targets at once with minimal side effects is expected to be known. There are five docking interactions, including the interaction of PRprogesterone, PR-brazilin, PR-brazilin-progesterone, PR-lonaprisan, and PRlonaprisan-progesterone. Protein and ligand preparation was performed by using Discovery Studio Client 2019 and PyRx 0.8, molecular docking was performed by using Hex 8.0.0 and visualization used Discovery Studio Client 2019. Virtual interaction results shows that lonaprisan has the most stable bond (lowest binding energy),-333.8kJ/mol but when progesterone was docked afterwards the result shows the opposite. Brazilin has a more stable bond compared to lonaprisan with a difference of 2.1kJ/mol and supported by hydrophobic bonds also capable of changing the position of progesterone in binding to PR so that it is estimated that brazilin has the potential as SPRMs, an alternative breast cancer drug to replace lonaprisan. Herbal medicine with brazilin can be estimated to fight breast cancer through 3 targets at once (survivin, Bcl-2, PR).

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“…These are transcribed from the same gene by two distinct promoters, resulting in different transcriptional and functional activities (146). The level and ratio of PR-A and PR-B in reproductive tissues vary based on developmental stage and hormonal status (147,148). In normal breast cells, the isoforms are coexpressed at similar levels, but in breast cancer cells, the ratio is disrupted, with PR-A being overexpressed (35,149).…”

Section: Regulatory Network Of the Progesterone Axis In Cscsmentioning

confidence: 99%

Involvement of the Estrogen and Progesterone Axis in Cancer Stemness: Elucidating Molecular Mechanisms and Clinical Significance

Chen

et al. 2020

Front. Oncol.

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Estrogen and progesterone regulate the growth and development of human tissues, including the reproductive system and breasts, through estrogen and progesterone receptors, respectively. These receptors are also important indicators for the clinical prognosis of breast cancer and various reproductive cancers. Many studies have reported that cancer stem cells (CSCs) play a key role in tumor initiation, progression, metastasis, and recurrence. Although the role of estrogen and progesterone in human organs and various cancers has been studied, the molecular mechanisms underlying the action of these hormones on CSCs remain unclear. Therefore, further elucidation of the effects of estrogen and progesterone on CSCs should provide a new direction for developing pertinent therapies. In this review, we summarize the current knowledge on the estrogen and progesterone axis involved in cancer stemness and discuss potential therapeutic strategies to inhibit CSCs by targeting relevant pathways.

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Biological and clinical impact of imbalanced progesterone receptor isoform ratios in breast cancer

Cited by 24 publications

References 131 publications

Progesterone and Breast Cancer: an NCI Workshop Report

Progesterone and Breast Cancer: an NCI Workshop Report

Virtual Inhibition Analysis of Bioactive Compound Brazilin (Caesalpinia sappan L.) Toward Progesterone Receptor or Lonaprisan in Breast Cancer Proliferation

Involvement of the Estrogen and Progesterone Axis in Cancer Stemness: Elucidating Molecular Mechanisms and Clinical Significance

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