Relationship of micro-RNA, mRNA and eIF Expression in Tamoxifen-Adapted MCF-7 Breast Cancer Cells: Impact of miR-1972 on Gene Expression, Proliferation and Migration

Behringer, Akhil; Stoimenovski, Darko; Porsch, Martin; Hoffmann, Katrin; Behre, Gerhard; Große, Ivo; Kalinski, Thomas; Haybaeck, Johannes; Naß, Norbert

doi:10.3390/biom12070916

Cited by 5 publications

(6 citation statements)

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“…Several deregulated genes identified by these means have been shown to have an impact on the prognosis of breast cancer patients. We have reported on gene expression changes in such a cellular model, focusing on lncRNAs [ 10 ], and extended this investigation on microRNAs and eukaryotic initiation factors [ 39 ]. We report herein on further studies on LINC00992, a long non-coding RNA that is down-regulated is response to long-term exposure of MCF-7 cells to low doses of 4OH-tamoxifen (10 nM) [ 10 ].…”

Section: Discussionmentioning

confidence: 99%

The tamoxifen-regulated, long non-coding RNA LINC00992 affects proliferation, migration, and expression of tamoxifen resistanceassociated genes in MCF-7 breast cancer cells

Gräf¹,

Haybaeck²,

Behre³

et al. 2022

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Introduction Tamoxifen-adapted MCF-7 breast cancer cells (MCF-7-TAM-R) are a model for acquired tamoxifen resistance in oestrogen receptor-positive breast cancer. In this system, the expression of long-non-coding RNA LINC00992 is decreased. LINC00992 might therefore contribute to tamoxifen adaption and associated gene expres-sion changes. Here, we investigated whether a modulation of LINC00992 modifies gene expression, proliferation, and migration. Material and methods Up- and down-- regulation of LINC00992 was performed using plasmid vectors and siRNA. Gene expression was measured via nCounter® and quantitative real-time polymerase chain reaction. Database analysis was performed using GEPIA2 and cBioportal. Furthermore, we performed scratch assays, colony-forming assays, and proliferation assays with MCF-7 and MCF-7-TAM-R after up-regulation of LINC00992. Results Up- and down-regulation of LINC00992 caused gene expression changes in 4 of the 42 tamoxifen-regulated genes tested. Especially ubiquitin D, single-minded homologue 1 (SIM1) carcinoembryonic antigen-related cell adhesion molecule 5 and the G-protein coupled oestrogen receptor 1 were affected. In tamoxifen-adapted MCF-7-TAM-R cells, LINC00992 overexpression resulted in augmented viability and proliferation and enhanced migration. Database analyses revealed that luminal breast cancers have increased expression of LINC00992 compared to Her2-type/neu- or basal type. Furthermore, higher expression of LINC00992 was associated with poor prognosis in luminal-A carcinomas. Conclusions Changes in the expression of tamoxifen-regulated genes could be induced by manipulating LINC00992’s abundance, suggesting that it is at least partially involved in the establishment of the tamoxifen-induced gene expression pattern. LINC00992 may also serve as a prognostic biomarker and may indicate the development of tamoxifen resistance.

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Section: Discussionmentioning

confidence: 99%

The tamoxifen-regulated, long non-coding RNA LINC00992 affects proliferation, migration, and expression of tamoxifen resistanceassociated genes in MCF-7 breast cancer cells

Gräf¹,

Haybaeck²,

Behre³

et al. 2022

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“…The cell growth inhibition rate, IC 50 , and reversal fold (RF) after combination drug treatment were calculated. 21 = RF IC IC 50 50 drug combination drug alone (4) where IC 50drug alone is the cell median inhibition rate of TAM on MCF-7/TAM cells, IC 50drug combination is the cell median inhibition rate of TAM-API combination treatment with nontoxic concentrations of IMP-RH60/mPEG−PLLA on MCF-7/TAM cells.…”

Section: Pharmacokinetic Studymentioning

confidence: 99%

Imperatorin-Loaded RH60/mPEG–PLLA Micelles for Reversing Tamoxifen Resistance in Breast Cancer

Li,

Zhao,

et al. 2024

ACS Appl. Nano Mater.

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Imperatorin (IMP) has demonstrated potential in reversing drug resistance in various tumor cells; however, its limited clinical application and development are attributed to its poor water solubility and low bioavailability. The current work is intended to enhance the oral bioavailability of IMP and its efficacy in overcoming tamoxifen (TAM) resistance in breast cancer cells. We employed mPEG−PLLA and Cremophor RH60 (RH60) to prepare imperatorin nanomicelles (IMP-RH60/mPEG−PLLA). The freeze-dried powder of IMP-RH60/mPEG−PLLA demonstrated a porous structure, and upon reconstitution, the resulting solution exhibited clarity and transparency. The particle size was measured to be 25.48 ± 0.92 nm, with a zeta potential of −5.50 ± 1.06 mV. The encapsulation efficiency was determined to be 85.78 ± 0.84%, while the drug loading was found to be 2.66 ± 0.03%. In comparison to the active pharmaceutical ingredients (APIs) of IMP, IMP-RH60/mPEG−PLLA exhibited a significant increase in in vitro release, improved bioavailability in rats, and enhanced uptake by MCF-7/TAM cells. The coadministration of IMP-RH60/mPEG−PLLA and TAM effectively inhibited the proliferation, colony formation, migration, and invasion of MCF-7/TAM cells. This outcome could potentially be attributed to the downregulation of GST-π and MDR1 drug resistance genes, consequently augmenting the susceptibility of MCF-7/TAM cells to TAM. An experimental model of BALB/c nude xenograft, consisting of human breast cancer cells resistant to tamoxifen (TAM), was established in order to assess the potential in vivo reversal of TAM resistance through the use of IMP-RH60/mPEG−PLLA. The growth of xenografts was inhibited by IMP-RH60/mPEG−PLLA, and it induced apoptosis in tumor tissues through the downregulation of K i -67, GST-π, and MDR1 gene expression. The findings indicated that the utilization of IMP-RH60/mPEG− PLLA micelles resulted in an enhancement of IMP's bioavailability and its efficacy in overcoming TAM resistance.

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“…4,9,21,44 Despite this established ER receptor actions, we acknowledged that ET resistance is multifactorial and we cannot exclude several other non-estrogen related pathways in several studies using tamoxifen and fulvestrant adapted cell lines. [51][52][53][54] Progesterone and progesterone receptor Progesterone is a steroid hormone produced by the corpus luteum in the human ovarium, which its primary duty is to prepare the female body for gestation. Breast epithelial cells are indispensable in affecting duct-alveolar changes in phases such as puberty, the luteal phase (pre-menstrual period), pregnancy, and lactation.…”

Section: Estrogen and Estrogen Receptormentioning

confidence: 99%

“…Distinguished studies also showed us that numerous studies of non-coding RNA especially miRNA play important roles in ET resistance, such as miRNA such as miRNA-1972, miRNA-375 and miRNA-221. 52,88 However there are still no clear depiction of p53 roles in ET resistance caused by miRNA involvement. It is due to the complexity of the network of both parties, in which miRNA could regulate p53 level and function and vice versa mutated p53 could regulate the miRNA expression and modulate miRNA biology activities due to its gain-of-function properties.…”

Section: Estrogen and Estrogen Receptormentioning

confidence: 99%

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p53 Mutation as Plausible Predictor for Endocrine Resistance Therapy in Luminal Breast Cancer

et al. 2022

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Endocrine therapy resistance in Luminal Breast Cancer is a significant issue to be tackled, but currently, no specific biomarker could be used to anticipate this event. p53 mutation is widely known as one of Breast Cancer’s most prominent genetic alterations. Its mutation could generate various effects in Estrogen Receptor and Progesterone Receptor molecular works, tangled in events leading to the aggravation of endocrine therapy resistance. Hence the possibility of p53 mutation utilization as an endocrine therapy resistance predictive biomarker is plausible. The purpose of this review is to explore the latest knowledge of p53 role in Estrogen Receptor and Progesterone Receptor molecular actions, thus aggravating the Endocrine Therapy resistance in Luminal Breast Cancer, from which we could define possibilities and limitations to utilize p53 as the predictive biomarker of endocrine therapy resistance in Luminal Breast Cancer.

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Relationship of micro-RNA, mRNA and eIF Expression in Tamoxifen-Adapted MCF-7 Breast Cancer Cells: Impact of miR-1972 on Gene Expression, Proliferation and Migration

Cited by 5 publications

References 76 publications

The tamoxifen-regulated, long non-coding RNA LINC00992 affects proliferation, migration, and expression of tamoxifen resistanceassociated genes in MCF-7 breast cancer cells

The tamoxifen-regulated, long non-coding RNA LINC00992 affects proliferation, migration, and expression of tamoxifen resistanceassociated genes in MCF-7 breast cancer cells

Imperatorin-Loaded RH60/mPEG–PLLA Micelles for Reversing Tamoxifen Resistance in Breast Cancer

p53 Mutation as Plausible Predictor for Endocrine Resistance Therapy in Luminal Breast Cancer

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