Estrogen Receptor-β Up-Regulates IGF1R Expression and Activity to Inhibit Apoptosis and Increase Growth of Medulloblastoma

Cookman, Clifford J.; Belcher, Scott M.

doi:10.1210/en.2015-1141

Cited by 27 publications

(25 citation statements)

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“…Considering the progressive nature of MB development in Ptch1 +/- , the apparent increased sensitivity of females to dysregulated SHH signaling could be related to the increased levels of circulating estrogens in mature females. These activities of estrogen are mediated through modulation of rapid estrogen signaling, estrogen receptor-regulated gene expression, and resulting modulation of growth factor-related signal transduction pathways (Cookman and Belcher, 2015; Garcia-Segura et al, 2006). Increased activation of ERβ signaling increases GCP mitogenesis and migration, and upregulates neuroprotective mechanisms in mature granule cells, which also act in the etiology and progression of MB to drive tumor progression (Belcher, 2008; Cookman and Belcher, 2015; Guillette et al, 2018).…”

Section: Discussionmentioning

confidence: 99%

“…These activities of estrogen are mediated through modulation of rapid estrogen signaling, estrogen receptor-regulated gene expression, and resulting modulation of growth factor-related signal transduction pathways (Cookman and Belcher, 2015; Garcia-Segura et al, 2006). Increased activation of ERβ signaling increases GCP mitogenesis and migration, and upregulates neuroprotective mechanisms in mature granule cells, which also act in the etiology and progression of MB to drive tumor progression (Belcher, 2008; Cookman and Belcher, 2015; Guillette et al, 2018). It is possible that the more sever phenotypes detected in Ptch1 +/- female mice are related to a relative increase in estrogen signaling in ERβ positive Ptch1 +/- granule cell-like precursors.…”

Section: Discussionmentioning

confidence: 99%

“…Estrogen receptor β (ERβ) is expressed in maturing GCPs and MB tumor cells and can modify MB growth and progression (Belcher, 2008; Jakab et al, 2001). Increased estrogen receptor signaling during cerebellar development and MB progression results in upregulation of cytoprotective ERβ-dependent insulin-like growth factor signaling that impacts GCP maturation and migration, and can increase MB tumor growth rate (Belcher, 2008; Cookman and Belcher, 2015).…”

Section: Introductionmentioning

confidence: 99%

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Heterozygous mutation of Sonic Hedgehog receptor (Ptch) drives cerebellar overgrowth and sex-specifically alters hippocampal and cortical layer structure, activity, and social behavior in female mice

Jackson

Bendfeldt

Beam

et al. 2020

Preprint

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Sonic hedgehog (SHH) signaling is essential for the differentiation and migration of early stem cell populations during cerebellar development. Dysregulation of SHH-signaling can result in cerebellar overgrowth and the formation of the brain tumor medulloblastoma. Treatment for medulloblastoma is extremely aggressive and patients suffer life-long side effects including behavioral deficits. Considering that other behavioral disorders including autism spectrum disorders, holoprosencephaly, and basal cell nevus syndrome are known to present with cerebellar abnormalities, it is proposed that some behavioral abnormalities could be inherent to the medulloblastoma sequalae rather than treatment. Using a haploinsufficient SHH receptor knockout mouse model (Ptch1+/-), a partner preference task was used to explore activity, social behavior and neuroanatomical changes resulting from dysregulated SHH signaling. Compared to wild-type, Ptch1+/- females displayed increased activity by traveling a greater distance in both open-field and partner preference tasks. Social behavior was also sex-specifically modified in Ptch1+/- females that interacted more with both novel and familiar animals in the partner preference task compared to same-sex wild-type controls. Haploinsufficency of PTCH resulted in cerebellar overgrowth in lobules IV/V and IX of both sexes, and female-specific decreases in hippocampal size and isocortical layer thickness. Taken together, neuroanatomical changes related to deficient SHH signaling may alter social behavior.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Heterozygous mutation of Sonic Hedgehog receptor (Ptch) drives cerebellar overgrowth and sex-specifically alters hippocampal and cortical layer structure, activity, and social behavior in female mice

Jackson

Bendfeldt

Beam

et al. 2020

Preprint

Self Cite

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“…Estrogen receptors play an important role in the regulation of numerous metabolic and proliferative processes, including tumorigenesis, preferentially through interaction with specifi c response element in the target genes (Mueller et al 2000;Cookman and Belcher 2015;Lau and To 2016;Ur Rahman and Cao 2016;Wesolowska et al 2016;Zhu et al 2016). Estrogen receptors are responsible for the regulation of cell growth and apoptosis as well as are involved, at least partly, in the development, proliferation, and progression of some cancers.…”

mentioning

confidence: 99%

“…At the same time, Li et al (2013) have shown that in U87 cells estrogen receptors inhibit the cell proliferation and reduced cells in the S+G2/M phase and that hypoxia induced estrogen receptor-β5 expression in glioma as a self-protective mechanism against tumor proliferation. Recently, Cookman and Belcher (2015) have demonstrated that estrogen promotes medulloblastoma growth through estrogen receptor-β-mediated increases in IGF1R expression and activity, which induce cytoprotective mechanisms that decrease apoptosis.…”

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confidence: 99%

Hypoxic regulation of the expression of genes encoded estrogen related proteins in U87 glioma cells: eff ect of IRE1 inhibition

et al. 2017

Endocrine Regulations

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Objective. Th e aim of the present study was to examine the eff ect of inhibition of endoplasmic reticulum stress signaling, mediated by IRE1 (inositol requiring enzyme 1), which is a central mediator of the unfolded protein response on the expression of genes encoded estrogen related proteins (NRIP1/RIP140, TRIM16/EBBP, ESRRA/NR3B1, FAM162A/E2IG5, PGRMC2/PMBP, and SLC39A6/LIV-1) and their hypoxic regulation in U87 glioma cells for evaluation of their possible signifi cance in the control of glioma cells proliferation.Methods. Th e expression of NRIP1, EBBP, ESRRA, E2IG5, PGRMC2, and SLC39A6 genes in U87 glioma cells, transfected by empty vector pcDNA3.1 (control) and cells without IRE1 signaling enzyme function (transfected by dnIRE1) upon hypoxia, was studied by a quantitative polymerase chain reaction.Results. Inhibition of both enzymatic activities (kinase and endoribonuclease) of IRE1 signaling enzyme function up-regulates the expression of EBBP, E2IG5, PGRMC2, and SLC39A6 genes is in U87 glioma cells in comparison with the control glioma cells, with more signifi cant changes for E2IG5 and PGRMC2 genes. At the same time, the expression of NRIP1 and ESRRA genes is strongly down-regulated in glioma cells upon inhibition of IRE1. We also showed that hypoxia increases the expression of E2IG5, PGRMC2, and EBBP genes and decreases NRIP1 and ESRRA genes expression in control glioma cells. Furthermore, the inhibition of IRE1 in U87 glioma cells decreases the eff ect of hypoxia on the expression of E2IG5 and PGRMC2 genes, eliminates hypoxic regulation of NRIP1 gene, and enhances the sensitivity of ESRRA gene to hypoxic condition. Furthermore, the expression of SLC39A6 gene is resistant to hypoxia in both the glioma cells with and without IRE1 signaling enzyme function. Conclusions.Results of this investigation demonstrate that inhibition of IRE1 signaling enzyme function aff ects the expression of NRIP1, EBBP, ESRRA, E2IG5, PGRMC2, and SLC39A6 genes in U87 glioma cells in gene specifi c manner and these changes possibly contribute to the suppression of the cell proliferation. Most of these genes are regulated by hypoxia and preferentially through IRE1 signaling pathway of endoplasmic reticulum stress.

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The pivotal role of irradiation‐induced apoptosis in the pathogenesis and therapy of medulloblastoma

Richard

2024

Cancer Reports

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BackgroundMedulloblastoma (MB) is a rare primitive neuroectodermal tumors originating from the cerebellum. MB is the most common malignant primary brain tumor of childhood. MB originates from neural precursor cells in distinctive regions of the rhombic lip, and their maturation occurs in the cerebellum or the brain stem during embryonal development. Also, apoptosis is a programmed cell death associated with numerous physiological as well as pathological regulations.Recent FindingsIrradiation (IR)‐induce apoptosis triggers cell death, with or without intervening mitosis within a few hours of IR and these share different morphologic alteration such as, loss of normal nuclear structure as well as degradation of DNA. Moreover, MB is strikingly sensitive to DNA‐damaging therapies and the role of apoptosis a key treatment modality. Furthermore, in MB, the apoptotic pathways are made up of several triggers, modulators, as well as effectors. Notably, IR‐induced apoptotic mechanisms in MB therapy are very complex and they either induce radiosensitivity or inhibit radioresistance leading to potential effective treatment strategies for MB.ConclusionThis review explicitly explores the pivotal roles of IR‐induced apoptosis in the pathogenesis and therapy of MB.

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Estrogen Receptor-β Up-Regulates IGF1R Expression and Activity to Inhibit Apoptosis and Increase Growth of Medulloblastoma

Cited by 27 publications

References 65 publications

Heterozygous mutation of Sonic Hedgehog receptor (Ptch) drives cerebellar overgrowth and sex-specifically alters hippocampal and cortical layer structure, activity, and social behavior in female mice

Heterozygous mutation of Sonic Hedgehog receptor (Ptch) drives cerebellar overgrowth and sex-specifically alters hippocampal and cortical layer structure, activity, and social behavior in female mice

Hypoxic regulation of the expression of genes encoded estrogen related proteins in U87 glioma cells: eff ect of IRE1 inhibition

The pivotal role of irradiation‐induced apoptosis in the pathogenesis and therapy of medulloblastoma

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