Your search keyword '"ESTROGEN receptors"' showing total 139 results

1. Estrogen and its receptors in adipose tissue from women and men : Associations with age, adiposity and type 2 diabetes

Author

Ahmed, Fozia and Ahmed, Fozia

Abstract

Obesity and its complications, such as insulin resistance and type 2 diabetes (T2D), are leading causes of morbidity and mortality globally. Adipose tissue is important for whole-body homeostasis, functioning as an energy storage reservoir and an endocrine organ. Estrogens mediate their effects through estrogen receptor alpha (ESR1) and beta (ESR2) and contribute to sex and menopause-related differences in body fat distribution. Moreover, estrogens can be produced from androgens in the adipose tissue by the enzyme aromatase. The overall aim of this thesis was to investigate the role of estrogen and estrogen signalling in human adipose tissue and their association with age, adiposity, and insulin resistance. In Paper I, we assessed ESR1 and ESR2 gene expression in subcutaneous adipose tissue (SAT) from pre- and postmenopausal women, and investigated the effects of estradiol on adipocyte glucose uptake. We found that ESR2 gene expression was higher in postmenopausal women than premenopausal women. Moreover, in late, but not pre- or early postmenopausal women, estradiol incubation reduced basal and insulin-stimulated glucose uptake, which corresponded to an increase in ESR2 gene expression levels. The inhibiting effect of estradiol on adipocyte glucose uptake was prevented using an ESR2 antagonist. Subsequently, in Paper II we assessed the role of ESR2 in SAT lipid and glucose metabolism and preadipocyte differentiation. ESR2 expression in SAT was inversely correlated with markers of central adiposity and positively correlated with markers of lipid accumulation. Moreover, ESR2 knockdown impaired subcutaneous preadipocyte differentiation and glucose utilization. In Paper III, we focused on adipocyte lipolysis in women, which is regulated, in part, by catecholamines. OCT3, which mediates catecholamine transport into adipocytes, where they can be degraded, was increased in SAT with age, and higher in postmenopausal women than premenopausal women. Moreover, its expressi

Published

2024

2. Estrogen and its receptors in adipose tissue from women and men : Associations with age, adiposity and type 2 diabetes

Author

Ahmed, Fozia and Ahmed, Fozia

Abstract

Obesity and its complications, such as insulin resistance and type 2 diabetes (T2D), are leading causes of morbidity and mortality globally. Adipose tissue is important for whole-body homeostasis, functioning as an energy storage reservoir and an endocrine organ. Estrogens mediate their effects through estrogen receptor alpha (ESR1) and beta (ESR2) and contribute to sex and menopause-related differences in body fat distribution. Moreover, estrogens can be produced from androgens in the adipose tissue by the enzyme aromatase. The overall aim of this thesis was to investigate the role of estrogen and estrogen signalling in human adipose tissue and their association with age, adiposity, and insulin resistance. In Paper I, we assessed ESR1 and ESR2 gene expression in subcutaneous adipose tissue (SAT) from pre- and postmenopausal women, and investigated the effects of estradiol on adipocyte glucose uptake. We found that ESR2 gene expression was higher in postmenopausal women than premenopausal women. Moreover, in late, but not pre- or early postmenopausal women, estradiol incubation reduced basal and insulin-stimulated glucose uptake, which corresponded to an increase in ESR2 gene expression levels. The inhibiting effect of estradiol on adipocyte glucose uptake was prevented using an ESR2 antagonist. Subsequently, in Paper II we assessed the role of ESR2 in SAT lipid and glucose metabolism and preadipocyte differentiation. ESR2 expression in SAT was inversely correlated with markers of central adiposity and positively correlated with markers of lipid accumulation. Moreover, ESR2 knockdown impaired subcutaneous preadipocyte differentiation and glucose utilization. In Paper III, we focused on adipocyte lipolysis in women, which is regulated, in part, by catecholamines. OCT3, which mediates catecholamine transport into adipocytes, where they can be degraded, was increased in SAT with age, and higher in postmenopausal women than premenopausal women. Moreover, its expressi

Published

2024

3. Gestational-onset Hypothyroidism Affects Genes Controlling Epididymal Sperm Maturation in F1 Progeny Rats

Author

Balaji, Sadhasivam, Shobana, Navaneethabalakrishnan, Kumar Navin, Ajit, Anbalagan, Jaganathan, Ravi Sankar, Bhaskaran, Ilangovan, Ramachandran, Michael Aruldhas, Mariajoseph, Balaji, Sadhasivam, Shobana, Navaneethabalakrishnan, Kumar Navin, Ajit, Anbalagan, Jaganathan, Ravi Sankar, Bhaskaran, Ilangovan, Ramachandran, and Michael Aruldhas, Mariajoseph

Abstract

Purpose: Hypothyroidism is associated with infertility. We have reported that gestational-onset hypothyroidism impairs post-testicular sperm maturation in F1 progeny rats, whereas the underlying mechanism remains obscure. In this study, we tested the hypothesis “transient gestational-onset hypothyroidism affects post-testicular sperm maturation by inducing oxidative stress and modifying the expression of specific genes controlling epididymal function in F1 progeny rats”. Methods: Hypothyroidism was induced by providing 0.05% methimazole in drinking water to pregnant rats during specific periods of foetal differentiation of testis and epididymis. On the postnatal day 120, epididymes were dissected out and used for various analyses. Sperm parameters and activities of antioxidants and pro-oxidants were assayed using standard protocols. qRT-PCR and western blot were carried out to assess the expression of epididymal functional genes and their respective proteins. Results: Gestational-onset hypothyroidism produced decrease of sperm motility and membrane integrity, and increase of abnormal sperm morphologies. While the concentration of reduced glutathione and specific activities of antioxidant enzymes superoxide dismutase, catalase and glutathione peroxidase decreased, levels of pro-oxidants hydrogen peroxide and lipid peroxidation increased. Expression levels of androgen and thyroid hormone receptors ?/?, aquaporin 9, and glutathione peroxidise 5 decreased, whereas estrogen receptors ?/? increased in rats with gestational-onset hypothyroidism. Conclusion: Our results support our hypothesis and we conclude that gestationalonset hypothyroidism impairs post-testicular sperm maturation due to oxidative stress and modified expression of nuclear hormone receptors and aquaporin 9 in the epididymis of F1 progeny.

Published

2022

4. Gestational-onset Hypothyroidism Affects Genes Controlling Epididymal Sperm Maturation in F1 Progeny Rats

Author

Balaji, Sadhasivam, Shobana, Navaneethabalakrishnan, Kumar Navin, Ajit, Anbalagan, Jaganathan, Ravi Sankar, Bhaskaran, Ilangovan, Ramachandran, Michael Aruldhas, Mariajoseph, Balaji, Sadhasivam, Shobana, Navaneethabalakrishnan, Kumar Navin, Ajit, Anbalagan, Jaganathan, Ravi Sankar, Bhaskaran, Ilangovan, Ramachandran, and Michael Aruldhas, Mariajoseph

Abstract

Purpose: Hypothyroidism is associated with infertility. We have reported that gestational-onset hypothyroidism impairs post-testicular sperm maturation in F1 progeny rats, whereas the underlying mechanism remains obscure. In this study, we tested the hypothesis “transient gestational-onset hypothyroidism affects post-testicular sperm maturation by inducing oxidative stress and modifying the expression of specific genes controlling epididymal function in F1 progeny rats”. Methods: Hypothyroidism was induced by providing 0.05% methimazole in drinking water to pregnant rats during specific periods of foetal differentiation of testis and epididymis. On the postnatal day 120, epididymes were dissected out and used for various analyses. Sperm parameters and activities of antioxidants and pro-oxidants were assayed using standard protocols. qRT-PCR and western blot were carried out to assess the expression of epididymal functional genes and their respective proteins. Results: Gestational-onset hypothyroidism produced decrease of sperm motility and membrane integrity, and increase of abnormal sperm morphologies. While the concentration of reduced glutathione and specific activities of antioxidant enzymes superoxide dismutase, catalase and glutathione peroxidase decreased, levels of pro-oxidants hydrogen peroxide and lipid peroxidation increased. Expression levels of androgen and thyroid hormone receptors ?/?, aquaporin 9, and glutathione peroxidise 5 decreased, whereas estrogen receptors ?/? increased in rats with gestational-onset hypothyroidism. Conclusion: Our results support our hypothesis and we conclude that gestationalonset hypothyroidism impairs post-testicular sperm maturation due to oxidative stress and modified expression of nuclear hormone receptors and aquaporin 9 in the epididymis of F1 progeny.

Published

2022

5. Sex differences in immune response and sex hormone receptor expression in healthy individuals and during viral infection

Author

Brundin, Peik M. A. and Brundin, Peik M. A.

Abstract

There is sex-bias in morbidity and mortality from infectious diseases. Infections kill more men than women and several studies have pointed out differences in the immune system as a reason. The sex hormones estrogen, progesterone and testosterone all shape the effect of the immune response on multiple levels. Women at fertile age have been suggested to have higher proinflammatory responses from inflammatory stimuli compared to men and post-menopausal women, which has been ascribed to their higher estrogen levels. This could possibly lead to a more active pathogen response but may also result in a detrimental immunopathology to infections or development of autoimmune reaction. The overall aim of this thesis is to study the contribution of sex hormones and sex hormone receptors (SHR) to sex differences in immune response. We focus on peripheral blood mononuclear cells (PBMCs) to study such relationships in healthy individuals, as well as in individuals with asymptomatic Torque Teno Virus infection, and individuals with acute Puumala virus infection. In Paper I, we investigated expression of SHR and immune response genes in PBMC from healthy premenopausal (pre-MP) women during the menstrual cycle. The expression levels were estimated using a qPCR Array (Taqman low-density array, TLDA). SHR expression did not change significantly during the menstrual cycle, but several key immune regulatory genes were significantly more expressed during the ovulatory and mid luteal phase. Further, we separated PBMC into cell subsets (CD4+ T-cells, CD8+ T-cells, CD56+ NK-cells, CD14+ monocytes and CD19+ B-cells) and analyzed the expression through qPCR of estrogen receptors (ERs), ERα, ERβ1 (wildtype) and the isoform ERβ2. For the first time and unexpectedly, we demonstrate that the isoform ERβ2 was more abundant than wildtype ERβ1. The data from this paper provides new knowledge on the contribution of the menstrual cycle on immune response. In Paper II, we explored the use of Torque Ten

Published

2021

6. Sex differences in immune response and sex hormone receptor expression in healthy individuals and during viral infection

Author

Brundin, Peik M. A. and Brundin, Peik M. A.

Abstract

There is sex-bias in morbidity and mortality from infectious diseases. Infections kill more men than women and several studies have pointed out differences in the immune system as a reason. The sex hormones estrogen, progesterone and testosterone all shape the effect of the immune response on multiple levels. Women at fertile age have been suggested to have higher proinflammatory responses from inflammatory stimuli compared to men and post-menopausal women, which has been ascribed to their higher estrogen levels. This could possibly lead to a more active pathogen response but may also result in a detrimental immunopathology to infections or development of autoimmune reaction. The overall aim of this thesis is to study the contribution of sex hormones and sex hormone receptors (SHR) to sex differences in immune response. We focus on peripheral blood mononuclear cells (PBMCs) to study such relationships in healthy individuals, as well as in individuals with asymptomatic Torque Teno Virus infection, and individuals with acute Puumala virus infection. In Paper I, we investigated expression of SHR and immune response genes in PBMC from healthy premenopausal (pre-MP) women during the menstrual cycle. The expression levels were estimated using a qPCR Array (Taqman low-density array, TLDA). SHR expression did not change significantly during the menstrual cycle, but several key immune regulatory genes were significantly more expressed during the ovulatory and mid luteal phase. Further, we separated PBMC into cell subsets (CD4+ T-cells, CD8+ T-cells, CD56+ NK-cells, CD14+ monocytes and CD19+ B-cells) and analyzed the expression through qPCR of estrogen receptors (ERs), ERα, ERβ1 (wildtype) and the isoform ERβ2. For the first time and unexpectedly, we demonstrate that the isoform ERβ2 was more abundant than wildtype ERβ1. The data from this paper provides new knowledge on the contribution of the menstrual cycle on immune response. In Paper II, we explored the use of Torque Ten

Published

2021

7. Individual- and neighborhood-level socioeconomic status and risk of aggressive breast cancer subtypes in a pooled cohort of women from Kaiser Permanente Northern California.

Author

Aoki, Rhonda-Lee F, Aoki, Rhonda-Lee F, Uong, Stephen P, Gomez, Scarlett Lin, Alexeeff, Stacey E, Caan, Bette J, Kushi, Lawrence H, Torres, Jacqueline M, Guan, Alice, Canchola, Alison J, Morey, Brittany N, Lin, Katherine, Kroenke, Candyce H, Aoki, Rhonda-Lee F, Aoki, Rhonda-Lee F, Uong, Stephen P, Gomez, Scarlett Lin, Alexeeff, Stacey E, Caan, Bette J, Kushi, Lawrence H, Torres, Jacqueline M, Guan, Alice, Canchola, Alison J, Morey, Brittany N, Lin, Katherine, and Kroenke, Candyce H

Abstract

BackgroundLow socioeconomic status (SES) has been associated with a higher risk of aggressive breast cancer (BC) subtypes, but few studies have examined the independent effects of both neighborhood-level socioeconomic status (nSES) and individual-level SES measures.MethodsThis study included 5547 women from the Pathways and Life After Cancer Epidemiology cohorts who were diagnosed with invasive BC. Generalized estimating equation models were used to examine associations of nSES (a composite score based on income, poverty, education, occupation, employment, rent, and house value) and individual-level SES (income and education) with BC subtypes: luminal B (LumB), Her2-enriched (Her2-e), and triple-negative breast cancer (TNBC) relative to luminal A (LumA). Models controlled for age, race, nativity, stage, days from diagnosis to survey, and study cohort and simultaneously for nSES and individual-level SES.ResultsIn fully adjusted models, low nSES was significantly associated with the LumB (odds ratio for quartile 1 vs quartile 4 [ORQ1vQ4 ], 1.31; 95% confidence interval [CI], 1.11-1.54; P for trend = .005) and TNBC subtypes (ORQ1vQ4 , 1.32; 95% CI, 1.02-1.71; P for trend = .037) relative to LumA. Conversely, individual education was significantly associated with only the Her2-e subtype (odds ratio for high school degree or less vs postgraduate, 1.68; 95% CI, 1.03-2.75; P for trend = .030) relative to LumA. Individual income was not significantly associated with any BC subtype.ConclusionsnSES and individual-level SES are independently associated with different BC subtypes; specifically, low nSES and individual-level education are independent predictors of more aggressive BC subtypes relative to LumA.

Published

2021

8. Individual- and neighborhood-level socioeconomic status and risk of aggressive breast cancer subtypes in a pooled cohort of women from Kaiser Permanente Northern California.

Author

Aoki, Rhonda-Lee F, Aoki, Rhonda-Lee F, Uong, Stephen P, Gomez, Scarlett Lin, Alexeeff, Stacey E, Caan, Bette J, Kushi, Lawrence H, Torres, Jacqueline M, Guan, Alice, Canchola, Alison J, Morey, Brittany N, Lin, Katherine, Kroenke, Candyce H, Aoki, Rhonda-Lee F, Aoki, Rhonda-Lee F, Uong, Stephen P, Gomez, Scarlett Lin, Alexeeff, Stacey E, Caan, Bette J, Kushi, Lawrence H, Torres, Jacqueline M, Guan, Alice, Canchola, Alison J, Morey, Brittany N, Lin, Katherine, and Kroenke, Candyce H

Abstract

BackgroundLow socioeconomic status (SES) has been associated with a higher risk of aggressive breast cancer (BC) subtypes, but few studies have examined the independent effects of both neighborhood-level socioeconomic status (nSES) and individual-level SES measures.MethodsThis study included 5547 women from the Pathways and Life After Cancer Epidemiology cohorts who were diagnosed with invasive BC. Generalized estimating equation models were used to examine associations of nSES (a composite score based on income, poverty, education, occupation, employment, rent, and house value) and individual-level SES (income and education) with BC subtypes: luminal B (LumB), Her2-enriched (Her2-e), and triple-negative breast cancer (TNBC) relative to luminal A (LumA). Models controlled for age, race, nativity, stage, days from diagnosis to survey, and study cohort and simultaneously for nSES and individual-level SES.ResultsIn fully adjusted models, low nSES was significantly associated with the LumB (odds ratio for quartile 1 vs quartile 4 [ORQ1vQ4 ], 1.31; 95% confidence interval [CI], 1.11-1.54; P for trend = .005) and TNBC subtypes (ORQ1vQ4 , 1.32; 95% CI, 1.02-1.71; P for trend = .037) relative to LumA. Conversely, individual education was significantly associated with only the Her2-e subtype (odds ratio for high school degree or less vs postgraduate, 1.68; 95% CI, 1.03-2.75; P for trend = .030) relative to LumA. Individual income was not significantly associated with any BC subtype.ConclusionsnSES and individual-level SES are independently associated with different BC subtypes; specifically, low nSES and individual-level education are independent predictors of more aggressive BC subtypes relative to LumA.

Published

2021

9. Sex differences in immune response and sex hormone receptor expression in healthy individuals and during viral infection

Author

Brundin, Peik M. A. and Brundin, Peik M. A.

Abstract

There is sex-bias in morbidity and mortality from infectious diseases. Infections kill more men than women and several studies have pointed out differences in the immune system as a reason. The sex hormones estrogen, progesterone and testosterone all shape the effect of the immune response on multiple levels. Women at fertile age have been suggested to have higher proinflammatory responses from inflammatory stimuli compared to men and post-menopausal women, which has been ascribed to their higher estrogen levels. This could possibly lead to a more active pathogen response but may also result in a detrimental immunopathology to infections or development of autoimmune reaction. The overall aim of this thesis is to study the contribution of sex hormones and sex hormone receptors (SHR) to sex differences in immune response. We focus on peripheral blood mononuclear cells (PBMCs) to study such relationships in healthy individuals, as well as in individuals with asymptomatic Torque Teno Virus infection, and individuals with acute Puumala virus infection. In Paper I, we investigated expression of SHR and immune response genes in PBMC from healthy premenopausal (pre-MP) women during the menstrual cycle. The expression levels were estimated using a qPCR Array (Taqman low-density array, TLDA). SHR expression did not change significantly during the menstrual cycle, but several key immune regulatory genes were significantly more expressed during the ovulatory and mid luteal phase. Further, we separated PBMC into cell subsets (CD4+ T-cells, CD8+ T-cells, CD56+ NK-cells, CD14+ monocytes and CD19+ B-cells) and analyzed the expression through qPCR of estrogen receptors (ERs), ERα, ERβ1 (wildtype) and the isoform ERβ2. For the first time and unexpectedly, we demonstrate that the isoform ERβ2 was more abundant than wildtype ERβ1. The data from this paper provides new knowledge on the contribution of the menstrual cycle on immune response. In Paper II, we explored the use of Torque Ten

Published

2021

10. Estrogen deficiency – a central paradigm in age-related impaired healing?

Author

EL MOHTADI, MOHAMED, Whitehead, Kathryn, Dempsey-Hibbert, Nina, Belboul, Amina, Ashworth, Jason, EL MOHTADI, MOHAMED, Whitehead, Kathryn, Dempsey-Hibbert, Nina, Belboul, Amina, and Ashworth, Jason

Abstract

Wound healing is a dynamic biological process achieved through four sequential, overlapping phases; hemostasis, inflammation, tissue proliferation and remodeling. For effective wound healing, all four phases must occur in the appropriate order and time frame. It is well accepted that the wound healing process becomes disrupted in the elderly, increasing the propensity of non-healing wound states that can lead to substantial patient morbidity and an enormous financial burden on healthcare systems. Estrogen deprivation in the elderly has been identified as the key driver of age-related delayed wound healing in both genders, with topical and systemic estrogen replacement reversing the detrimental effects of aging on wound repair. Evidence suggests estrogen deprivation may contribute to the development of chronic wound healing states in the elderly but research in this area is somewhat limited, warranting further investigations. Moreover, although the beneficial effects of estrogen on cutaneous healing have been widely explored, the development of estrogen-based treatments to enhance wound repair in the elderly have yet to be widely exploited. This review explores the critical role of estrogen in reversing age-related impaired healing and evaluates the prospect of developing more focused novel therapeutic strategies that enhance wound repair in the elderly via activation of specific estrogen signaling pathways in regenerating tissues, whilst leaving non-target tissues largely unaffected.

Published

2021

11. Individual- and neighborhood-level socioeconomic status and risk of aggressive breast cancer subtypes in a pooled cohort of women from Kaiser Permanente Northern California.

Author

Aoki, Rhonda-Lee F, Aoki, Rhonda-Lee F, Uong, Stephen P, Gomez, Scarlett Lin, Alexeeff, Stacey E, Caan, Bette J, Kushi, Lawrence H, Torres, Jacqueline M, Guan, Alice, Canchola, Alison J, Morey, Brittany N, Lin, Katherine, Kroenke, Candyce H, Aoki, Rhonda-Lee F, Aoki, Rhonda-Lee F, Uong, Stephen P, Gomez, Scarlett Lin, Alexeeff, Stacey E, Caan, Bette J, Kushi, Lawrence H, Torres, Jacqueline M, Guan, Alice, Canchola, Alison J, Morey, Brittany N, Lin, Katherine, and Kroenke, Candyce H

Abstract

BackgroundLow socioeconomic status (SES) has been associated with a higher risk of aggressive breast cancer (BC) subtypes, but few studies have examined the independent effects of both neighborhood-level socioeconomic status (nSES) and individual-level SES measures.MethodsThis study included 5547 women from the Pathways and Life After Cancer Epidemiology cohorts who were diagnosed with invasive BC. Generalized estimating equation models were used to examine associations of nSES (a composite score based on income, poverty, education, occupation, employment, rent, and house value) and individual-level SES (income and education) with BC subtypes: luminal B (LumB), Her2-enriched (Her2-e), and triple-negative breast cancer (TNBC) relative to luminal A (LumA). Models controlled for age, race, nativity, stage, days from diagnosis to survey, and study cohort and simultaneously for nSES and individual-level SES.ResultsIn fully adjusted models, low nSES was significantly associated with the LumB (odds ratio for quartile 1 vs quartile 4 [ORQ1vQ4 ], 1.31; 95% confidence interval [CI], 1.11-1.54; P for trend = .005) and TNBC subtypes (ORQ1vQ4 , 1.32; 95% CI, 1.02-1.71; P for trend = .037) relative to LumA. Conversely, individual education was significantly associated with only the Her2-e subtype (odds ratio for high school degree or less vs postgraduate, 1.68; 95% CI, 1.03-2.75; P for trend = .030) relative to LumA. Individual income was not significantly associated with any BC subtype.ConclusionsnSES and individual-level SES are independently associated with different BC subtypes; specifically, low nSES and individual-level education are independent predictors of more aggressive BC subtypes relative to LumA.

Published

2021

12. Estrogen and Estrogen Receptor a Risk Factor in Breast Cancer - A Review

Author

Saini, Akanksha, Utkarsh, Kumar, Neha, Priyadarshini, Anjali, Saini, Akanksha, Utkarsh, Kumar, Neha, and Priyadarshini, Anjali

Abstract

There are many evidences which shows that estrogens play a crucial role in the development of breast cancer. Most established risk factors for breast cancer in humans probably act through hormone-related pathways, and increased concentrations of circulating estrogens have been found to be strongly associated with increased risk for breast cancer in postmenopausal woman. In this review we describe in detail estrogen metabolism and associated genetic variations, and provide a critical review of the current literature regarding the role of estrogens and their metabolites in breast cancer risk. Estrogens display intriguing tissue selective action that is of great biomedical importance in the development of optimal therapeutics for the prevention and treatment of breast caner. Tamoxifen has been the only drug of choice for more than 30 years to treat patients with estrogen related (ER) positive breast tumor.

Published

2021

13. Estrogen and Estrogen Receptor a Risk Factor in Breast Cancer - A Review

Author

Saini, Akanksha, Utkarsh, Kumar, Neha, Priyadarshini, Anjali, Saini, Akanksha, Utkarsh, Kumar, Neha, and Priyadarshini, Anjali

Abstract

There are many evidences which shows that estrogens play a crucial role in the development of breast cancer. Most established risk factors for breast cancer in humans probably act through hormone-related pathways, and increased concentrations of circulating estrogens have been found to be strongly associated with increased risk for breast cancer in postmenopausal woman. In this review we describe in detail estrogen metabolism and associated genetic variations, and provide a critical review of the current literature regarding the role of estrogens and their metabolites in breast cancer risk. Estrogens display intriguing tissue selective action that is of great biomedical importance in the development of optimal therapeutics for the prevention and treatment of breast caner. Tamoxifen has been the only drug of choice for more than 30 years to treat patients with estrogen related (ER) positive breast tumor.

Published

2021

14. A standardized extract of Danggui Buxue Tang decoction selectively exerts estrogenic activities distinctly from tamoxifen

Author

Zhou, Liping, Wong, Ka-Ying, Cao, Sisi, Poon, Christina Chui-Wa, Yu, Wenxuan, Dong, Xiaoli, Tsim, Karl Wah Keung, Wong, Man-Sau, Zhou, Liping, Wong, Ka-Ying, Cao, Sisi, Poon, Christina Chui-Wa, Yu, Wenxuan, Dong, Xiaoli, Tsim, Karl Wah Keung, and Wong, Man-Sau

Abstract

More and more menopausal women use Danggui Buxue Tang (DBT) for relieving their symptoms. Concerns for its safety have been raised as it contains phytoestrogen and acts via estrogen receptors (ERs). Our study aimed to determine whether DBT could selectively exert estrogenic activities and interact with tamoxifen in bone, brain, uterus, and breast by using ovariectomized (OVX) rats and ER-positive cells. In OVX rats, DBT induced a 31.4% increase in bone mineral density and restored the mRNA expression of dopamine biomarker in striatum, 3.32-fold for tyrosine hydrolase (p <.001) and 0.21-fold for dopamine transporter (p <.001), which was similar to tamoxifen; tamoxifen, but not DBT, increased uterus weight and Complement component 3 expression by more than twofold (p <.001); unlike tamoxifen, DBT induced mild proliferation in mammary gland. Two-way ANOVA indicated the interactions between them in OVX rats (p <.05) but DBT did not alter the responses to tamoxifen. DBT stimulated proliferation or differentiation and estrogen response element in MCF-7, MG-63, Ishikawa, and SHSY5Y cells and altered the effects of tamoxifen. In summary, DBT exerted estrogenic effects in tissue-selective manner, which was different from tamoxifen. DBT interacted with tamoxifen but did not significantly alter its effects in OVX rats.

Published

2021

15. Estrogen deficiency – a central paradigm in age-related impaired healing?

Author

EL MOHTADI, MOHAMED, Whitehead, Kathryn, Dempsey-Hibbert, Nina, Belboul, Amina, Ashworth, Jason, EL MOHTADI, MOHAMED, Whitehead, Kathryn, Dempsey-Hibbert, Nina, Belboul, Amina, and Ashworth, Jason

Abstract

Wound healing is a dynamic biological process achieved through four sequential, overlapping phases; hemostasis, inflammation, tissue proliferation and remodeling. For effective wound healing, all four phases must occur in the appropriate order and time frame. It is well accepted that the wound healing process becomes disrupted in the elderly, increasing the propensity of non-healing wound states that can lead to substantial patient morbidity and an enormous financial burden on healthcare systems. Estrogen deprivation in the elderly has been identified as the key driver of age-related delayed wound healing in both genders, with topical and systemic estrogen replacement reversing the detrimental effects of aging on wound repair. Evidence suggests estrogen deprivation may contribute to the development of chronic wound healing states in the elderly but research in this area is somewhat limited, warranting further investigations. Moreover, although the beneficial effects of estrogen on cutaneous healing have been widely explored, the development of estrogen-based treatments to enhance wound repair in the elderly have yet to be widely exploited. This review explores the critical role of estrogen in reversing age-related impaired healing and evaluates the prospect of developing more focused novel therapeutic strategies that enhance wound repair in the elderly via activation of specific estrogen signaling pathways in regenerating tissues, whilst leaving non-target tissues largely unaffected.

Published

2021

16. FLTX2: A Novel Tamoxifen Derivative Endowed with Antiestrogenic, Fluorescent, and Photosensitizer Properties

Author

Universidad de La Laguna, La Caixa, Cabildo de Tenerife, Ministerio de Economía y Empresa (España), Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), European Commission, Díaz, Mario, Lobo, Fernando, Hernández, Dácil, Amesty, Ángel, Valdés-Baizabal, Catalina, Canerina-Amaro, Ana, Mesa-Herrera, Fátima, Soler, Kevin, Boto, Alicia, Marín, Raquel, Estévez-Braun, Ana, Lahoz, Fernando, Universidad de La Laguna, La Caixa, Cabildo de Tenerife, Ministerio de Economía y Empresa (España), Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), European Commission, Díaz, Mario, Lobo, Fernando, Hernández, Dácil, Amesty, Ángel, Valdés-Baizabal, Catalina, Canerina-Amaro, Ana, Mesa-Herrera, Fátima, Soler, Kevin, Boto, Alicia, Marín, Raquel, Estévez-Braun, Ana, and Lahoz, Fernando

Abstract

Tamoxifen is the most widely used selective modulator of estrogen receptors (SERM) and the first strategy as coadjuvant therapy for the treatment of estrogen-receptor (ER) positive breast cancer worldwide. In spite of such success, tamoxifen is not devoid of undesirable effects, the most life-threatening reported so far affecting uterine tissues. Indeed, tamoxifen treatment is discouraged in women under risk of uterine cancers. Recent molecular design efforts have endeavoured the development of tamoxifen derivatives with antiestrogen properties but lacking agonistic uterine tropism. One of this is FLTX2, formed by the covalent binding of tamoxifen as ER binding core, 7-nitrobenzofurazan (NBD) as the florescent dye, and Rose Bengal (RB) as source for reactive oxygen species. Our analyses demonstrate (1) FLTX2 is endowed with similar antiestrogen potency as tamoxifen and its predecessor FLTX1, (2) shows a strong absorption in the blue spectral range, associated to the NBD moiety, which efficiently transfers the excitation energy to RB through intramolecular FRET mechanism, (3) generates superoxide anions in a concentration- and irradiation time-dependent process, and (4) Induces concentration- and time-dependent MCF7 apoptotic cell death. These properties make FLTX2 a very promising candidate to lead a novel generation of SERMs with the endogenous capacity to promote breast tumour cell death in situ by photosensitization.

Published

2021

17. Role of neuroglobin in the neuroprotective actions of estradiol and estrogenic compounds

Author

Barreto, George E., McGovern, A.J, García-Segura, Luis M., Barreto, George E., McGovern, A.J, and García-Segura, Luis M.

Abstract

Estradiol exerts neuroprotective actions that are mediated by the regulation of a variety of signaling pathways and homeostatic molecules. Among these is neuroglobin, which is upregulated by estradiol and translocated to the mitochondria to sustain neuronal and glial cell adaptation to injury. In this paper, we will discuss the role of neuroglobin in the neuroprotective mechanisms elicited by estradiol acting on neurons, astrocytes and microglia. We will also consider the role of neuroglobin in the neuroprotective actions of clinically relevant synthetic steroids, such as tibolone. Finally, the possible contribution of the estrogenic regulation of neuroglobin to the generation of sex differences in brain pathology and the potential application of neuroglobin as therapy against neurological diseases will be examined.

Published

2021

18. Fytoestrogeny

Author

Nováková Mužáková, Vladimíra, Mičková, Anna, Nováková Mužáková, Vladimíra, and Mičková, Anna

Abstract

Předmětem práce je zhodnocení fytoestrogenů v souvislosti s obdobím klimakteria u žen, kdy dochází ke snížení produkce estrogenů. Tato práce se zaměřuje na rozdělení fytoestrogenů a jejich interakci s estrogenními receptory., The subject of the work is the evalution of phytoestrogens in connection with menopause in women, when there is a reduction in estrogen production. This work focuses on the division of phytoestrogens and their interaction with estrogen receptors., Fakulta chemicko-technologická, 1. Prezentace výsledků bakalářské práce. 2. Diskuze k posudku vedoucího bakalářské práce. 3. Studentka zodpověděla všechny dotazy a připomínky k BP., Dokončená práce s úspěšnou obhajobou

Published

2021

19. Anabolic androgenic steroids exert a selective remodeling of the plasma lipidome that mirrors the decrease of the de novo lipogenesis in the liver

Author

Balgoma, David, Zelleroth, Sofia, Grönbladh, Alfhild, Hallberg, Mathias, Pettersson, Curt, Hedeland, Mikael, Balgoma, David, Zelleroth, Sofia, Grönbladh, Alfhild, Hallberg, Mathias, Pettersson, Curt, and Hedeland, Mikael

Abstract

Introduction: The abuse of anabolic androgenic steroids (AASs) is a source of public concern because of their adverse effects. Supratherapeutic doses of AASs are known to be hepatotoxic and regulate the lipoproteins in plasma by modifying the metabolism of lipids in the liver, which is associated with metabolic diseases. However, the effect of AASs on the profile of lipids in plasma is unknown. Objectives: To describe the changes in the plasma lipidome exerted by AASs and to discuss these changes in the light of previous research about AASs and de novo lipogenesis in the liver. Methods: We treated male Wistar rats with supratherapeutic doses of nandrolone decanoate and testosterone undecanoate. Subsequently, we isolated the blood plasma and performed lipidomics analysis by liquid chromatography-high resolution mass spectrometry. Results: Lipid profiling revealed a decrease of sphingolipids and glycerolipids with palmitic, palmitoleic, stearic, and oleic acids. In addition, lipid profiling revealed an increase in free fatty acids and glycerophospholipids with odd-numbered chain fatty acids and/or arachidonic acid. Conclusion: The lipid profile presented herein reports the imprint of AASs on the plasma lipidome, which mirrors the downregulation of de novo lipogenesis in the liver. In a broader perspective, this profile will help to understand the influence of androgens on the lipid metabolism in future studies of diseases with dysregulated lipogenesis (e.g. type 2 diabetes, fatty liver disease, and hepatocellular carcinoma).

Published

2020

20. Anabolic androgenic steroids exert a selective remodeling of the plasma lipidome that mirrors the decrease of the de novo lipogenesis in the liver

Author

Balgoma, David, Zelleroth, Sofia, Grönbladh, Alfhild, Hallberg, Mathias, Pettersson, Curt, Hedeland, Mikael, Balgoma, David, Zelleroth, Sofia, Grönbladh, Alfhild, Hallberg, Mathias, Pettersson, Curt, and Hedeland, Mikael

Abstract

Introduction: The abuse of anabolic androgenic steroids (AASs) is a source of public concern because of their adverse effects. Supratherapeutic doses of AASs are known to be hepatotoxic and regulate the lipoproteins in plasma by modifying the metabolism of lipids in the liver, which is associated with metabolic diseases. However, the effect of AASs on the profile of lipids in plasma is unknown. Objectives: To describe the changes in the plasma lipidome exerted by AASs and to discuss these changes in the light of previous research about AASs and de novo lipogenesis in the liver. Methods: We treated male Wistar rats with supratherapeutic doses of nandrolone decanoate and testosterone undecanoate. Subsequently, we isolated the blood plasma and performed lipidomics analysis by liquid chromatography-high resolution mass spectrometry. Results: Lipid profiling revealed a decrease of sphingolipids and glycerolipids with palmitic, palmitoleic, stearic, and oleic acids. In addition, lipid profiling revealed an increase in free fatty acids and glycerophospholipids with odd-numbered chain fatty acids and/or arachidonic acid. Conclusion: The lipid profile presented herein reports the imprint of AASs on the plasma lipidome, which mirrors the downregulation of de novo lipogenesis in the liver. In a broader perspective, this profile will help to understand the influence of androgens on the lipid metabolism in future studies of diseases with dysregulated lipogenesis (e.g. type 2 diabetes, fatty liver disease, and hepatocellular carcinoma).

Published

2020

21. Anabolic androgenic steroids exert a selective remodeling of the plasma lipidome that mirrors the decrease of the de novo lipogenesis in the liver

Author

Balgoma, David, Zelleroth, Sofia, Grönbladh, Alfhild, Hallberg, Mathias, Pettersson, Curt, Hedeland, Mikael, Balgoma, David, Zelleroth, Sofia, Grönbladh, Alfhild, Hallberg, Mathias, Pettersson, Curt, and Hedeland, Mikael

Abstract

Introduction: The abuse of anabolic androgenic steroids (AASs) is a source of public concern because of their adverse effects. Supratherapeutic doses of AASs are known to be hepatotoxic and regulate the lipoproteins in plasma by modifying the metabolism of lipids in the liver, which is associated with metabolic diseases. However, the effect of AASs on the profile of lipids in plasma is unknown. Objectives: To describe the changes in the plasma lipidome exerted by AASs and to discuss these changes in the light of previous research about AASs and de novo lipogenesis in the liver. Methods: We treated male Wistar rats with supratherapeutic doses of nandrolone decanoate and testosterone undecanoate. Subsequently, we isolated the blood plasma and performed lipidomics analysis by liquid chromatography-high resolution mass spectrometry. Results: Lipid profiling revealed a decrease of sphingolipids and glycerolipids with palmitic, palmitoleic, stearic, and oleic acids. In addition, lipid profiling revealed an increase in free fatty acids and glycerophospholipids with odd-numbered chain fatty acids and/or arachidonic acid. Conclusion: The lipid profile presented herein reports the imprint of AASs on the plasma lipidome, which mirrors the downregulation of de novo lipogenesis in the liver. In a broader perspective, this profile will help to understand the influence of androgens on the lipid metabolism in future studies of diseases with dysregulated lipogenesis (e.g. type 2 diabetes, fatty liver disease, and hepatocellular carcinoma).

Published

2020

22. A Possible Link of Genetic Variations in ER/IGF1R Pathway and Risk of Melanoma.

Author

Yuan, Tze-An, Yuan, Tze-An, Yourk, Vandy, Farhat, Ali, Guo, Katherine L, Garcia, Angela, Meyskens, Frank L, Liu-Smith, Feng, Yuan, Tze-An, Yuan, Tze-An, Yourk, Vandy, Farhat, Ali, Guo, Katherine L, Garcia, Angela, Meyskens, Frank L, and Liu-Smith, Feng

Abstract

The mechanism of gender disparity in cutaneous melanoma incidence remains unclear. Steroid hormones including estrogens have long been implicated in the course of melanoma, but the conclusion is controversial. Estrogen receptors (ERs) and insulin-like growth factor 1 receptor (IGF1R) show extensive crosstalk in cancer development, but how the ER/IGF1R network impacts melanoma is currently unclear. Here we studied the melanoma associations of selected SNPs from the ER/IGF1R network. Part of the International Genes, Environment, and Melanoma (GEM) cohort was used as a discovery set, and the Gene Environment Association Studies Initiative (GENEVA) dataset served as a validation set. Based on the associations with other malignant disease conditions, thirteen single nucleotide polymorphism (SNP) variants in ESR1, ESR2, IGF1, and IGF1R were selected for candidate gene association analyses. The rs1520220 in IGF1 and rs2229765 in IGF1R variants were significantly associated with melanoma risk in the GEM dataset after Benjamini-Hochberg multiple comparison correction, although they were not validated in the GENEVA set. The discrepancy may be caused by the multiple melanoma characteristics in the GEM patients. Further analysis of gender disparity was carried out for IGF1 and IGF1R SNPs in the GEM dataset. The GG phenotype in IGF1 rs1520220 (recessive model) presented an increased risk of melanoma (OR = 8.11, 95% CI: 2.20, 52.5, p = 0.006) in men but a significant opposite effect in women (OR = 0.15, 95% CI: 0.018, 0.86, p = 0.045). The AA genotype in IGF1R rs2229765 (recessive model) showed a significant protective effect in men (OR = 0.24, 95% CI: 0.07, 0.64, p = 0.008) and no effect in women. Results from the current study are warranted for further validation.

Published

2020

23. A standardized extract of Danggui Buxue Tang decoction selectively exerts estrogenic activities distinctly from tamoxifen

Author

Zhou, Liping, Wong, Ka-Ying, Cao, Sisi, Poon, Christina Chui-Wa, Yu, Wenxuan, Dong, Xiaoli, Tsim, Karl Wah Keung, Wong, Man-Sau, Zhou, Liping, Wong, Ka-Ying, Cao, Sisi, Poon, Christina Chui-Wa, Yu, Wenxuan, Dong, Xiaoli, Tsim, Karl Wah Keung, and Wong, Man-Sau

Abstract

More and more menopausal women use Danggui Buxue Tang (DBT) for relieving their symptoms. Concerns for its safety have been raised as it contains phytoestrogen and acts via estrogen receptors (ERs). Our study aimed to determine whether DBT could selectively exert estrogenic activities and interact with tamoxifen in bone, brain, uterus, and breast by using ovariectomized (OVX) rats and ER-positive cells. In OVX rats, DBT induced a 31.4% increase in bone mineral density and restored the mRNA expression of dopamine biomarker in striatum, 3.32-fold for tyrosine hydrolase (p <.001) and 0.21-fold for dopamine transporter (p <.001), which was similar to tamoxifen; tamoxifen, but not DBT, increased uterus weight and Complement component 3 expression by more than twofold (p <.001); unlike tamoxifen, DBT induced mild proliferation in mammary gland. Two-way ANOVA indicated the interactions between them in OVX rats (p <.05) but DBT did not alter the responses to tamoxifen. DBT stimulated proliferation or differentiation and estrogen response element in MCF-7, MG-63, Ishikawa, and SHSY5Y cells and altered the effects of tamoxifen. In summary, DBT exerted estrogenic effects in tissue-selective manner, which was different from tamoxifen. DBT interacted with tamoxifen but did not significantly alter its effects in OVX rats.

Published

2020

24. A standardized extract of Danggui Buxue Tang decoction selectively exerts estrogenic activities distinctly from tamoxifen

Author

Zhou, Liping, Wong, Ka-Ying, Cao, Sisi, Poon, Christina Chui-Wa, Yu, Wenxuan, Dong, Xiaoli, Tsim, Karl Wah Keung, Wong, Man-Sau, Zhou, Liping, Wong, Ka-Ying, Cao, Sisi, Poon, Christina Chui-Wa, Yu, Wenxuan, Dong, Xiaoli, Tsim, Karl Wah Keung, and Wong, Man-Sau

Abstract

More and more menopausal women use Danggui Buxue Tang (DBT) for relieving their symptoms. Concerns for its safety have been raised as it contains phytoestrogen and acts via estrogen receptors (ERs). Our study aimed to determine whether DBT could selectively exert estrogenic activities and interact with tamoxifen in bone, brain, uterus, and breast by using ovariectomized (OVX) rats and ER-positive cells. In OVX rats, DBT induced a 31.4% increase in bone mineral density and restored the mRNA expression of dopamine biomarker in striatum, 3.32-fold for tyrosine hydrolase (p <.001) and 0.21-fold for dopamine transporter (p <.001), which was similar to tamoxifen; tamoxifen, but not DBT, increased uterus weight and Complement component 3 expression by more than twofold (p <.001); unlike tamoxifen, DBT induced mild proliferation in mammary gland. Two-way ANOVA indicated the interactions between them in OVX rats (p <.05) but DBT did not alter the responses to tamoxifen. DBT stimulated proliferation or differentiation and estrogen response element in MCF-7, MG-63, Ishikawa, and SHSY5Y cells and altered the effects of tamoxifen. In summary, DBT exerted estrogenic effects in tissue-selective manner, which was different from tamoxifen. DBT interacted with tamoxifen but did not significantly alter its effects in OVX rats.

Published

2020

25. A Possible Link of Genetic Variations in ER/IGF1R Pathway and Risk of Melanoma.

Author

Yuan, Tze-An, Yuan, Tze-An, Yourk, Vandy, Farhat, Ali, Guo, Katherine L, Garcia, Angela, Meyskens, Frank L, Liu-Smith, Feng, Yuan, Tze-An, Yuan, Tze-An, Yourk, Vandy, Farhat, Ali, Guo, Katherine L, Garcia, Angela, Meyskens, Frank L, and Liu-Smith, Feng

Abstract

The mechanism of gender disparity in cutaneous melanoma incidence remains unclear. Steroid hormones including estrogens have long been implicated in the course of melanoma, but the conclusion is controversial. Estrogen receptors (ERs) and insulin-like growth factor 1 receptor (IGF1R) show extensive crosstalk in cancer development, but how the ER/IGF1R network impacts melanoma is currently unclear. Here we studied the melanoma associations of selected SNPs from the ER/IGF1R network. Part of the International Genes, Environment, and Melanoma (GEM) cohort was used as a discovery set, and the Gene Environment Association Studies Initiative (GENEVA) dataset served as a validation set. Based on the associations with other malignant disease conditions, thirteen single nucleotide polymorphism (SNP) variants in ESR1, ESR2, IGF1, and IGF1R were selected for candidate gene association analyses. The rs1520220 in IGF1 and rs2229765 in IGF1R variants were significantly associated with melanoma risk in the GEM dataset after Benjamini-Hochberg multiple comparison correction, although they were not validated in the GENEVA set. The discrepancy may be caused by the multiple melanoma characteristics in the GEM patients. Further analysis of gender disparity was carried out for IGF1 and IGF1R SNPs in the GEM dataset. The GG phenotype in IGF1 rs1520220 (recessive model) presented an increased risk of melanoma (OR = 8.11, 95% CI: 2.20, 52.5, p = 0.006) in men but a significant opposite effect in women (OR = 0.15, 95% CI: 0.018, 0.86, p = 0.045). The AA genotype in IGF1R rs2229765 (recessive model) showed a significant protective effect in men (OR = 0.24, 95% CI: 0.07, 0.64, p = 0.008) and no effect in women. Results from the current study are warranted for further validation.

Published

2020

26. Anabolic androgenic steroids exert a selective remodeling of the plasma lipidome that mirrors the decrease of the de novo lipogenesis in the liver

Author

Balgoma, David, Zelleroth, Sofia, Grönbladh, Alfhild, Hallberg, Mathias, Pettersson, Curt, Hedeland, Mikael, Balgoma, David, Zelleroth, Sofia, Grönbladh, Alfhild, Hallberg, Mathias, Pettersson, Curt, and Hedeland, Mikael

Abstract

Introduction: The abuse of anabolic androgenic steroids (AASs) is a source of public concern because of their adverse effects. Supratherapeutic doses of AASs are known to be hepatotoxic and regulate the lipoproteins in plasma by modifying the metabolism of lipids in the liver, which is associated with metabolic diseases. However, the effect of AASs on the profile of lipids in plasma is unknown. Objectives: To describe the changes in the plasma lipidome exerted by AASs and to discuss these changes in the light of previous research about AASs and de novo lipogenesis in the liver. Methods: We treated male Wistar rats with supratherapeutic doses of nandrolone decanoate and testosterone undecanoate. Subsequently, we isolated the blood plasma and performed lipidomics analysis by liquid chromatography-high resolution mass spectrometry. Results: Lipid profiling revealed a decrease of sphingolipids and glycerolipids with palmitic, palmitoleic, stearic, and oleic acids. In addition, lipid profiling revealed an increase in free fatty acids and glycerophospholipids with odd-numbered chain fatty acids and/or arachidonic acid. Conclusion: The lipid profile presented herein reports the imprint of AASs on the plasma lipidome, which mirrors the downregulation of de novo lipogenesis in the liver. In a broader perspective, this profile will help to understand the influence of androgens on the lipid metabolism in future studies of diseases with dysregulated lipogenesis (e.g. type 2 diabetes, fatty liver disease, and hepatocellular carcinoma).

Published

2020

27. Anabolic androgenic steroids exert a selective remodeling of the plasma lipidome that mirrors the decrease of the de novo lipogenesis in the liver

Author

Balgoma, David, Zelleroth, Sofia, Grönbladh, Alfhild, Hallberg, Mathias, Pettersson, Curt, Hedeland, Mikael, Balgoma, David, Zelleroth, Sofia, Grönbladh, Alfhild, Hallberg, Mathias, Pettersson, Curt, and Hedeland, Mikael

Abstract

Introduction: The abuse of anabolic androgenic steroids (AASs) is a source of public concern because of their adverse effects. Supratherapeutic doses of AASs are known to be hepatotoxic and regulate the lipoproteins in plasma by modifying the metabolism of lipids in the liver, which is associated with metabolic diseases. However, the effect of AASs on the profile of lipids in plasma is unknown. Objectives: To describe the changes in the plasma lipidome exerted by AASs and to discuss these changes in the light of previous research about AASs and de novo lipogenesis in the liver. Methods: We treated male Wistar rats with supratherapeutic doses of nandrolone decanoate and testosterone undecanoate. Subsequently, we isolated the blood plasma and performed lipidomics analysis by liquid chromatography-high resolution mass spectrometry. Results: Lipid profiling revealed a decrease of sphingolipids and glycerolipids with palmitic, palmitoleic, stearic, and oleic acids. In addition, lipid profiling revealed an increase in free fatty acids and glycerophospholipids with odd-numbered chain fatty acids and/or arachidonic acid. Conclusion: The lipid profile presented herein reports the imprint of AASs on the plasma lipidome, which mirrors the downregulation of de novo lipogenesis in the liver. In a broader perspective, this profile will help to understand the influence of androgens on the lipid metabolism in future studies of diseases with dysregulated lipogenesis (e.g. type 2 diabetes, fatty liver disease, and hepatocellular carcinoma).

Published

2020

28. Farnesoid X receptor as marker of osteotropism of breast cancers through its role in the osteomimetism of tumor cells

Author

Absil, Lara, Journé, Fabrice, Larsimont, Denis, Body, Jean-Jacques, Tafforeau, Lionel, Nonclercq, Denis, Absil, Lara, Journé, Fabrice, Larsimont, Denis, Body, Jean-Jacques, Tafforeau, Lionel, and Nonclercq, Denis

Abstract

Background: The skeleton is the first and most common distant metastatic site for breast cancer. Such metastases complicate cancer management, inducing considerable morbidities and decreasing patient survival. Osteomimetism is part of the complex process of osteotropism of breast cancer cells. Recent data indicate that Farnesoid X Receptor (FXR) is involved in the transformation and progression of breast cancer. Methods: The expression of FXR, Runt-related transcription factor 2 (RUNX2) and bone proteins were evaluated on two tumor cell lines (MCF-7 and MDA-MB-231) by immunohistochemistry, immunofluorescence and western blotting and quantified. Results: In a series of 81 breast cancer patients who developed distant metastases, we found a strong correlation between FXR expression in primary breast tumors and the development of bone metastases, especially in patients with histological grade 3 tumors. In in vitro studies, FXR activation by Chenodeoxycholic acid (CDCA) increased the expression of numerous bone proteins. FXR inhibition by lithocholic acid and z-guggulsterone decreased bone protein expression. Short Hairpin RNA (ShRNA) against FXR validated the involvement of FXR in the osteomimetism of breast cancer cells. Conclusion: Our experimental results point to a relationship between the expression of FXR in breast cancer cells and the propensity of these tumor cells to develop bone metastases. FXR induces the expression of RUNX2 which itself causes the synthesis of bone proteins by tumor cells., SCOPUS: ar.j, info:eu-repo/semantics/published

Published

2020

29. Tumor-suppressive functions of 4-MU on breast cancer cells of different ER status : Regulation of hyaluronan/HAS2/CD44 and specific matrix effectors

Author

Karalis, Theodoros T., Heldin, Paraskevi, Vynios, Demitrios H., Neill, Thomas, Buraschi, Simone, Iozzo, Renato V., Karamanos, Nikos K., Skandalis, Spyros S., Karalis, Theodoros T., Heldin, Paraskevi, Vynios, Demitrios H., Neill, Thomas, Buraschi, Simone, Iozzo, Renato V., Karamanos, Nikos K., and Skandalis, Spyros S.

Abstract

The malignant phenotype of various cancers is linked to enhanced expression of hyaluronan, a proangiogenic glycosaminoglycan whose expression is suppressed by 4-methylumbelliferone (4-MU), a non-toxic oral agent used as a dietary supplement to improve health and combat prostate cancer. In this study, we investigated the role of 4-MU in mammary carcinoma cells with distinct malignant phenotypes and estrogen receptor (ER) status, a major prognostic factor in the clinical management of breast cancers. We focused on two breast cancer cell lines, the low metastatic and ER alpha+ MCF-7 cells, and the highly-aggressive and ER alpha-MDA-MB-231 cells. Treatment with 4-MU caused a dose-dependent decrease of hyaluronan accumulation in the extracellular matrix as well as within the breast cancer cells, most prevalent in cells lacking ER alpha. This decrease in hyaluronan was accompanied by suppression of Hyaluronan Synthase 2 (HAS2), the major enzyme responsible for the synthesis of hyaluronan, and by induction of hyaluronidases (HYALs) -1 and -2. Moreover, 4-MU induced intense phenotypic changes and substantial loss of CD44, a major hyaluronan receptor, from cell protrusions. Importantly, 4-MU evoked differential effects depending on the absence or presence of ER alpha. Only the ER alpha+ cells showed signs of apoptosis, as determined by cleaved PARP-1, and anoikis as shown by concurrent loss of E-cadherin and beta-catenin. Interestingly, 4-MU significantly reduced migration, adhesion and invasion of ER alpha- breast cancer cells, and concurrently reduced the expression and activity of several matrix degrading enzymes and pro-inflammatory molecules with tumor-promoting functions. Collectively, our findings suggest that 4-MU could represent a novel therapeutic for specific breast cancer subtypes with regard to their ER status via suppression of hyaluronan synthesis and regulation of HAS2, CD44, matrix-degrading enzymes and inflammatory mediators.

Published

2019

30. Estrogenic regulation of neuroprotective and neuroinflammatory mechanisms: implications for depression and cognition

Author

Ministerio de Economía, Industria y Competitividad (España), Centro de Investigación Biomédica en Red de Fragilidad y Envejecimiento Saludable (España), Instituto de Salud Carlos III, European Commission, Yanguas-Casás, Natalia, Brocca, M.E., Azcoitia, I., Arévalo, María Ángeles, García-Segura, Luis M., Ministerio de Economía, Industria y Competitividad (España), Centro de Investigación Biomédica en Red de Fragilidad y Envejecimiento Saludable (España), Instituto de Salud Carlos III, European Commission, Yanguas-Casás, Natalia, Brocca, M.E., Azcoitia, I., Arévalo, María Ángeles, and García-Segura, Luis M.

Abstract

Glial cells, such as astrocytes and microglia, contribute to maintain tissue homeostasis in the brain and are involved in the control of neuronal function, synaptic plasticity, and neuroinflammation. In the aged brain and under neurodegenerative conditions, microglial cells acquire a senescent reactive phenotype, which involves a dysregulated inflammatory response that affects the normal function and metabolism of neurons and other cell types, including astrocytes. The impaired function of astrocytes and microglia in the aged brain increases neuroinflammation, which is associated with depressive disorders and cognitive deficits. Estradiol, from gonadal origin or locally produced in the brain, exerts anti-inflammatory actions in the central nervous system, regulating the reactive phenotype of astrocytes and microglia. In addition, estrogen receptor signaling exerts direct neuroprotective actions on neurons and interacts with the signaling of other neuroprotective and anti-inflammatory factors in the brain. These actions of estradiol and estrogen receptors contribute to maintain a proper neuronal information processing, promoting cognitive function and preventing affective disorders. The effects of estradiol are imitated by synthetic estrogenic compounds, such as some selective estrogen receptor modulators and tibolone.

Published

2019

31. Molecular mechanisms involved in the protective actions of Selective Estrogen Receptor Modulators in brain cells

Author

Pontificia Universidad Javeriana, Baez-Jurado, E., Rincón-Benavides, M.A., Hidalgo-Lanussa, O., Guio-Vega, G., Ashraf, G.M., Sahebkar, A., Echeverria, Valentina, García-Segura, Luis M., Barreto, George E., Pontificia Universidad Javeriana, Baez-Jurado, E., Rincón-Benavides, M.A., Hidalgo-Lanussa, O., Guio-Vega, G., Ashraf, G.M., Sahebkar, A., Echeverria, Valentina, García-Segura, Luis M., and Barreto, George E.

Abstract

Synthetic selective modulators of the estrogen receptors (SERMs) have shown to protect neurons and glial cells against toxic insults. Among the most relevant beneficial effects attributed to these compounds are the regulation of inflammation, attenuation of astrogliosis and microglial activation, prevention of excitotoxicity and as a consequence the reduction of neuronal cell death. Under pathological conditions, the mechanism of action of the SERMs involves the activation of estrogen receptors (ERs) and G protein-coupled receptor for estrogens (GRP30). These receptors trigger neuroprotective responses such as increasing the expression of antioxidants and the activation of kinase-mediated survival signaling pathways. Despite the advances in the knowledge of the pathways activated by the SERMs, their mechanism of action is still not entirely clear, and there are several controversies. In this review, we focused on the molecular pathways activated by SERMs in brain cells, mainly astrocytes, as a response to treatment with raloxifene and tamoxifen.

Published

2019

32. Differential expression of gonadotropin and estrogen receptors and oocyte cytology during follicular maturation associated with egg viability in European eel (Anguilla anguilla)

Author

da Silva, Filipa F. G., Tveiten, Helge, Maugars, Gersende, Lafont, Anne-Gaëlle, Dufour, Sylvie, Støttrup, Josianne Gatt, Kjørsvik, Elin, Tomkiewicz, Jonna, da Silva, Filipa F. G., Tveiten, Helge, Maugars, Gersende, Lafont, Anne-Gaëlle, Dufour, Sylvie, Støttrup, Josianne Gatt, Kjørsvik, Elin, and Tomkiewicz, Jonna

Abstract

In captivity, oogenesis and ovarian follicle maturation in European eel can be induced experimentally using hormonal therapy. The follicle's ability to respond effectively to the induction of maturation and ovulation, resulting in viable eggs, depends on the oocyte stage at the time of induction. We hypothesized that variation in the expression of key hormone receptors in the ovary and size of oocyte lipid droplets are associated with changes in oocyte stage. Thus, we induced ovarian follicle maturation using a priming dose of fish pituitary extract followed by the administration of a 17α, 20β-dihydroxy-4-pregnen-3-one (DHP) injection. Females were then strip-spawned, the eggs were fertilized in vitro, incubated and larval survival was recorded at 3 days post hatch (dph). The expression of gonadotropin receptors (fshr, lhcgr1 and lhcgr2) and estrogen receptors (esr1, esr2a, esr2b, gpera and gperb) was quantified and the size of oocyte lipid droplets measured. Larval survival at 3 dph was used to differentiate high- and low-quality egg batches. Results showed significantly higher abundance of lhcgr1 and esr2a at priming for high-quality egg batches whereas fshr and gperb transcripts were significantly higher at DHP injection for low-quality egg batches. Therefore, high levels of lhcgr1 and esr2a may be important for attaining follicular maturational competence, while high fshr and gperb mRNA levels may indicate inadequate maturational competence. Furthermore, lipid droplet size at DHP and in ovulated eggs was significantly smaller in high-quality egg batches than in low-quality, which indicates that droplet size may be a useful marker of follicular maturational stage.

Published

2018

33. Morphological characteristics and expression of estrogen and progesterone receptors in the canine endometrium during the estrus cycle, cystic endometrial hyperplasia and pyometra

Author

Marinković, Darko, Aničić, Milan, Vakanjac, Slobodanka, Nedić, Svetlana, Magaš, Vladimir, Marinković, Darko, Aničić, Milan, Vakanjac, Slobodanka, Nedić, Svetlana, and Magaš, Vladimir

Abstract

The estrus cycle of bitches is divided into four phases: proestrus, estrus, diestrus and anestrus, during which different morphological changes, and also cyclic changes of estrogen and progesterone receptors are present. Several pathological changes can be differentiated on the endometrium, but one of these is the most important - cystic endometrial hyperplasia, which frequently develops into pyometra. The aim of the present study was to describe morphological characteristics, and expression of estrogen and progesterone receptors on the endometrium of mixed-breed bitches during the different phases of the estrus cycle, cystic endometrial hyperplasia and pyometra. The uterus and ovaries of 36 mixed breed bitches in different phases of the estrus cycle and also with cystic endometrial hyperplasia (CEH) and chronic purulent endometritis - pyometra were examined macroscopically, histopathologically, and immunohistochemically for estrogen receptors (ER) and progesterone receptors (PR). During proestrus uterine cells showed a weak reaction for both estrogen and progesterone receptors, but during estrus a large number of uterine cells showed a strong reaction on estrogen receptors and moderate reaction on progesterone receptors. On the contrary, during diestrus the scores for the estrogen receptors decreased, while the progesterone receptors level increased - uterine cells expressed strong reaction for progesterone receptors, and moderate reaction for estrogen receptors. Uterine cells in cystic endometrial hyperplasia expressed a strong reaction for estrogen receptors, and moderate reaction for progesterone receptors, but on the other hand the uterine cells in the uterus with pyometra expressed a moderate to strong reaction for progesterone receptors, and a weak reaction for estrogen receptors. In further investigations it would be interesting to perform quantitative analysis for both estrogen and progesterone receptors during different phases of the estrus cycle and also

Published

2018

34. Estrogen receptor a- (ERa), but not ERb-signaling, is crucial for mechanostimulation of bone fracture healing

Author

Haffner-Luntzer, M, Lackner, I, Vikmann, A, Mödinger, Y, Ignatius, A, Haffner-Luntzer, M, Lackner, I, Vikmann, A, Mödinger, Y, and Ignatius, A

Published

2018

35. Role of estrogens in fish immunity with special emphasis on GPER1

Author

Cabas, Isabel, Chaves-Pozo, Elena, Mulero, Victoriano, García-Ayala, Alfonsa, Cabas, Isabel, Chaves-Pozo, Elena, Mulero, Victoriano, and García-Ayala, Alfonsa

Abstract

It is well accepted that estrogens, the primary female sex hormones, play a key role in modulating different aspects of the immune response. Moreover, estrogens have been linked with the sexual dimorphism observed in some immune disorders, such as chronic inflammatory and autoimmune diseases. Nevertheless, their effects are often controversial and depend on several factors, such as the pool of estrogen receptors (ERs) involved in the response. Their classical mode of action is through nuclear ERs, which act as transcription factors, promoting the regulation of target genes. However, it has long been noted that some of the estrogen-mediated effects cannot be explained by these classical receptors, since they are rapid and mediated by non-genomic signaling pathways. Hence, the interest in membrane ERs, especially in G protein-coupled estrogen receptor 1 (GPER1), has grown in recent years. Although the presence of nuclear ERs, and ER signaling, in immune cells in mammals and fish has been well documented, information on membrane ERs is much scarcer. In this context, the present manuscript aims to review our knowledge concerning the effect of estrogens on fish immunity, with special emphasis on GPER1. For example, the numerous tools developed over recent years allowed us to report for the first time that the regulation of fish granulocyte functions by estrogens through GPER1 predates the split of fish and tetrapods more than 450 million years ago, pointing to the relevance of estrogens as modulators of the immune responses, and the pivotal role of GPER1 in immunity.

Published

2018

36. Morphological characteristics and expression of estrogen and progesterone receptors in the canine endometrium during the estrus cycle, cystic endometrial hyperplasia and pyometra

Author

Marinković, Darko, Aničić, Milan, Vakanjac, Slobodanka, Nedić, Svetlana, Magaš, Vladimir, Marinković, Darko, Aničić, Milan, Vakanjac, Slobodanka, Nedić, Svetlana, and Magaš, Vladimir

Abstract

The estrus cycle of bitches is divided into four phases: proestrus, estrus, diestrus and anestrus, during which different morphological changes, and also cyclic changes of estrogen and progesterone receptors are present. Several pathological changes can be differentiated on the endometrium, but one of these is the most important - cystic endometrial hyperplasia, which frequently develops into pyometra. The aim of the present study was to describe morphological characteristics, and expression of estrogen and progesterone receptors on the endometrium of mixed-breed bitches during the different phases of the estrus cycle, cystic endometrial hyperplasia and pyometra. The uterus and ovaries of 36 mixed breed bitches in different phases of the estrus cycle and also with cystic endometrial hyperplasia (CEH) and chronic purulent endometritis - pyometra were examined macroscopically, histopathologically, and immunohistochemically for estrogen receptors (ER) and progesterone receptors (PR). During proestrus uterine cells showed a weak reaction for both estrogen and progesterone receptors, but during estrus a large number of uterine cells showed a strong reaction on estrogen receptors and moderate reaction on progesterone receptors. On the contrary, during diestrus the scores for the estrogen receptors decreased, while the progesterone receptors level increased - uterine cells expressed strong reaction for progesterone receptors, and moderate reaction for estrogen receptors. Uterine cells in cystic endometrial hyperplasia expressed a strong reaction for estrogen receptors, and moderate reaction for progesterone receptors, but on the other hand the uterine cells in the uterus with pyometra expressed a moderate to strong reaction for progesterone receptors, and a weak reaction for estrogen receptors. In further investigations it would be interesting to perform quantitative analysis for both estrogen and progesterone receptors during different phases of the estrus cycle and also

Published

2018

37. Effect of Thyponium flageliforme in Combination with Curcuma zedoaria and Phyllanthus niruri in Expression of Protein Estrogen Receptor and Caspase-9 on Breast Cancer Mice

Author

Widayati, Eni, Chodidjah, Nasihun, Taufiqurrachman, Widayati, Eni, Chodidjah, and Nasihun, Taufiqurrachman

Abstract

Introduction: Incidence of breast cancer is high and constitutes a significant cause of female mortality. One of breast cancer type is Estrogen and Progesteron Receptor (ER and PR) positive, therefore affected by estrogen and progesteron concentration. Treatment of Thyponium flageliforme in combination with Curcuma zedoaria, and Phyllanthus niruri (TCP) have been proven capable of inhibiting tumor cells proliferation. Objective: To evaluate the expression of protein estrogen receptor and caspase-9 in C3H mice were inoculated with adenocarcinoma cells. Methods: 18 mice were inoculated with one million cells of breast adenocarcinoma per mouse and assigned into three groups. TCP with dosage 85 and 125 mg were treated for 21 days to evaluate the expression of protein estrogen receptor and caspase-9 measured by immuno-histochemical staining. Results: Mann Whitney analysis demonstrated that expression of protein estrogen receptor and caspase-9 in TCP 125 was significant (p < 0.05). Conclusion: Expression of protein estrogen receptor was decreased and caspase-9 expression was increased by TCP administration.

Published

2018

38. Mitochondrial estrogen receptors as a vulnerability factor of chronic stress and mediator of fluoxetine treatment in female and male rat hippocampus

Author

Adžić, Miroslav, Mitić, Miloš, Radoičić, Marija B., Adžić, Miroslav, Mitić, Miloš, and Radoičić, Marija B.

Abstract

Depression is a disease of an abnormal brain energy metabolism also marked with increased apoptosis in specific brain regions. Mounting evidence indicates that the mitochondrial oxidative phosphorylation and apoptosis are novel targets for the actions of estrogen receptors (ERs). In this study, we examined the effects of antidepressant (AD) fluoxetine (FLU) treatment on the mitochondria] ER alpha (ER alpha), ER beta (total and phospho-pER(beta) and their association with cytochrome c (cyt oxidase activity and apoptotic Bcl2/Bax-molecules in the hippocampal mitochondria of chronically isolated (CPSI) female and male rats depicting depression. Impaired behaviour induced by CPSI was followed by decreased corticosterone (CORT) in both sexes and downregulation of cyt c oxidase in males. CPSI did not affect the ERa in either of sexes, but it decreased mitochondrial ER beta and increased pER beta in both sexes. Stress-reduced ER beta is associated with a decrease in mitochondrial energetic processes in males and with apoptotic mechanisms in females. FLU normalized behaviour in both sexes and increased cyt c oxidase in females. FLU elevated ERa in males, increased ER beta and decreased pERB in both sexes. The AD-induced alterations of ER beta paralleled with bioenergetics and pro-survival pathways in females. In conclusion, sex-unspecific regulation of ER beta by the stress and by AD and its differential convergence with bioenergetics and apoptotic pathways in females and males implies its role as a vulnerability factor in the stress response and emphasizes mitochondrial ER beta-dependent pathways as an important gateway of ADs action, at least in females. (C) 2017 Elsevier B.V. All rights reserved.

Published

2017

39. Mitochondrial estrogen receptors as a vulnerability factor of chronic stress and mediator of fluoxetine treatment in female and male rat hippocampus

Author

Adžić, Miroslav, Mitić, Miloš, Radoičić, Marija B., Adžić, Miroslav, Mitić, Miloš, and Radoičić, Marija B.

Abstract

Depression is a disease of an abnormal brain energy metabolism also marked with increased apoptosis in specific brain regions. Mounting evidence indicates that the mitochondrial oxidative phosphorylation and apoptosis are novel targets for the actions of estrogen receptors (ERs). In this study, we examined the effects of antidepressant (AD) fluoxetine (FLU) treatment on the mitochondria] ER alpha (ER alpha), ER beta (total and phospho-pER(beta) and their association with cytochrome c (cyt oxidase activity and apoptotic Bcl2/Bax-molecules in the hippocampal mitochondria of chronically isolated (CPSI) female and male rats depicting depression. Impaired behaviour induced by CPSI was followed by decreased corticosterone (CORT) in both sexes and downregulation of cyt c oxidase in males. CPSI did not affect the ERa in either of sexes, but it decreased mitochondrial ER beta and increased pER beta in both sexes. Stress-reduced ER beta is associated with a decrease in mitochondrial energetic processes in males and with apoptotic mechanisms in females. FLU normalized behaviour in both sexes and increased cyt c oxidase in females. FLU elevated ERa in males, increased ER beta and decreased pERB in both sexes. The AD-induced alterations of ER beta paralleled with bioenergetics and pro-survival pathways in females. In conclusion, sex-unspecific regulation of ER beta by the stress and by AD and its differential convergence with bioenergetics and apoptotic pathways in females and males implies its role as a vulnerability factor in the stress response and emphasizes mitochondrial ER beta-dependent pathways as an important gateway of ADs action, at least in females. (C) 2017 Elsevier B.V. All rights reserved.

Published

2017

40. Interaction of sex chromosome complement, gonadal hormones and neuronal steroid synthesis on the sexual differentiation of mammalian neurons

Author

Agencia Nacional de Promoción Científica y Tecnológica (Argentina), Consejo Nacional de Investigaciones Científicas y Técnicas (Argentina), Universidad de Córdoba (España), Consejo Superior de Investigaciones Científicas (España), Ministerio de Economía, Industria y Competitividad (España), Centro de Investigación Biomédica en Red de Fragilidad y Envejecimiento Saludable (España), Instituto de Salud Carlos III, European Commission, Cambiasso, M. J, Cisternas, Carla D., Ruiz-Palmero, Isabel, Scerbo, M. Julia, Arévalo, María Ángeles, Azcoitia, I., García-Segura, Luis M., Agencia Nacional de Promoción Científica y Tecnológica (Argentina), Consejo Nacional de Investigaciones Científicas y Técnicas (Argentina), Universidad de Córdoba (España), Consejo Superior de Investigaciones Científicas (España), Ministerio de Economía, Industria y Competitividad (España), Centro de Investigación Biomédica en Red de Fragilidad y Envejecimiento Saludable (España), Instituto de Salud Carlos III, European Commission, Cambiasso, M. J, Cisternas, Carla D., Ruiz-Palmero, Isabel, Scerbo, M. Julia, Arévalo, María Ángeles, Azcoitia, I., and García-Segura, Luis M.

Abstract

Female mouse hippocampal and hypothalamic neurons growing in vitro show a faster development of neurites than male mouse neurons. This sex difference in neuritogenesis is determined by higher expression levels of the neuritogenic factor neurogenin 3 in female neurons. Experiments with the four core genotype mouse model, in which XX and XY animals with male gonads and XX and XY animals with female gonads are generated, indicate that higher levels of neurogenin 3 in developing neurons are determined by the presence of the XX chromosome complement. Female XX neurons express higher levels of estrogen receptors than male XY neurons. In female XX neurons, neuronal derived estradiol increases neurogenin 3 expression and neuritogenesis. In contrast, neuronal-derived estradiol is not able to upregulate neurogenin 3 in male XY neurons, resulting in decreased neuritogenesis compared to female neurons. However, exogenous testosterone increases neurogenin 3 expression and neuritogenesis in male XY neurons. These findings suggest that sex differences in neuronal development are determined by the interaction of sex chromosomes, neuronal derived estradiol and gonadal hormones.

Published

2017

41. Effect of macrophages on breast cancer cell proliferation, and on expression of hormone receptors, uPAR and HER-2

Author

Lindsten, Therése, Hedbrant, Alexander, Ramberg, Anna, Wijkander, Jonny, Solterbeck, Anja, Eriksson, Margareta, Delbro, Dick, Erlandsson, Ann, Lindsten, Therése, Hedbrant, Alexander, Ramberg, Anna, Wijkander, Jonny, Solterbeck, Anja, Eriksson, Margareta, Delbro, Dick, and Erlandsson, Ann

Abstract

Malignant tumors, including breast cancers, are frequently infiltrated with innate immune cells and tumor-associated macrophages (TAMs) represent the major inflammatory component in stroma of many tumors. In this study, we examined the immunoreactivity of the macrophage markers CD68 and CD163 as well as the hormone receptors estrogen receptor alpha (ER alpha), progesterone receptor (PR), estrogen receptor beta 1 (ER beta 1), human epidermal growth factor receptor 2 (HER-2), matrix metalloproteinase 9 (MMP-9), urokinase-type plasminogen activator receptor (uPAR) and the proliferations marker Ki67 in 17 breast cancer biopsies. The quantitative score for CD68(+) and CD163(+) strongly indicate M2 phenotype dominance in the currently investigated biopsies. We found that an increasing level of macrophages was negatively associated with ER alpha or PR, whereas a positive association was observed for Ki-67 or uPAR. No significant association could be seen between the level of macrophage and HER-2, ER beta 1 or MMP-9 expression. Effect of conditioned media (CM) generated from cultured human M1 and M2 macrophage phenotypes were investigated on the proliferation and expression of selected markers in the T47D breast cancer cell line. We found that in contrast to the in vivo situation, in particularly the CM from M1 macrophages decreased the growth and Ki67 expression in T47D, and significantly increased ER beta 1 mRNA levels. Moreover, in accordance to the in vivo situation the CM from the macrophages decreased the expression of ER alpha protein as well as ER alpha or PR mRNA. In conclusion our results show that macrophages alone have the capability to decrease the tumor cell expression of ER alpha and PR in vitro. In the tumor environment in vivo macrophages also contribute to an increase in tumor cell expression of uPAR and Ki67, suggesting that macrophages are involved in impairing the prognosis for breast cancer patients., Funding Agencies:County Council of Värmland Karlstad University Örebro University

Published

2017

42. The Involvement of Estrogen Receptors in Astrocyte Survival

Author

Johnson, Lauren M and Johnson, Lauren M

Abstract

Estrogens are a class of hormones that are demonstrated to be neuroprotective. The levels of estrogen in the body decline during menopause which can cause a variety of symptoms. Hormone replacement therapy (HRT) is a treatment option for menopause, however, it has been demonstrated to have adverse side effects. Of the treatment options for adverse side effects of HRT, Selective estrogen Down-regulators do not appear to have an agonist effects on estrogen receptors while Selective estrogen receptor Modulators do. The aim of this study was to determine the role that estrogen receptors play in the survival of astrocytes when placed under stress with epinephrine as well as when treated with a well-known SERD. The results of this experiment indicated that treatment with estrogens did not offer any neuroprotection. Future studies should focus on differing concentrations of variables and different exposure times to further evaluate the mechanisms of estrogen signaling.

Published

2016

43. The Involvement of Estrogen Receptors in Astrocyte Survival

Author

Johnson, Lauren M and Johnson, Lauren M

Abstract

Estrogens are a class of hormones that are demonstrated to be neuroprotective. The levels of estrogen in the body decline during menopause which can cause a variety of symptoms. Hormone replacement therapy (HRT) is a treatment option for menopause, however, it has been demonstrated to have adverse side effects. Of the treatment options for adverse side effects of HRT, Selective estrogen Down-regulators do not appear to have an agonist effects on estrogen receptors while Selective estrogen receptor Modulators do. The aim of this study was to determine the role that estrogen receptors play in the survival of astrocytes when placed under stress with epinephrine as well as when treated with a well-known SERD. The results of this experiment indicated that treatment with estrogens did not offer any neuroprotection. Future studies should focus on differing concentrations of variables and different exposure times to further evaluate the mechanisms of estrogen signaling.

Published

2016

44. Fytoestrogeny a jejich vliv na lidské zdraví

Author

Korecká, Lucie, Novotná, Tereza, Korecká, Lucie, and Novotná, Tereza

Abstract

Tato bakalářská práce se věnuje fytoestrogenům. Je zde popsána jejich struktura, mechanismus účinku a biochemické vlastnosti. V této bakalářské práci jsou shrnuty nejnovější poznatky o účincích fytoestrogenů na lidské zdraví. Je popsán také jejich výskyt v potravinách a možnosti stanovení fytoestrogenů., This thesis is mainly focused on phytoestrogens, their structure, mechanism of action and their biochemistry properties. It also includes new insights on phytoestrogens affect on human health, analysis of phytoestrogens and their occurrence in food., Fakulta chemicko-technologická

Published

2016

45. Estrogen Dependent Regulation of the Amp-Activated Protein Kinase Pathway

Author

Brooks, Heddwen, Elfring, Lisa, Doetschman, Thomas, Tsao, Tsu-Shuen, Konhilas, John P., Lipovka, Yulia, Brooks, Heddwen, Elfring, Lisa, Doetschman, Thomas, Tsao, Tsu-Shuen, Konhilas, John P., and Lipovka, Yulia

Abstract

Sex differences exist in the progression of heart disease, as premenopausal women are protected from developing severe hypertension, aortic stenosis, myocardial infarction and hypertrophic cardiomyopathies. The susceptibility and progression of cardiovascular disease increases in post-menopausal women. This is at least partially underlined by a pronounced decrease in circulating estrogen levels. Estradiol (E2), the most abundant estrogen in premenopausal women, is known to be cardioprotective. Recently, AMP-activated protein kinase (AMPK) has emerged as a prominent player in the development of cardiac hypertrophy and heart failure. AMPK is central to the energetic metabolism of the cell and is activated in response to energy deprivation. E2 has been shown to activate AMPK, by yet an unknown mechanism. The first part of this dissertation focuses on describing the molecular mechanism behind this AMPK activation. We found that E2 activates AMPK through a non- genomic pathway and involves direct interaction of classical estrogen receptors (ERα and ERβ) with the α-catalytic subunit of AMPK. These receptors also associate with the upstream kinase LKB1, which is required for E2-dependent activation of AMPK. Furthermore, the two estrogen receptors play opposite roles, where ERα increases AMPK activation, and ERβ acts as a repressor, inhibiting AMPK phosphorylation. To translate our findings to heart disease, the next step was to determine the effect of ovarian failure, underlined by E2 loss, on AMPK signaling during the progression of cardiac hypertrophy. We hypothesized that ovarian failure decreases cardiac AMPK signaling, translating in worsening of hypertrophy. We found that the status of cardiac AMPK signaling depends on the nature of the hypertrophic stimulus and the timing of ovarian failure in relation to the onset of hypertrophy. Furthermore, we did not detect any differences in the development of cardiac hypertrophy between wild type mice and mice in ovarian failu

Published

2015

46. Signaling mechanisms mediating the regulation of synaptic plasticity and memory by estradiol

Author

Arévalo, María Ángeles, Azcoitia, I., González-Burgos, I., García-Segura, Luis M., Arévalo, María Ángeles, Azcoitia, I., González-Burgos, I., and García-Segura, Luis M.

Abstract

© 2015 Elsevier Inc.. This article is part of a Special Issue >Estradiol and Cognition>.Estradiol participates in the regulation of the function and plasticity of synaptic circuits in key cognitive brain regions, such as the prefrontal cortex and the hippocampus. The mechanisms elicited by estradiol are mediated by the regulation of transcriptional activity by nuclear estrogen receptors and by intracellular signaling cascades activated by estrogen receptors associated with the plasma membrane. In addition, the mechanisms include the interaction of estradiol with the signaling of other factors involved in the regulation of cognition, such as brain derived neurotrophic factor, insulin-like growth factor-1 and Wnt. Modifications in these signaling pathways by aging or by a long-lasting ovarian hormone deprivation after menopause may impair the enhancing effects of estradiol on synaptic plasticity and cognition.

Published

2015

47. Development of Coactivator-Dependent, First-in-Class Therapies for Breast Cancer

Author

BAYLOR COLL OF MEDICINE HOUSTON TX, O'Malley, Bert W, BAYLOR COLL OF MEDICINE HOUSTON TX, and O'Malley, Bert W

Abstract

By integrating multiple signaling pathways that cancer cells rely on for growth and survival, p160 steroid receptor coactivator (SRC) family members (SRC-1, SRC-2/TIF2/GRIP1, SRC- 3/AIB1/pCIP/RAC3) represent emerging targets for anti-cancer drug development. During this reporting period, we have characterized and published our work on two potent and selective small molecule inhibitors (SMIs), bufalin and verrucarin A, against SRCs from high throughput screening efforts. Cryo-electron microscopic analyses of DNA/estrogen receptor/SRC-3 protein complexes achieved by our group are providing powerful new insights into understanding the conformation of intact, full length proteins in a complex and should provide valuable new information on the mechanism of action of SRC SMIs as well., The original document contains color images.

Published

2014

48. A Drug Discovery Partnership for Personalized Breast Cancer Therapy

Author

XAVIER UNIV OF LOUISIANA NEW ORLEANS, Foroozesh, Maryam, Weise, Thomas, Sridhar, Jayalakshmi, Beckman, Barbara, Burow, Matthew, Jones, Frank, Stevens, Cheryl, XAVIER UNIV OF LOUISIANA NEW ORLEANS, Foroozesh, Maryam, Weise, Thomas, Sridhar, Jayalakshmi, Beckman, Barbara, Burow, Matthew, Jones, Frank, and Stevens, Cheryl

Abstract

Xavier University of Louisiana is in the unique position of developing capability in drug discovery especially in the areas of cancer and health disparities. A significant proportion of the funded research on Xavier s campus including collaborative projects involving Tulane University are related to cancer, drug design, synthesis, and drug delivery. This project expands the partnership between Xavier University and Tulane Cancer Center to develop and validate drugs for breast cancer therapy. The Drug Design Team at Xavier consists of experts in computer-aided drug design methods and synthesis and has formed a productive partnership with the Cancer Drug Validation Team at the Tulane Cancer Center. This inter-university collaboration involves training Xavier researchers, including undergraduate students, to carryout the experiments necessary to determine if new compounds would be suitable as new drugs to treat breast cancer. Three separate studies are ongoing as subprojects: (1) Design and synthesis of novel ceramide analogs that potentially reverse chemotherapy drug resistance, (2) Design and synthesis of small molecule inhibitors of HER2 tyrosine kinase to suppress tumorigenesis, and (3) Identification of compounds with the potential for estrogen receptor activity., The original document contains color images.

Published

2014

49. Gestational bisphenol A exposure and testis development

Author

Williams, Cecilia, Bondesson, Maria, Krementsov, Dimitry N., Teuscher, Cory, Williams, Cecilia, Bondesson, Maria, Krementsov, Dimitry N., and Teuscher, Cory

Abstract

Virtually all humans are exposed to bisphenol A (BPA). Since BPA can act as a ligand for estrogen receptors, potential hazardous effects of BPA should be evaluated in the context of endogenous estrogenic hormones. Because estrogen is metabolized in the placenta, developing fetuses are normally exposed to very low endogenous estrogen levels. BPA, on the other hand, passes through the placenta and might have distinct adverse consequences during the sensitive stages of fetal development. Testicular gametogenesis and steroidogenesis begin early during fetal development. These processes are sensitive to estrogens and play a role in determining the number of germ stem cells, sperm count, and male hormone levels in adulthood. Although studies have shown a correlation between BPA exposure and perturbed reproduction, a clear consensus has yet to be established as to whether current human gestational BPA exposure results in direct adverse effects on male genital development and reproduction. However, studies in animals and in vitro have provided direct evidence for the ability of BPA exposure to influence male reproductive development. This review discusses the current knowledge of potential effects of BPA exposure on male reproductive health and whether gestational exposure adversely affects testis development., QC 20161206

Published

2014

50. Assessment of the Prognostic and Treatment-Predictive Performance of the Combined HOXB13:IL17BR-MGI Gene Expression Signature in the Trans-ATAC Cohort

Author

GENERAL HOSPITAL CORP BOSTON MA, Sgroi, Dennis, GENERAL HOSPITAL CORP BOSTON MA, and Sgroi, Dennis

Abstract

We compared the prognostic ability of the Breast Cancer Index (BCI), Oncotype DX Recurrence Score (RS) and IHC4 for both early and late recurrence among patients with ER+, node negative (N0) disease with the ATAC clinical trial. BCI was performed from 1102 primary tumor samples from ER+ patients were evaluated. BCI-L, IHC4 and RS had significant prognostic performance for early DR (BCO-L, p0-0002), while only BCI-L was significant for late DR (LR- X2: 7-97, p=0- 0048). For risk of early DR at 5 years, BCI-L classified 59%, 25%, and 16% of patients with 1.3%, 5.6%, and 18.1% for low, intermediate and high risk, respectively. For risk of late DR at 10 years, BCI-L classified 61%, 25%, and 14% of patients., The original document contains color images.

Published

2013