Estrogen Replacement in Turner Syndrome: Literature Review and Practical Considerations

Klein, Karen Oerter; Rosenfield, Robert L.; Santen, Richard J.; Gawlik, Aneta; Backeljauw, Philippe; Gravholt, Claus Højbjerg; Sas, Theo C J; Mauras, Nelly

doi:10.1210/jc.2017-02183

Cited by 118 publications

(94 citation statements)

References 105 publications

(122 reference statements)

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“…We expected that if genotypes differed on behavioral measures, that some of the differences might disappear if they depended on group differences in levels of gonadal hormones in any life stage. However, sex- hormone replacement therapies in adulthood do not appear to remediate the cognitive deficits observed in people with KS (Fales et al, 2003; Kompus et al, 2011; Liberato et al, 2017; Skakkebæk et al, 2017) or TS (Klein et al, 2018; Ross et al, 2002, 2004), and the cognitive consequences of reducing/blocking sex hormones in people with either KS or TS, or in this animal model, are unknown.…”

Section: Introductionmentioning

confidence: 93%

“…Some effects of KS and TS are potentially attributed to altered levels of gonadal hormones. KS men have lower levels of testosterone than XY men (Gravholt et al, 2018; Klein et al, 2018), and TS women have altered ovarian function (Klein et al, 2018; Romans et al, 1998; Ross et al, 1995, 2004; Rovet, 2004). Accordingly, we analyzed the role of gonadal hormones on task performance by comparing gonadectomized mice to gonad-intact controls.…”

Section: Introductionmentioning

confidence: 99%

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Reversal learning performance in the XY* mouse model of Klinefelter and Turner Syndromes

Aarde¹,

Hrncir²,

Arnold³

et al. 2019

Preprint

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Klinefelter syndrome (KS; 47, XXY) and Turner syndrome (TS; 45, XO) are caused by two relatively common sex chromosome aneuploidies. These conditions are associated with an increased odds of neuropsychiatric disorders, including attention deficit/hyperactivity disorder (ADHD), as well as impairments in cognition that include learning delays, attentional dysfunction and impulsivity. We studied cognitive functions in the XY* mouse model, which allows comparison of XXY to XY males (KS model), and XO to XX females (TS model). We evaluated adult mice with and without gonads, using a version of an operant reversal-learning task (RLT) that can be used to measure various facets of learning, impulsivity and attention. In the KS model, only one measure related to impulsivity – perseverative responding under reversal conditions – reliably discriminated gonadally intact XXY and XY mice. In contrast, a fundamental learning impairment (more trials to criterion in acquisition phase) in XXY mice, as compared to XY, was observed in gonadectomized subjects. No other task measures showed differences consistent with KS. In the TS mouse model, XO mice did not show a pattern of results consistent with TS, similar to past observations. Thus, the application of this RLT to these XY* models reveals only limited behavioral impairments relevant to KS.

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Section: Introductionmentioning

confidence: 93%

Section: Introductionmentioning

confidence: 99%

Reversal learning performance in the XY* mouse model of Klinefelter and Turner Syndromes

Aarde¹,

Hrncir²,

Arnold³

et al. 2019

Preprint

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“…Low doses of estradiol are initiated and titrated to promote secondary sexual characteristics and uterine growth without early closure of the growth plates, ensure a normal tempo of bone mineralization (Cleemann et al, ), normalize cognitive maturation (Ross, Roeltgen, Feuillan, Kushner, & Cutler Jr., ; Ross, Roeltgen, Feuillan, Kushner, & Cutler Jr., ), body composition (Cleemann et al, ), reduce lipids (Gravholt, Naeraa, et al, ) and liver enzymes (Koulouri, Ostberg, & Conway, ) and reduce cardiovascular risk in the long term (Gravholt, Naeraa, et al, ; Ostberg et al, ). Transdermal estradiol is the preferred method for estrogen administration (Gravholt, Andersen, et al, , section 6.1; Klein et al, ), but oral estradiol can also be used. Estrogen replacement strategies for pubertal induction in girls with Turner syndrome (Gravholt, Andersen, et al, , table 5) recommend increasing the dose by 25 to 100% every 6 months to attain adult dosing over the span of 2–3 years.…”

Section: Endocrine Issuesmentioning

confidence: 99%

Recognition and management of adults with Turner syndrome: From the transition of adolescence through the senior years

Lin

Prakash

Andersen

et al. 2019

American J of Med Genetics Pt A

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Turner syndrome is recognized now as a syndrome familiar not only to pediatricians and pediatric specialists, medical geneticists, adult endocrinologists, and cardiologists, but also increasingly to primary care providers, internal medicine specialists, obstetricians, and reproductive medicine specialists. In addition, the care of women with Turner syndrome may involve social services, and various educational and neuropsychologic therapies. This article focuses on the recognition and management of Turner syndrome

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“…These patterns have been previously associated with increased breast cancer risk 30. Oestrogen given as physiologic replacement in hypogonadal girls and women is critically important for a plethora of beneficial metabolic effects, not only for mammary and female organs normal growth, but also beneficial for plasma lipids, cardiovascular health and bone, among others 7,32. In contrast, because of the rapidly changing oestrogen milieu, the levels in pubertal girls are far more variable than in prepubertal girls, making it difficult to pick up the differences in endogenous concentrations depending on adiposity as compared to girls prior to any gonadal activation.Ever being overweight in childhood increases the risk of all cause and breast cancer death later in life,31 suggesting that there are critical developmental periods when exposure to environmental factors, including genotoxic oestrogen metabolites, could significantly affect the impact of mammary cancers later in life 31.…”

mentioning

confidence: 98%

“…Ever being overweight in childhood increases the risk of all cause and breast cancer death later in life,31 suggesting that there are critical developmental periods when exposure to environmental factors, including genotoxic oestrogen metabolites, could significantly affect the impact of mammary cancers later in life 31. Oestrogen given as physiologic replacement in hypogonadal girls and women is critically important for a plethora of beneficial metabolic effects, not only for mammary and female organs normal growth, but also beneficial for plasma lipids, cardiovascular health and bone, among others 7,32. Hence, the route of administration becomes an important variable in the selection of oestrogen used as replacement.…”

mentioning

confidence: 99%

Impact of route of administration on genotoxic oestrogens concentrations using oral vs transdermal oestradiol in girls with Turner syndrome

Mauras

Torres-Santiago

Santen

et al. 2018

Clinical Endocrinology

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Objective:The established link between oestrogen and breast cancer occurs via both oestrogen receptor (ER)-mediated and non ER-mediated mechanisms. The term genotoxic estrogens describes mutagenic metabolites, including oestrogen catechols and quinones, which have been linked to breast carcinogenesis in post-menopausal women. We aimed to assess whether the route of administration of 17β oestradiol (E 2 ) affects the accumulation of genotoxic oestrogen metabolites in a model of ovarian failure in young girls with Turner syndrome.Methods: Stored plasma samples obtained at 0 and 12 months were used from 40 adolescents with Turner syndrome who participated in a 12 months randomized controlled trial of the metabolic impact of E 2 orally (2 mg/d) vs transdermally (100 µg/d);dose escalation allowed matching of unconjugated E 2 levels in the parent study. We measured 12 oestrogen metabolites (total concentrations = conjugated and unconjugated) using a highly sensitive LCMSMS assay. Results from 48 normally menstruating adolescents were used for comparison. Results: After treatment, least square mean (SE) total E 2 concentrations were higher in the oral vs transdermal group (6784 pmol/L vs 1123 [1614], P < 0.0001), as was oestrone (E 1 ) (91 060 pmol/L vs 19 278 [16 534], P < 0.0001). Also, higher after oral treatment were catechol-oestrogens 4-hydroxy-E 2 (149 vs 28 [±49] pmol/L), 2-hydroxy-E 2 (300 vs 76 [±52]), 4-hydroxy-E 1 (450 vs 105 [±113]), 2-hydroxy-E 1 (3094 vs 740 [±684]) and 16α-hydroxy-E 1 (3,007 vs 157 [±534]) (<0.001 between groups). Levels were much closer to controls in the transdermal group. Conclusions: Common feminizing doses of oral oestradiol for 12 months result in substantial accumulation of unphysiologic, genotoxic oestrogens compared to transdermal oestradiol, expanding concerns about oral oestrogens' first hepatic passage.Further studies assessing long-term risks of these metabolites in women taking different forms of oestrogen are needed. K E Y W O R D Sbreast cancer, children, genotoxic oestrogens, LCMSMS assay, oestradiol, transdermal, Turner syndrome

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Estrogen Replacement in Turner Syndrome: Literature Review and Practical Considerations

Cited by 118 publications

References 105 publications

Reversal learning performance in the XY* mouse model of Klinefelter and Turner Syndromes

Reversal learning performance in the XY* mouse model of Klinefelter and Turner Syndromes

Recognition and management of adults with Turner syndrome: From the transition of adolescence through the senior years

Impact of route of administration on genotoxic oestrogens concentrations using oral vs transdermal oestradiol in girls with Turner syndrome

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