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Primary ovarian insufficiency

January 01, 1970

Primary ovarian insufficiency (POI), also called premature ovarian insufficiency, premature menopause, and premature ovarian failure, is the partial or total loss of reproductive and hormonal function of the ovaries before age 40 because of follicular (egg producing area) dysfunction or early loss of eggs.[1][4][6] POI can be seen as part of a continuum of changes leading to menopause[7] that differ from age-appropriate menopause in the age of onset, degree of symptoms, and sporadic return to normal ovarian function.[8] POI affects approximately 1 in 10,000 women under age 20, 1 in 1,000 women under age 30, and 1 in 100 of those under age 40.[6] A medical triad for the diagnosis is amenorrhea, hypergonadotropism, and hypoestrogenism.[5]

Primary ovarian insufficiency[1][2]
Other namesPremature ovarian insufficiency,[3] premature menopause,[1][4] and premature ovarian failure.[5]
SpecialtyObstetrics and gynecology

Physical and emotional symptoms are similar to those seen during menopause and can include hot flashes, night sweats, dry skin, vaginal dryness, irregular or absent menstruation, anxiety, depression, mental fog, irritability, nervousness, decreased libido, and increased autoimmune disruption.[9] The sense of shock and distress on being informed of the diagnosis can be overwhelming.[1] Hormonal therapy with estrogen and progesterone is the first line treatment and is associated with improvement of symptoms and possibly improvement in other parameters such as bone density, mortality and cardiovascular risk.[10] The general treatment is for symptoms, bone protection, and mental health.[1][11] Although 5 to 10% of women with POI may ovulate sporadically and become pregnant without treatment,[12] others may use assisted reproductive technology including in vitro fertilization and egg donation[13] or decide to adopt or remain childless.[14]

The causes of POI are heterogeneous and are unknown in 90% of cases.[6] It can be associated with genetic causes, autoimmune disease, enzyme deficiency, infection, environmental factors, radiation, or surgery in 10%.[15] Two to 5% of women with POI and a premutation in FMR1, a genetic abnormality, are at risk of having a child with fragile X syndrome, the most common cause of inherited intellectual disability.[8][6]

The diagnosis is based on ages less than 40, amenorrhea, and elevated serum follicle-stimulating hormone (FSH) levels.[4] Typical serum FSH levels in POI patients is in the post-menopausal range.[2] Treatment will vary depending on the symptoms. It can include hormone replacement therapy, fertility management, and psychosocial support, as well as annual screenings of thyroid and adrenal function.[16]

Signs and symptoms edit

The signs and symptoms of POI can be seen as part of a continuum of changes leading to menopause.[7] POI contrasts with age-appropriate menopause in the age of onset, degree of symptoms and sporadic return to normal ovarian function.[8] As some women retain partial ovarian function, symptoms may not be as severe as regular menopause.[8] In others, particularly with coexistent depression, symptoms such as decreased quality of life can be severe.[9]

Hormonally, POI is defined by abnormally low levels of estrogen and high levels of FSH, which demonstrate that the ovaries are no longer responding to circulating FSH by producing estrogen and developing fertile eggs. The ovaries will likely appear smaller than normal.[medical citation needed] The age of onset can be as early as 11 years.[17] POI can be seen as part of a continuum of changes leading to menopause[7] that differ from age-appropriate menopause in the age of onset, degree of symptoms, and sporadic return to normal ovarian function.[8] A contrasting problem can be when a girl never begins menstruation due to a genetic condition causing primary amenorrhea.[15]

Causes edit

Genetic associations[18]
Type OMIM Gene Locus
POF1 311360 FMR1 Xq26-q28
POF2A 300511 DIAPH2 Xq13.3-q21.1
POF2B 300604 POF1B Xq13.3-q21.1
POF3 608996 FOXL2 3q23
POF4 300510 BMP15 Xp11.2
POF5 611548 NOBOX 7q35
POF6 612310 FIGLA 2p12
POF7 612964 NR5A1 9q33

The cause of POI is idiopathic in 39-67% of cases.[10] Some cases of POI are attributed to autoimmune disorders such as autoimmune oophoritis,[19] Hashimoto thyroiditis, Addison disease, type I diabetes mellitus, pernicious anemia, genetic disorders such as Turner syndrome and Fragile X syndrome, metabolic defects, and enzyme defects.[15] One study showed a strong correlation between incidence of POI and certain variants in the inhibin alpha gene.[20] Chemotherapy and radiation treatments (especially radiation to the pelvis) for cancer can sometimes cause POI. The effect of chemotherapy or radiation is variable and in a mouse model, with results consistent with observations in humans, cyclophosphamide can result in an 87% reduction in primordial follicles 72 hours after administration.[15] Women who have had a hysterectomy tend to go through menopause early and have a nearly twofold increased risk of POI.[15] Almost any pelvic surgery has the potential to damage the ovary by affecting its blood supply or causing inflammation in the area resulting in POI, especially surgery to the ovaries themselves (e.g. for treatment of ovarian cysts or endometriosis).[15][10] Certain environmental toxins such as phthalates, bisphenols, and dioxins are also associated with POI.[10] Certain infectious diseases, such as mumps or HIV may also damage the ovaries, leading to POI.[10]

Galactosemia edit

Women who have inherited classic galactosemia (galactose intolerance) may develop primary ovarian insufficiency.[21]

Mechanism edit

The pathogenic mechanisms of POI are highly heterogeneous and can be divided into four major categories: follicular migration defect early in embryogenesis; an early decrease in the primordial follicles; increased follicular death; and altered maturation or recruitment of primordial follicles.[15] These result in a decrease of the ovaries' general supply of eggs that normally lasts until an average age of 51 for age of age-appropriate menopause.[22]

Genetic causes such as Turner syndrome have initial ovarian development but then ovaries degenerate rapidly during prenatal life, often leading to gonadal dysgenesis with streak ovaries. In those cases where POI is associated with adrenal autoimmunity, histological examination almost always confirms the presence of an autoimmune oophoritis in which follicles are infiltrated by lymphocytes, plasma cells, and macrophages that attack mainly steroid-producing cells and eventually result in follicular depletion.[15]

In some women FSH may bind to the FSH receptor site, but be inactive. By lowering the endogenous FSH levels with ethinylestradiol (EE) or with a GnRH-a the receptor sites are free and treatment with exogenous recombinant FSH activates the receptors and normal follicle growth and ovulation can occur.[23][24] (Since the serum Anti-Müllerian hormone (AMH) level is correlated with the number of remaining primordial follicles some researchers believe the above two phenotypes can be distinguished by measuring serum AMH levels.[25]

Genetic associations include genetic disorders,[8] autoimmune diseases,[3] enzyme defects,[15] and resistant ovaries.[8]

Mutations in FOXL2 cause blepharophimosis, ptosis, epicanthus inversus syndrome (BPES). Premature ovarian failure is part of the BPES Type I variant of the syndrome but not of the BPES Type II variant.[26]

DNA repair deficiency edit

BRCA1 protein plays an essential role in the repair of DNA double-strand breaks by homologous recombination. Women with a germline BRCA1 mutation tend to have premature menopause as evidenced by the final amenorrhea appearing at a younger age.[27] BRCA1 mutations are associated with occult POI.[28] Impairment of the repair of DNA double-strand breaks due to a BRCA1 defect leads to premature ovarian aging in both mice and humans.[29]

In addition to BRCA1, the MCM8-MCM9 protein complex also plays a crucial role in the recombinational repair of DNA double-strand breaks.[30] In humans, an MCM8 mutation can give rise to premature ovarian failure, as well as chromosomal instability.[31] MCM9, as well as MCM8, mutations are also associated with ovarian failure and chromosomal instability.[32][33] The MCM8-MCM9 complex is likely required for the homologous recombinational repair of DNA double-strand breaks that are present during the pachytene stage of meiosis I. In women homozygous for MCM8 or MCM9 mutations, failure to repair breaks apparently leads to oocyte death and small or absent ovaries.[31][32]

Diagnosis edit

The diagnosis is based on age less than forty, amenorrhea, and two elevated serum follicle-stimulating hormone (FSH) and decreased estrogen measurements at one-month intervals.[10] The anterior pituitary secretes FSH and LH at high levels to try to increase the low estrogen levels that are due to the dysfunction of the ovaries. Typical FSH in POI patients is over 40 mlU/ml (post-menopausal range).[2] The evaluation of amenorrhea for other common causes includes checking a blood pregnancy test, checking the prolactin level, as prolactinomas or certain medications can increase prolactin levels and lead to amenorrhea, and checking the thyrotropin (thyroid hormone) level, as hypothyroidism can cause amenorrhea.[10] A karyotype (to evaluate for Turner's Syndrome) and a Fragile-X premutation carrier analysis is also recommended, with additional genetic testing possibly being warranted based on family history of amenorrhea or early menopause or signs and symptoms of a genetic disorder.[10]

Treatment edit

Fertility edit

Between 5 and 10 percent of women with POI may become pregnant with no treatment.[12] As of 2016 no fertility treatment has been found to effectively increase fertility in women with POI, and the use of donor eggs with in-vitro fertilization (IVF) and adoption are a means of achieving parenthood for women with POI.[13] Some women with POI choose to live child-free.[14]

Researchers have investigated the use of a hormone called dehydroepiandrosterone (DHEA) in women with POI to increase spontaneous pregnancy rates.[34][35] Results from studies on DHEA in 2010 indicated that DHEA may increase spontaneously conceived pregnancies, decrease spontaneous miscarriage rates and improve IVF success rates in women with POI.[36] This includes women referred for donor eggs or surrogacy in 2009.[37] In 2018, there was no significant improvement in ovarian function by 12-month on DHEA supplementation in women with POI.[35] Given the inconclusiveness of potential benefits and risks of testosterone and DHEA supplementation, longer-term, randomized studies are warranted for women and girls with POI.[38]

Ovarian tissue cryopreservation can be performed on prepubertal girls at risk for premature ovarian failure, and this procedure is as feasible and safe as comparable operative procedures in children.[39]

In 2013, Kawamura in Japan and his collaborators at Stanford University published treatment of infertility of POI patients by fragmenting ovaries followed by in vitro treatment of ovarian fragments with phosphatidylinositol-3 kinase activators to enhance the AKT pathway followed by autografting. They successfully promoted follicle growth, retrieved mature oocytes, and performed in vitro fertilization. Following embryo transfer, a healthy baby was delivered.[40][41] A 2020 review covered variations including phosphatidylinositol-3 kinase activators to enhance the AKT pathway, fragmentation of ovarian cortex, combining those two into in-vitro activation (IVA), and drug-free IVA. Two laparoscopies are needed in conventional IVA and one with drug-free IVA.[40]

Hormonal replacement edit

Women with POI can develop symptoms of estrogen deficiency, including vasomotor flushes and vaginal dryness that respond to physiologic replacement of hormones.[9][4] Most authorities recommend that this hormone replacement continue until age 50 years, the normal age of menopause. The leading hormone replacement regimen recommended involves the administration of estradiol daily by either skin patch or vaginal ring. This approach reduces the risk of pulmonary embolism and deep venous thrombosis by avoiding the first pass effect on the liver that is induced by oral estrogen therapy.[4][42] The transdermal estradiol patch also provides the replacement by steady infusion rather than by bolus when taking daily pills.[42]

Concerns of estrogen supplement are addressed in The US Medical Eligibility Criteria for Contraceptive Use, 2010 provides guidance for safety of contraceptive methods and include guidance for conditions associated with increased risk of thrombosis such as postpartum, history of thrombosis, thrombogenic mutations, systemic lupus erythematosus, diabetes, and hypertension.[43] There is also an increased risk with valvular heart disease and cardiomyopathy.[44]

To avoid the development of endometrial cancer young women taking estradiol replacement need also to take a progestin in a regular cyclic fashion. The most evidence supports the use of medroxyprogesterone acetate per day for days one through 12 of each calendar month. This will induce regular and predictable menstrual cycles. It is important that women taking this regimen keep a menstrual calendar. If the next expected menses is late it is important to get a pregnancy test. It this is positive, the woman should stop taking the hormone replacement. Approximately 5 to 10% of women with confirmed POI conceive a pregnancy after the diagnosis without medical intervention.[4]

In observational studies, hormone replacement therapy in women with primary ovarian insufficiency and other causes of early menopause was associated with a lower risk of cardiovascular disease, increased bone density, and a reduced mortality.[10]

Prognosis edit

Primary ovarian insufficiency is associated with co-morbidities associated with menopause including osteoporosis (decreased bone density), which affects almost all women with POI due to an insufficiency of estrogen. There is also an increased risk of heart disease,[8] hypothyroidism such as Hashimoto's thyroiditis, Addison's disease, and other autoimmune disorders.[45]

Emotional health edit

The most common words women use to describe how they felt in the two hours after being given the diagnosis of POI are "devastated", "shocked," and "confused."[1][46] The diagnosis is more than infertility and affects a woman's physical and emotional well-being.[4] Patients face the acute shock of the diagnosis, associated stigma of infertility, grief from the death of dreams, anxiety and depression from the disruption of life plans, confusion around the cause, shame, insecurity and lowered self-esteem, anger in reflection of being letdown by the medical system, symptoms of estrogen deficiency, worry over the associated potential medical sequelae such as reduced bone density and cardiovascular risk, and the uncertain future that all of these factors create.[1][4][6] Women diagnosed with POI in their 20s have disproportionately reported experiencing dismissiveness, bias, and "not being taken seriously" by healthcare professionals.[47]

Some have advocated formation of a patient registry as well as a community-based research consortium with integrative care to better understand the etiology and treatment of the condition, including treatment of its psychological effects.[7] Women with POI perceive lower social support than control women, so building a trusted community of practice for them would be expected to improve their well-being. Also, when having that social support, it often helps with reducing stress and having better coping skills.[47][48][49][50] It is important to connect women with POI to an appropriate collaborative care team because the condition has been clearly associated with suicide related to the stigma of infertility.[49] Suicide rates are known to be increased in women who experience infertility.[51]

Epidemiology edit

The prevalence increases with age and is approximately 1 in 10,000 women under age 20, 1 in 1,000 women under age 30, and one percent by age of 40.[6][52] It occurs in 3.7% of women worldwide and 1% of women in the United States. In the United States, the incidence is 1% in White women, 1.4% in Black and Hispanic women, with lower rates seen in Chinese and Japanese women, at 0.5% and 0.1% respectively.[10]

History edit

Fuller Albright et al. in 1942 reported a syndrome with amenorrhea, estrogen deficiency, menopausal FSH levels, and short stature. They used the term "primary ovarian insufficiency" to distinguished POI from ovarian insufficiency secondary to a primary failure of pituitary FSH and other hormonal secretion.[53][54] POI has been described as a more accurate and less stigmatizing term than premature ovarian failure[4] or premature menopause.[4][11]

Chapter 28 of the early Qing dynasty work Fù Qīngzhǔ Nǚkē (《傅青主女科》Fù Qīngzhǔ's Gynecology) describes the cause and appropriate treatment for premature menopause. 年未老经水断 (niánwèilǎo jīngshuǐduàn) glosses as 'not yet old, menstrual water cut-off.'[55]

References edit

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  53. ^ Hubayter ZR, Popat V, Vanderhoof VH, Ndubizu O, Johnson D, Mao E, et al. (October 2010). "A prospective evaluation of antral follicle function in women with 46,XX spontaneous primary ovarian insufficiency". Fertility and Sterility. 94 (5): 1769–74. doi:10.1016/j.fertnstert.2009.10.023. PMC 2888894. PMID 19939372.
  54. ^ Albright F, Smith PH, Fraser R (1941). "A syndrome characterized by primary ovarian insufficiency and decreased stature: report of 11 cases with a digression on hormonal control of axillary and pubic hair". Am J Med Sci. 204: 625–48. doi:10.1097/00000441-194211000-00001. S2CID 59095440.
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External links edit

  • Primary Ovarian Insufficiency (POI): Overview National Institutes of Health

January 01, 1970
primary, ovarian, insufficiency, also, called, premature, ovarian, insufficiency, premature, menopause, premature, ovarian, failure, partial, total, loss, reproductive, hormonal, function, ovaries, before, because, follicular, producing, area, dysfunction, ear. Primary ovarian insufficiency POI also called premature ovarian insufficiency premature menopause and premature ovarian failure is the partial or total loss of reproductive and hormonal function of the ovaries before age 40 because of follicular egg producing area dysfunction or early loss of eggs 1 4 6 POI can be seen as part of a continuum of changes leading to menopause 7 that differ from age appropriate menopause in the age of onset degree of symptoms and sporadic return to normal ovarian function 8 POI affects approximately 1 in 10 000 women under age 20 1 in 1 000 women under age 30 and 1 in 100 of those under age 40 6 A medical triad for the diagnosis is amenorrhea hypergonadotropism and hypoestrogenism 5 Primary ovarian insufficiency 1 2 Other namesPremature ovarian insufficiency 3 premature menopause 1 4 and premature ovarian failure 5 SpecialtyObstetrics and gynecology Physical and emotional symptoms are similar to those seen during menopause and can include hot flashes night sweats dry skin vaginal dryness irregular or absent menstruation anxiety depression mental fog irritability nervousness decreased libido and increased autoimmune disruption 9 The sense of shock and distress on being informed of the diagnosis can be overwhelming 1 Hormonal therapy with estrogen and progesterone is the first line treatment and is associated with improvement of symptoms and possibly improvement in other parameters such as bone density mortality and cardiovascular risk 10 The general treatment is for symptoms bone protection and mental health 1 11 Although 5 to 10 of women with POI may ovulate sporadically and become pregnant without treatment 12 others may use assisted reproductive technology including in vitro fertilization and egg donation 13 or decide to adopt or remain childless 14 The causes of POI are heterogeneous and are unknown in 90 of cases 6 It can be associated with genetic causes autoimmune disease enzyme deficiency infection environmental factors radiation or surgery in 10 15 Two to 5 of women with POI and a premutation in FMR1 a genetic abnormality are at risk of having a child with fragile X syndrome the most common cause of inherited intellectual disability 8 6 The diagnosis is based on ages less than 40 amenorrhea and elevated serum follicle stimulating hormone FSH levels 4 Typical serum FSH levels in POI patients is in the post menopausal range 2 Treatment will vary depending on the symptoms It can include hormone replacement therapy fertility management and psychosocial support as well as annual screenings of thyroid and adrenal function 16 Contents 1 Signs and symptoms 2 Causes 2 1 Galactosemia 3 Mechanism 3 1 DNA repair deficiency 4 Diagnosis 5 Treatment 5 1 Fertility 5 2 Hormonal replacement 6 Prognosis 6 1 Emotional health 7 Epidemiology 8 History 9 References 10 External linksSigns and symptoms editThe signs and symptoms of POI can be seen as part of a continuum of changes leading to menopause 7 POI contrasts with age appropriate menopause in the age of onset degree of symptoms and sporadic return to normal ovarian function 8 As some women retain partial ovarian function symptoms may not be as severe as regular menopause 8 In others particularly with coexistent depression symptoms such as decreased quality of life can be severe 9 Hormonally POI is defined by abnormally low levels of estrogen and high levels of FSH which demonstrate that the ovaries are no longer responding to circulating FSH by producing estrogen and developing fertile eggs The ovaries will likely appear smaller than normal medical citation needed The age of onset can be as early as 11 years 17 POI can be seen as part of a continuum of changes leading to menopause 7 that differ from age appropriate menopause in the age of onset degree of symptoms and sporadic return to normal ovarian function 8 A contrasting problem can be when a girl never begins menstruation due to a genetic condition causing primary amenorrhea 15 Causes editGenetic associations 18 Type OMIM Gene Locus POF1 311360 FMR1 Xq26 q28 POF2A 300511 DIAPH2 Xq13 3 q21 1 POF2B 300604 POF1B Xq13 3 q21 1 POF3 608996 FOXL2 3q23 POF4 300510 BMP15 Xp11 2 POF5 611548 NOBOX 7q35 POF6 612310 FIGLA 2p12 POF7 612964 NR5A1 9q33 The cause of POI is idiopathic in 39 67 of cases 10 Some cases of POI are attributed to autoimmune disorders such as autoimmune oophoritis 19 Hashimoto thyroiditis Addison disease type I diabetes mellitus pernicious anemia genetic disorders such as Turner syndrome and Fragile X syndrome metabolic defects and enzyme defects 15 One study showed a strong correlation between incidence of POI and certain variants in the inhibin alpha gene 20 Chemotherapy and radiation treatments especially radiation to the pelvis for cancer can sometimes cause POI The effect of chemotherapy or radiation is variable and in a mouse model with results consistent with observations in humans cyclophosphamide can result in an 87 reduction in primordial follicles 72 hours after administration 15 Women who have had a hysterectomy tend to go through menopause early and have a nearly twofold increased risk of POI 15 Almost any pelvic surgery has the potential to damage the ovary by affecting its blood supply or causing inflammation in the area resulting in POI especially surgery to the ovaries themselves e g for treatment of ovarian cysts or endometriosis 15 10 Certain environmental toxins such as phthalates bisphenols and dioxins are also associated with POI 10 Certain infectious diseases such as mumps or HIV may also damage the ovaries leading to POI 10 Galactosemia edit Women who have inherited classic galactosemia galactose intolerance may develop primary ovarian insufficiency 21 Mechanism editThe pathogenic mechanisms of POI are highly heterogeneous and can be divided into four major categories follicular migration defect early in embryogenesis an early decrease in the primordial follicles increased follicular death and altered maturation or recruitment of primordial follicles 15 These result in a decrease of the ovaries general supply of eggs that normally lasts until an average age of 51 for age of age appropriate menopause 22 Genetic causes such as Turner syndrome have initial ovarian development but then ovaries degenerate rapidly during prenatal life often leading to gonadal dysgenesis with streak ovaries In those cases where POI is associated with adrenal autoimmunity histological examination almost always confirms the presence of an autoimmune oophoritis in which follicles are infiltrated by lymphocytes plasma cells and macrophages that attack mainly steroid producing cells and eventually result in follicular depletion 15 In some women FSH may bind to the FSH receptor site but be inactive By lowering the endogenous FSH levels with ethinylestradiol EE or with a GnRH a the receptor sites are free and treatment with exogenous recombinant FSH activates the receptors and normal follicle growth and ovulation can occur 23 24 Since the serum Anti Mullerian hormone AMH level is correlated with the number of remaining primordial follicles some researchers believe the above two phenotypes can be distinguished by measuring serum AMH levels 25 Genetic associations include genetic disorders 8 autoimmune diseases 3 enzyme defects 15 and resistant ovaries 8 Mutations in FOXL2 cause blepharophimosis ptosis epicanthus inversus syndrome BPES Premature ovarian failure is part of the BPES Type I variant of the syndrome but not of the BPES Type II variant 26 DNA repair deficiency edit BRCA1 protein plays an essential role in the repair of DNA double strand breaks by homologous recombination Women with a germline BRCA1 mutation tend to have premature menopause as evidenced by the final amenorrhea appearing at a younger age 27 BRCA1 mutations are associated with occult POI 28 Impairment of the repair of DNA double strand breaks due to a BRCA1 defect leads to premature ovarian aging in both mice and humans 29 In addition to BRCA1 the MCM8 MCM9 protein complex also plays a crucial role in the recombinational repair of DNA double strand breaks 30 In humans an MCM8 mutation can give rise to premature ovarian failure as well as chromosomal instability 31 MCM9 as well as MCM8 mutations are also associated with ovarian failure and chromosomal instability 32 33 The MCM8 MCM9 complex is likely required for the homologous recombinational repair of DNA double strand breaks that are present during the pachytene stage of meiosis I In women homozygous for MCM8 or MCM9 mutations failure to repair breaks apparently leads to oocyte death and small or absent ovaries 31 32 Diagnosis editThe diagnosis is based on age less than forty amenorrhea and two elevated serum follicle stimulating hormone FSH and decreased estrogen measurements at one month intervals 10 The anterior pituitary secretes FSH and LH at high levels to try to increase the low estrogen levels that are due to the dysfunction of the ovaries Typical FSH in POI patients is over 40 mlU ml post menopausal range 2 The evaluation of amenorrhea for other common causes includes checking a blood pregnancy test checking the prolactin level as prolactinomas or certain medications can increase prolactin levels and lead to amenorrhea and checking the thyrotropin thyroid hormone level as hypothyroidism can cause amenorrhea 10 A karyotype to evaluate for Turner s Syndrome and a Fragile X premutation carrier analysis is also recommended with additional genetic testing possibly being warranted based on family history of amenorrhea or early menopause or signs and symptoms of a genetic disorder 10 Treatment editFertility edit Between 5 and 10 percent of women with POI may become pregnant with no treatment 12 As of 2016 no fertility treatment has been found to effectively increase fertility in women with POI and the use of donor eggs with in vitro fertilization IVF and adoption are a means of achieving parenthood for women with POI 13 Some women with POI choose to live child free 14 Researchers have investigated the use of a hormone called dehydroepiandrosterone DHEA in women with POI to increase spontaneous pregnancy rates 34 35 Results from studies on DHEA in 2010 indicated that DHEA may increase spontaneously conceived pregnancies decrease spontaneous miscarriage rates and improve IVF success rates in women with POI 36 This includes women referred for donor eggs or surrogacy in 2009 37 In 2018 there was no significant improvement in ovarian function by 12 month on DHEA supplementation in women with POI 35 Given the inconclusiveness of potential benefits and risks of testosterone and DHEA supplementation longer term randomized studies are warranted for women and girls with POI 38 Ovarian tissue cryopreservation can be performed on prepubertal girls at risk for premature ovarian failure and this procedure is as feasible and safe as comparable operative procedures in children 39 In 2013 Kawamura in Japan and his collaborators at Stanford University published treatment of infertility of POI patients by fragmenting ovaries followed by in vitro treatment of ovarian fragments with phosphatidylinositol 3 kinase activators to enhance the AKT pathway followed by autografting They successfully promoted follicle growth retrieved mature oocytes and performed in vitro fertilization Following embryo transfer a healthy baby was delivered 40 41 A 2020 review covered variations including phosphatidylinositol 3 kinase activators to enhance the AKT pathway fragmentation of ovarian cortex combining those two into in vitro activation IVA and drug free IVA Two laparoscopies are needed in conventional IVA and one with drug free IVA 40 Hormonal replacement edit Women with POI can develop symptoms of estrogen deficiency including vasomotor flushes and vaginal dryness that respond to physiologic replacement of hormones 9 4 Most authorities recommend that this hormone replacement continue until age 50 years the normal age of menopause The leading hormone replacement regimen recommended involves the administration of estradiol daily by either skin patch or vaginal ring This approach reduces the risk of pulmonary embolism and deep venous thrombosis by avoiding the first pass effect on the liver that is induced by oral estrogen therapy 4 42 The transdermal estradiol patch also provides the replacement by steady infusion rather than by bolus when taking daily pills 42 Concerns of estrogen supplement are addressed in The US Medical Eligibility Criteria for Contraceptive Use 2010 provides guidance for safety of contraceptive methods and include guidance for conditions associated with increased risk of thrombosis such as postpartum history of thrombosis thrombogenic mutations systemic lupus erythematosus diabetes and hypertension 43 There is also an increased risk with valvular heart disease and cardiomyopathy 44 To avoid the development of endometrial cancer young women taking estradiol replacement need also to take a progestin in a regular cyclic fashion The most evidence supports the use of medroxyprogesterone acetate per day for days one through 12 of each calendar month This will induce regular and predictable menstrual cycles It is important that women taking this regimen keep a menstrual calendar If the next expected menses is late it is important to get a pregnancy test It this is positive the woman should stop taking the hormone replacement Approximately 5 to 10 of women with confirmed POI conceive a pregnancy after the diagnosis without medical intervention 4 In observational studies hormone replacement therapy in women with primary ovarian insufficiency and other causes of early menopause was associated with a lower risk of cardiovascular disease increased bone density and a reduced mortality 10 Prognosis editPrimary ovarian insufficiency is associated with co morbidities associated with menopause including osteoporosis decreased bone density which affects almost all women with POI due to an insufficiency of estrogen There is also an increased risk of heart disease 8 hypothyroidism such as Hashimoto s thyroiditis Addison s disease and other autoimmune disorders 45 Emotional health edit The most common words women use to describe how they felt in the two hours after being given the diagnosis of POI are devastated shocked and confused 1 46 The diagnosis is more than infertility and affects a woman s physical and emotional well being 4 Patients face the acute shock of the diagnosis associated stigma of infertility grief from the death of dreams anxiety and depression from the disruption of life plans confusion around the cause shame insecurity and lowered self esteem anger in reflection of being letdown by the medical system symptoms of estrogen deficiency worry over the associated potential medical sequelae such as reduced bone density and cardiovascular risk and the uncertain future that all of these factors create 1 4 6 Women diagnosed with POI in their 20s have disproportionately reported experiencing dismissiveness bias and not being taken seriously by healthcare professionals 47 Some have advocated formation of a patient registry as well as a community based research consortium with integrative care to better understand the etiology and treatment of the condition including treatment of its psychological effects 7 Women with POI perceive lower social support than control women so building a trusted community of practice for them would be expected to improve their well being Also when having that social support it often helps with reducing stress and having better coping skills 47 48 49 50 It is important to connect women with POI to an appropriate collaborative care team because the condition has been clearly associated with suicide related to the stigma of infertility 49 Suicide rates are known to be increased in women who experience infertility 51 Epidemiology editThe prevalence increases with age and is approximately 1 in 10 000 women under age 20 1 in 1 000 women under age 30 and one percent by age of 40 6 52 It occurs in 3 7 of women worldwide and 1 of women in the United States In the United States the incidence is 1 in White women 1 4 in Black and Hispanic women with lower rates seen in Chinese and Japanese women at 0 5 and 0 1 respectively 10 History editFuller Albright et al in 1942 reported a syndrome with amenorrhea estrogen deficiency menopausal FSH levels and short stature They used the term primary ovarian insufficiency to distinguished POI from ovarian insufficiency secondary to a primary failure of pituitary FSH and other hormonal secretion 53 54 POI has been described as a more accurate and less stigmatizing term than premature ovarian failure 4 or premature menopause 4 11 Chapter 28 of the early Qing dynasty work Fu Qingzhǔ Nǚke 傅青主女科 Fu Qingzhǔ s Gynecology describes the cause and appropriate treatment for premature menopause 年未老经水断 nianweilǎo jingshuǐduan glosses as not yet old menstrual water cut off 55 References edit a b c d e f g Santoro NF Cooper AR 2016 Santoro NF Cooper AR eds Primary Ovarian Insufficiency A Clinical Guide to Early Menopause Springer pp i 207 doi 10 1007 978 3 319 22491 6 ISBN 978 3 319 22490 9 Each scientific chapter begins with a clinical vignette 1 I almost fell out of my chair 2 I could not stop crying 3 I felt like an old woman 4 Great More bad news 5 just see what happened and hope 6 You push yourself through the fog that is in your head 7 I was shocked Considering I was only 28 years old 8 She is overwhelmed and distraught 9 Despite this devastation 10 some women have more pronounced mood responses to hormonal changes than others 11 could a scientist create more lt eggs gt from a skin biopsy Surely this kind of technology should exist somewhere and 12 night sweats severe sleep disturbance dry eyes and memory loss a b c Pastore LM Christianson MS Stelling J Kearnsa WG Segars JH January 2018 Reproductive ovarian testing and the alphabet soup of diagnoses DOR POI POF POR and FOR Journal of Assisted Reproduction and Genetics 35 1 17 23 doi 10 1007 s10815 017 1058 4 PMC 5758472 PMID 28971280 a b Kirshenbaum M Orvieto R November 2019 Premature ovarian insufficiency POI and autoimmunity an update appraisal Journal of Assisted Reproduction and Genetics 36 11 2207 2215 doi 10 1007 s10815 019 01572 0 PMC 6885484 PMID 31440958 a b c d e f g h i j Nelson LM February 2009 Clinical practice Primary ovarian insufficiency The New England Journal of Medicine 360 6 606 14 doi 10 1056 NEJMcp0808697 PMC 2762081 PMID 19196677 a b Zhang C March 2019 The roles of different stem cells on premature ovarian failure Current Stem Cell Research amp Therapy 15 6 473 481 doi 10 2174 1574888X14666190314123006 PMID 30868961 S2CID 76665931 a b c d e f Martin LA Porter AG Pelligrini VA Schnatz PF Jiang X Kleinstreuer N et al March 2017 A design thinking approach to primary ovarian insufficiency Panminerva Medica 59 1 15 32 doi 10 23736 S0031 0808 16 03259 6 PMID 27827529 a b c d Cooper AR Baker VL Sterling EW Ryan ME Woodruff TK Nelson LM May 2011 The time is now for a new approach to primary ovarian insufficiency Fertility and Sterility 95 6 1890 7 doi 10 1016 j fertnstert 2010 01 016 PMC 2991394 PMID 20188353 a b c d e f g h Eckhardt S Wellons M 2016 Chapter 1 Defining Menopause What Is Early What Is Late In Santoro NF Cooper AR eds Primary Ovarian Insufficiency A Clinical Guide to Early Menopause Springer pp 1 17 doi 10 1007 978 3 319 22491 6 ISBN 978 3 319 22490 9 a b c Allshouse AA Semple AL 2016 Chapter 3 Signs and Symptoms of Primary Ovarian Insufficiency In Santoro NF Cooper AR eds Primary Ovarian Insufficiency A Clinical Guide to Early Menopause Springer pp 40 49 doi 10 1007 978 3 319 22491 6 ISBN 978 3 319 22490 9 a b c d e f g h i j Stuenkel Cynthia A Gompel Anne 12 January 2023 Primary Ovarian Insufficiency New England Journal of Medicine 388 2 154 163 doi 10 1056 NEJMcp2116488 PMID 36630623 a b Welt CK April 2008 Primary ovarian insufficiency a more accurate term for premature ovarian failure Clinical Endocrinology 68 4 499 509 doi 10 1111 j 1365 2265 2007 03073 x PMID 17970776 S2CID 21359408 a b van Kasteren YM Schoemaker J 1999 Premature ovarian failure a systematic review on therapeutic interventions to restore ovarian function and achieve pregnancy Human Reproduction Update 5 5 483 92 doi 10 1093 humupd 5 5 483 PMID 10582785 a b Ikhena DE Robins JC 2016 Chapter 8 IVF and Egg Donation Special Considerations In Santoro NF Cooper AR eds Primary Ovarian Insufficiency A Clinical Guide to Early Menopause Springer pp 125 136 doi 10 1007 978 3 319 22491 6 ISBN 978 3 319 22490 9 a b Bevilacqua B 2016 Chapter 10 Primary Ovarian Insufficiency POI and Mood Disorders In Santoro NF Cooper AR eds Primary Ovarian Insufficiency A Clinical Guide to Early Menopause Springer pp 145 138 doi 10 1007 978 3 319 22491 6 ISBN 978 3 319 22490 9 a b c d e f g h i Foyouzi N Green LJ Camper SA 2016 Chapter 2 Etiologies of Primary Ovarian Insufficiency In Santoro NF Cooper AR eds Primary Ovarian Insufficiency A Clinical Guide to Early Menopause Springer pp 19 35 doi 10 1007 978 3 319 22491 6 ISBN 978 3 319 22490 9 Tiosano D Mears JA Buchner DA October 2019 Mitochondrial Dysfunction in Primary Ovarian Insufficiency Endocrinology 160 10 2353 2366 doi 10 1210 en 2019 00441 PMC 6760336 PMID 31393557 Going through the menopause aged 11 BBC News 13 April 2018 OMIM Online Mendelian Inheritance in Man omim org Johns Hopkins University 3 November 2020 Retrieved 4 November 2020 An Online Catalog of Human Genes and Genetic Disorders Komorowska B 2017 Autoimmune premature ovarian failure Przeglad Menopauzalny Menopause Review 15 4 210 214 doi 10 5114 pm 2016 65666 PMC 5327623 PMID 28250725 Marozzi A Porta C Vegetti W Crosignani PG Tibiletti MG Dalpra L amp Ginelli E 2002 Mutation analysis of the inhibin alpha gene in a cohort of Italian women affected by ovarian failure Human Reproduction 17 1741 1745 doi 10 1093 humrep 17 7 1741 Thakur Mili Feldman Gerald Puscheck Elizabeth E January 2018 Primary ovarian insufficiency in classic galactosemia current understanding and future research opportunities Journal of Assisted Reproduction and Genetics 35 1 3 16 doi 10 1007 s10815 017 1039 7 ISSN 1573 7330 PMC 5758462 PMID 28932969 de Bruin JP Bovenhuis H van Noord PA Pearson PL van Arendonk JA te Velde ER et al September 2001 The role of genetic factors in age at natural menopause Human Reproduction 16 9 2014 8 doi 10 1093 humrep 16 9 2014 PMID 11527915 Blumenfeld Z Halachmi S Peretz BA Shmuel Z Golan D Makler A Brandes JM April 1993 Premature ovarian failure the prognostic application of autoimmunity on conception after ovulation induction Fertility and Sterility 59 4 750 5 doi 10 1016 S0015 0282 16 55854 3 PMID 8458491 Blumenfeld Z September 2007 Pregnancies in patients with POF gonadotropin stimulation and pretreatment with ethinyl estradiol Fertility and Sterility 88 3 763 author reply 763 doi 10 1016 j fertnstert 2007 07 001 PMID 17681336 Meduri G Massin N Guibourdenche J Bachelot A Fiori O Kuttenn F et al January 2007 Serum anti Mullerian hormone expression in women with premature ovarian failure Human Reproduction 22 1 117 23 doi 10 1093 humrep del346 PMID 16954410 Blepharophimosis ptosis and epicanthus inversus syndrome Medline Plus Retrieved 10 November 2020 Rzepka Gorska I Tarnowski B Chudecka Glaz A Gorski B Zielinska D Toloczko Grabarek A November 2006 Premature menopause in patients with BRCA1 gene mutation Breast Cancer Research and Treatment 100 1 59 63 doi 10 1007 s10549 006 9220 1 PMID 16773440 S2CID 19572648 Oktay K Kim JY Barad D Babayev SN January 2010 Association of BRCA1 mutations with occult primary ovarian insufficiency a possible explanation for the link between infertility and breast ovarian cancer risks Journal of Clinical Oncology 28 2 240 4 doi 10 1200 JCO 2009 24 2057 PMC 3040011 PMID 19996028 Titus S Li F Stobezki R Akula K Unsal E Jeong K et al February 2013 Impairment of BRCA1 related DNA double strand break repair leads to ovarian aging in mice and humans Science Translational Medicine 5 172 172ra21 doi 10 1126 scitranslmed 3004925 PMC 5130338 PMID 23408054 Lee KY Im JS Shibata E Park J Handa N Kowalczykowski SC Dutta A July 2015 MCM8 9 complex promotes resection of double strand break ends by MRE11 RAD50 NBS1 complex Nature Communications 6 7744 Bibcode 2015NatCo 6 7744L doi 10 1038 ncomms8744 PMC 4525285 PMID 26215093 a b AlAsiri S Basit S Wood Trageser MA Yatsenko SA Jeffries EP Surti U et al January 2015 Exome sequencing reveals MCM8 mutation underlies ovarian failure and chromosomal instability The Journal of Clinical Investigation 125 1 258 62 doi 10 1172 JCI78473 PMC 4382257 PMID 25437880 a b Wood Trageser MA Gurbuz F Yatsenko SA Jeffries EP Kotan LD Surti U et al December 2014 MCM9 mutations are associated with ovarian failure short stature and chromosomal instability American Journal of Human Genetics 95 6 754 62 doi 10 1016 j ajhg 2014 11 002 PMC 4259971 PMID 25480036 Fauchereau F Shalev S Chervinsky E Beck Fruchter R Legois B Fellous M et al May 2016 A non sense MCM9 mutation in a familial case of primary ovarian insufficiency Clinical Genetics 89 5 603 7 doi 10 1111 cge 12736 PMID 26771056 S2CID 33006407 Mamas L Mamas E August 2009 Dehydroepiandrosterone supplementation in assisted reproduction rationale and results Current Opinion in Obstetrics amp Gynecology 21 4 306 8 doi 10 1097 gco 0b013e32832e0785 PMID 19610174 S2CID 23452697 a b Wong QH Yeung TW Yung SS Ko JK Li HW Ng EH May 2018 The effect of 12 month dehydroepiandrosterone supplementation on the menstrual pattern ovarian reserve markers and safety profile in women with premature ovarian insufficiency Journal of Assisted Reproduction and Genetics 35 5 857 862 doi 10 1007 s10815 018 1152 2 PMC 5984890 PMID 29520734 Gleicher N Weghofer A Barad DH November 2010 Dehydroepiandrosterone DHEA reduces embryo aneuploidy direct evidence from preimplantation genetic screening PGS Reproductive Biology and Endocrinology 8 140 doi 10 1186 1477 7827 8 140 PMC 2992540 PMID 21067609 Mamas L Mamas E February 2009 Premature ovarian failure and dehydroepiandrosterone Fertility and Sterility 91 2 644 6 doi 10 1016 j fertnstert 2007 11 055 PMID 18321501 Joachim CM 2016 Chapter 12 Hormone Replacement Therapy in Women with POI A Patient s Perspective In Santoro NF Cooper AR eds Primary Ovarian Insufficiency A Clinical Guide to Early Menopause Springer pp 179 199 doi 10 1007 978 3 319 22491 6 ISBN 978 3 319 22490 9 Jadoul P Dolmans MM Donnez J 2010 Fertility preservation in girls during childhood is it feasible efficient and safe and to whom should it be proposed Human Reproduction Update 16 6 617 30 doi 10 1093 humupd dmq010 PMID 20462941 a b Ferreri J Fabregues F Calafell JM Solernou R Borras A Saco A Manau D Carmona F February 2020 Drug free in vitro activation of follicles and fresh tissue autotransplantation as a therapeutic option in patients with primary ovarian insufficiency Reprod Biomed Online 40 2 254 260 doi 10 1016 j rbmo 2019 11 009 PMID 31956062 S2CID 210830148 Kawamura K Cheng Y Suzuki N Deguchi M Sato Y Takae S et al October 2013 Hippo signaling disruption and Akt stimulation of ovarian follicles for infertility treatment Proceedings of the National Academy of Sciences of the United States of America 110 43 17474 9 Bibcode 2013PNAS 11017474K doi 10 1073 pnas 1312830110 PMC 3808580 PMID 24082083 a b Kalantaridou SN Nelson LM 2000 Premature ovarian failure is not premature menopause Annals of the New York Academy of Sciences 900 1 393 402 Bibcode 2000NYASA 900 393K doi 10 1111 j 1749 6632 2000 tb06251 x PMID 10818427 S2CID 37586048 Tepper NK Whiteman MK Marchbanks PA James AH Curtis KM December 2016 Progestin only contraception and thromboembolism A systematic review Contraception 94 6 678 700 doi 10 1016 j contraception 2016 04 014 PMC 11034842 PMID 27153743 American College of Obstetricians Gynecologists Committee on Adolescent Health Care November 2020 Gynecologic considerations for adolescents and young women with cardiac conditions ACOG Committee Opinion Number 813 Obstet Gynecol 136 5 e90 e99 doi 10 1097 AOG 0000000000004133 PMID 33093425 Santoro NF Wierman ME Canty Woessner C 2016 Chapter 6 Nonreproductive Conditions Associated with Primary Ovarian Insufficiency POI In Santoro NF Cooper AR eds Primary Ovarian Insufficiency A Clinical Guide to Early Menopause Springer pp 101 114 doi 10 1007 978 3 319 22491 6 ISBN 978 3 319 22490 9 Groff AA Covington SN Halverson LR Fitzgerald OR Vanderhoof V Calis K Nelson LM June 2005 Assessing the emotional needs of women with spontaneous premature ovarian failure Fertility and Sterility 83 6 1734 41 doi 10 1016 j fertnstert 2004 11 067 PMID 15950644 a b Orshan SA Ventura JL Covington SN Vanderhoof VH Troendle JF Nelson LM August 2009 Women with spontaneous 46 XX primary ovarian insufficiency hypergonadotropic hypogonadism have lower perceived social support than control women Fertility and Sterility 92 2 688 93 doi 10 1016 j fertnstert 2008 07 1718 PMC 2734403 PMID 18829005 Nelson LM May 2011 Synchronizing the world of women s health young Turks and transformational leaders report for duty Fertility and Sterility 95 6 1902 doi 10 1016 j fertnstert 2011 03 009 PMC 3153063 PMID 21841843 a b Nelson LM May 2011 One world one woman a transformational leader s approach to primary ovarian insufficiency Menopause 18 5 480 487 doi 10 1097 GME 0b013e318213f250 PMC 3115754 PMID 21686065 Sterling EW Nelson LM July 2011 From victim to survivor to thriver helping women with primary ovarian insufficiency integrate recovery self management and wellness Seminars in Reproductive Medicine 29 4 353 61 doi 10 1055 s 0031 1280920 PMC 4350677 PMID 21969269 Kjaer TK Jensen A Dalton SO Johansen C Schmiedel S Kjaer SK September 2011 Suicide in Danish women evaluated for fertility problems Human Reproduction 26 9 2401 7 doi 10 1093 humrep der188 PMID 21672927 Beck Peccoz P Persani L April 2006 Premature ovarian failure Orphanet Journal of Rare Diseases 1 9 doi 10 1186 1750 1172 1 9 PMC 1502130 PMID 16722528 Hubayter ZR Popat V Vanderhoof VH Ndubizu O Johnson D Mao E et al October 2010 A prospective evaluation of antral follicle function in women with 46 XX spontaneous primary ovarian insufficiency Fertility and Sterility 94 5 1769 74 doi 10 1016 j fertnstert 2009 10 023 PMC 2888894 PMID 19939372 Albright F Smith PH Fraser R 1941 A syndrome characterized by primary ovarian insufficiency and decreased stature report of 11 cases with a digression on hormonal control of axillary and pubic hair Am J Med Sci 204 625 48 doi 10 1097 00000441 194211000 00001 S2CID 59095440 Qing Zhu F 1992 Fu Qing zhu s Gynecology Translated by Yang SZ Liu DW Boulder CO Blue Poppy Press ISBN 978 0 936185 35 4 External links editPrimary Ovarian Insufficiency POI Overview National Institutes of Health Retrieved from https en wikipedia org w index php title Primary ovarian insufficiency amp oldid 1221312191, wikipedia, wiki, book, books, library,

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