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Turner's syndrome

 
Medical Encyclopedia: Turner Syndrome
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Definition

Turner syndrome is a chromosomal disorder affecting females wherein one of the two X-chromosomes is defective or completely absent.

Description

Chromosomes are structures in the nucleus of every cell in the human body. Chromosomes contain the genetic information necessary to direct the growth and normal functioning of all cells and systems of the body. A normal individual has a total of 46 chromosomes in each cell, two of which are responsible for determining gender. Normally, females have two X-chromosomes and males have one X and one Y-chromosome.

In Turner syndrome, an error occurring very early in development results in an abnormal number and arrangement of chromosomes. Most commonly, an individual with Turner syndrome will be born with 45 chromosomes in each cell rather than 46. The missing chromosome is an X-chromosome. The affected person is always female.

The prevalence of Turner syndrome is widely reported as being approximately one per 2,000 live female births although researchers have reported prevalence rates that range from one in 3,125 to one in 5,000 live female births.

About 1% to 2% of all female conceptions have a missing X-chromosome. Of these, the majority (99%) spontaneously abort, usually during the first trimester of pregnancy. With ultrasound being used more frequently, researchers have realized that some pregnancies with a missing X-chromosome that progress into the second trimester are associated with nuchal cysts, severe lymphedema, or hydrops fetalis. These pregnancies are associated with a high frequency of fetal death.

— L. Fleming Fallon, Jr., MD, PhD, DrPH


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Dictionary: Tur·ner's syndrome   (tûr'nərz) pronunciation
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n.
A congenital condition of females associated with a defect or absence of an X-chromosome, characterized by short stature, sexual underdevelopment, and other physical abnormalities.

[After Henry Hubert Turner (1892-1970), American endocrinologist.]


Dental Dictionary: Turner’s syndrome
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n.pr
XO syndrome, gonadal dysgenesis, genital dwarfism

Absence of one of the X chromosomes, with affected females being sterile and short of stature and having various congenital anomalies, such as webbing of the neck, low-set ears, wide-set eyes, shield-like chest, absence of breasts, and cubitus valgus. Common orofacial findings are hypoplastic mandible, high palatal vault, and dental anomalies.

Children's Health Encyclopedia: Turner Syndrome
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Definition

Turner syndrome is a birth defect caused by the absence of an X chromosome in some or all cells of a female, which inhibits sexual development and usually causes infertility.

Description

Chromosomes are structures in the nucleus of every cell in the human body that contain the genetic information necessary to direct the growth and normal functioning of all cells and systems of the body. A normal individual has a total of 46 chromosomes in each cell, two of which are responsible for determining gender. Normally, females have two X chromosomes, and males have one X and one Y chromosome.

In Turner syndrome, an error occurring very early in development results in an abnormal number and arrangement of chromosomes. Most commonly, an individual with Turner syndrome will be born with 45 chromosomes in each cell rather than 46. The missing chromosome is an X chromosome. The affected person is always female.

Turner syndrome may result in a wide spectrum of symptoms, from major heart defects to minor cosmetic issues. Some individuals with Turner syndrome may only have a few symptoms while others may have many. Almost all girls with Turner syndrome have short stature and loss of ovarian function, but the severity of the symptoms varies among individuals.

Turner syndrome is also referred to as Bonnevie-Ullrich syndrome, gonadal dysgenesis, and monosomy X.

Demographics

The prevalence of Turner syndrome is widely reported as being approximately one per 2,500 live female births, although researchers have reported prevalence rates that range from one in 3,125 to one in 5,000 live female births. About 1 to 2 percent of all female conceptions have a missing X chromosome. Of these, the majority (99%) spontaneously abort, usually during the first trimester of pregnancy.

Causes and Symptoms

Turner syndrome usually occurs sporadically, which means that the mutation occurs during fetal development and is not inherited from either parent. In rare cases, a parent may carry rearranged chromosomes that can result in Turner syndrome in a daughter, which is the only situation in which the Turner syndrome is inherited.

More than half of all girls with Turner syndrome are mosaics, which means that the mutation occurs in some but not all cells of their body. Therefore, Turner syndrome can vary in severity. The fewer the affected cells, the milder the disease.

Symptoms of a girl with Turner syndrome include:

  • short stature
  • webbed skin of the neck
  • abnormal eye features (drooping eyelids)
  • abnormal bone development, such as a "shield-shaped," broad flat chest
  • absent or retarded development of secondary sexual characteristics that normally appear at puberty, including sparse pubic hair and small breasts
  • coarctation (narrowing) of the aorta
  • bicuspid aortic valve
  • infertility
  • dry eyes
  • absence of menstruation

Growth in children with Turner syndrome is characterized by a slight intrauterine growth retardation, relatively normal growth rates for the first several years of life, a progressive deceleration of growth later in childhood, and the lack of a pubertal growth spurt. The average height of Turner women is 147 cm (57.8 inches), varying between 135 (53 inches) and 163 cm (64 inches). This is about 20 cm (7.8 inches) shorter than the height of women with normal chromosomes.

Normal pubertal development and spontaneous menstrual periods do not occur in the majority of children with Turner syndrome. Most girls with Turner syndrome do not have ovaries with healthy oocytes capable of fertilization and embryo formation. However, it is estimated that 3 to 8 percent of girls with a single X chromosome and 12 to 21 percent of females with sex chromosome mosaicism may have normal pubertal development and spontaneous menstrual periods. A few pregnancies have been reported in women with Turner syndrome.

Individuals with Turner syndrome report an increased incidence of fractures in childhood and osteoporotic fractures in adulthood. The primary cause of osteoporosis may be inadequate levels of estrogen circulating in the body; however, defects in bone structure or strength may also be related to the loss of unknown X-chromosome genes.

The incidence of type II diabetes, also known as insulin resistant diabetes (glucose intolerance), has been reported to be increased in Turner syndrome, with individuals having twice the risk of the general population for developing this disease. The muscles of many persons with Turner syndrome fail to use glucose efficiently, which may contribute to the development of high blood sugar.

Many women with Turner syndrome have high blood pressure, which may even occur during childhood. High blood pressure may be due to aortic constriction or to kidney abnormalities; however, in a majority of cases, no specific cause for high blood pressure can be identified.

Kidney problems are present in about one third of girls with Turner syndrome and may contribute to high blood pressure. Three types of kidney problems have been reported: the presence of a single horse-shoe shaped kidney (normally two distinct, bean-shaped structures are present); an abnormal urine-collecting system; or an abnormal artery supply to the kidneys.

From 5 to 10 percent of girls with Turner syndrome have a severe constriction of the major blood vessel coming from the heart (coarctation of the aorta). This defect is thought to be a result of an obstructed lymphatic system compressing the aorta during fetal development. Other major defects and its major vessels are reported to a lesser degree. As many as 15 percent of children with Turner syndrome have bicuspid aortic valves, where the major blood vessel from the heart has only two rather than three components to the valve regulating blood flow.

Juvenile rheumatoid arthritis, an autoimmune condition, has been associated with Turner syndrome. The prevalence seems to be at least six times greater than would be expected if the two conditions were only randomly associated. Girls with Turner syndrome have an elevated prevalence rate of dental caries and such other periodontal conditions as gum disease and plaque.

Approximately one-third of girls with Turner syndrome have a thyroid disorder, usually hypothyroidism. Symptoms of this condition include decreased energy, dry skin, cold-intolerance, and poor growth.

Contrary to earlier reports, most individuals with Turner syndrome are not mentally retarded. They may have some learning disabilities, particularly with regard to spatial perception, visual-motor coordination, and mathematics. This specific learning problem is referred to as Turner neurocognitive phenotype and appears to be due to loss of X chromosome genes important for selected aspects of nervous system development. The verbal skills of girls with Turner syndrome are usually normal. Some girls with Turner syndrome may also have difficulties with memory and motor coordination, which may be related to estrogen deficiency.

When to Call the Doctor

Parents should call their healthcare provider if their infant has symptoms of this disorder or if an adolescent girl's sexual development appears to be delayed.

Diagnosis

Turner syndrome is either diagnosed at birth because of associated anomalies or at puberty when there is absent or delayed menses and delayed development of normal secondary sexual characteristics. During a physical examination, the doctor looks for underdeveloped breasts and genitalia, webbed neck, short stature, low hairline in back, simian crease (a single crease in the palm), and abnormal development of the chest. An ultrasound may reveal small or undeveloped female reproductive organs while a gynecologic examination may reveal a dry vaginal lining. A kidney ultrasound can be used to evaluate abnormalities of the kidneys. After diagnosis, echocardiogram (heart ultrasound) and an MRI of the chest are performed to evaluate possible cardiac defects.

Hands and feet of infants with Turner syndrome may be swollen or puffy at birth; there may be swelling at the nape of the neck. These babies often have soft nails that turn upwards on the ends when they are older. These features appear to be due to obstruction of the lymphatic system during fetal development. Another characteristic cosmetic feature is the presence of multiple pigmented nevi (colored spots on the skin).

Turner syndrome is confirmed on the basis of genetic analysis of chromosomes, which can be done prior to birth. However, the predictive value of amniocentesis in diagnosing Turner syndrome varies from 21 to 67 percent. There is no significant relation between the mother's age and risk of Turner syndrome.

Treatment

Most individuals with Turner syndrome require female hormone therapy to promote development of secondary sexual characteristics and menstruation. The time of beginning therapy varies with individuals. Experts recommend that therapy begin when a woman expresses concern about her onset of puberty or by the age of 15. Girls and women with Turner syndrome should be treated with estrogen/progesterone to maintain their secondary sexual development and to protect their bones from osteoporosis until at the least the usual age of menopause (50 years). The use of estrogen therapy may also improve memory and motor coordination problems associated with estrogen deficiency. Assisted reproductive technology may allow for women with Turner syndrome to become pregnant with donated ooctyes.

All women receiving long-term, female hormone therapy require periodic gynecological examinations, because those with Turner syndrome have an increased risk of developing neoplasms, such as gonadoblastoma and dysgerminoma, which arise from their rudimentary streak gonads (a condition in which germ cells are absent and the ovary is replaced by a fibrous streak).

Because it is so dangerous, experts suggest early screening and surgery for aortic coarctation of the artery in girls with Turner syndrome. Bicuspid aortic valves can deteriorate or become infected, so it is advised that all girls with Turner syndrome undergo annual cardiac evaluations. Kidney problems may also be corrected surgically, but there still may be a tendency for high blood pressure and infections. Diabetes type II can be controlled through careful monitoring of blood-sugar levels, diet, exercise, regular health care, and medication if necessary. Hypothryoidism can be easily treated with thyroid hormone supplements.

Plastic surgery to correct webbing of the neck should be considered at an early age (before entering school) for girls with Turner syndrome.

Final adult height in individuals with Turner syndrome can be increased if growth hormone (GH) treatment is given relatively early in childhood. However, not all individuals get a good growth response to GH.

Prognosis

Most children with Turner syndrome can live relatively normal lives. The prognosis for a person with Turner syndrome is dependent on the other associated conditions that may be present. Care must be taken to regularly monitor patients for the health problems that are associated with Turner syndrome. For example, heart or kidney defects may significantly impact their quality of life. Without these types of conditions, however, their life expectancy is normal. Support will be necessary to help an adolescent girl cope with body image issues and to help some women accept the fact that they will never be able to have children.

Parental Concerns

Families may wish to seek counseling regarding the effects of the syndrome on relationships within the family. Many people respond with guilt, fear, or blame when a genetic disorder is diagnosed in the family, or they may overprotect the affected member. Support groups are often good sources of information about Turner syndrome; they can offer helpful suggestions about living with it as well as emotional support.

Resources

Books

All about Me: Growing Up with Turner Syndrome and Nonverbal Learning Disabilities. Wallington, VT: Maple Leaf Center, 2004.

Roche, Alex F., and Shumei S. Sun. Human Growth: Assessment and Interpretation. Cambridge, UK: Cambridge University Press, 2003.

Turner Syndrome: A Medical Dictionary, Bibliography, and Annotated Research Guide to Internet References. San Diego, CA: Icon Health Publications, 2004.

Organizations

Human Growth Foundation. 997 Glen Cove Avenue, Glen Head, NY 11545. Web site: www.hgfound.org.

Turner Syndrome Society of the United States. 14450 TC Jester, Houston, TX 77014. Web site: www.turner-syndrome-us.org.

Turner Syndrome Support Society (UK). Hardgate, Clydebank, UK. Web site: .

Web Sites

"Turner Syndrome." National Institute of Child Health and Human Development, National Institutes of Health. Available online at (accessed November 15, 2004).

[Article by: Judith Sims, MS L. Fleming Fallon, MD, PhD, DrPH]


Britannica Concise Encyclopedia: Turner syndrome
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Chromosomal disorder (from the presence of only one sex chromosome, X, in all or some of the body's cells) that causes abnormal sexual development in females. The syndrome may include absent or undeveloped ovaries, underdeveloped secondary sex characteristics, low hairline, webbed neck, shield-shaped chest with wide-spaced nipples, and kidney and heart malformations with coarctation (narrowing) of the aorta. It may not be recognized until a girl fails to undergo puberty at a normal age. Estrogen treatment results in puberty, adult appearance, and normal sex drive but not fertility. Surgery can correct malformations.

For more information on Turner syndrome, visit Britannica.com.

Wikipedia: Turner syndrome
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Turner Syndrome
Classification and external resources

45,X karyotype - note unpaired X at lower right.
ICD-10 Q96.
ICD-9 758.6
DiseasesDB 13461
MedlinePlus 000379
eMedicine ped/2330
MeSH D014424

Turner syndrome or Ullrich-Turner syndrome (also known as "Gonadal dysgenesis"[1]:550) encompasses several conditions, of which monosomy X (absence of an entire sex chromosome) is most common. It is a chromosomal disorder in which all or part of one of the sex chromosomes is absent (unaffected humans have 46 chromosomes, of which 2 are sex chromosomes). Typical females have 2 X chromosomes, but in Turner syndrome, one of those sex chromosomes is missing or has other abnormalities. In some cases, the missing chromosome is present in some cells but not others, a condition referred to as mosaicism[2] or 'Turner mosaicism'.

Occurring in 1 out of every 2500 girls, the syndrome manifests itself in a number of ways. There are characteristic physical abnormalities, such as short stature, swelling, broad chest, low hairline, low-set ears, and webbed necks.[3] Girls with Turner syndrome typically experience gonadal dysfunction (non-working ovaries), which results in amenorrhea (absence of menstrual cycle) and sterility. Concurrent health concerns are also frequently present, including congenital heart disease, hypothyroidism (reduced hormone secretion by the thyroid), diabetes, vision problems, hearing concerns, and many other autoimmune diseases.[4] Finally, a specific pattern of cognitive deficits is often observed, with particular difficulties in visuospatial, mathematical, and memory areas.[5]

Contents

Symptoms

Common symptoms of Turner syndrome include:

  • Short stature
  • Lymphedema (swelling) of the hands and feet
  • Broad chest (shield chest) and widely-spaced nipples
  • Low hairline
  • Low-set ears
  • Reproductive sterility
  • Rudimentary ovaries gonadal streak (underdeveloped gonadal structures)
  • Amenorrhea, or the absence of a menstrual period
  • Increased weight, obesity
  • Shield shaped thorax of heart
  • Shortened metacarpal IV (of hand)
  • Small fingernails
  • Characteristic facial features
  • Webbed neck from cystic hygroma in infancy
  • Coarctation of the aorta
  • Poor breast development
  • Horseshoe kidney
  • Visual impairments sclera, cornea, glaucoma, etc.
  • Ear infections and hearing loss

Other symptoms may include a small lower jaw (micrognathia), cubitus valgus (turned-out elbows), soft upturned nails, palmar crease and drooping eyelids. Less common are pigmented moles, hearing loss, and a high-arch palate (narrow maxilla). Turner syndrome manifests itself differently in each female affected by the condition, and no two individuals will share the same symptoms.

Risk factors

Risk factors for Turner syndrome are not well known. Nondisjunctions increase with maternal age, such as for Down syndrome, but that effect is not clear for Turner syndrome. It is also unknown if there is a genetic predisposition present that causes the abnormality, though most researchers and doctors treating Turners women agree that this is highly unlikely. There is currently no known cause for Turner syndrome, though there are several theories surrounding the subject. The only solid fact that is known today is that during conception part or all of the second sex chromosome is not transferred to the fetus.[6]

Incidence

Approximately 98 percent of all fetuses with Turner syndrome result in miscarriage.[citation needed] Turner syndrome accounts for about 10 percent of the total number of spontaneous abortions in the United States. The incidence of Turner syndrome in live female births is believed to be 1 in 2500.

History

The syndrome is named after Henry Turner, an Oklahoma endocrinologist, who described it in 1938.[7] In Europe, it is often called Ullrich-Turner syndrome or even Bonnevie-Ullrich-Turner syndrome to acknowledge that earlier cases had also been described by European doctors. The first published report of a female with a 45,X karyotype was in 1959 by Dr. Charles Ford and colleagues in Harwell, Oxfordshire and Guy's Hospital in London.[8] It was found in a 14-year-old girl with signs of Turner syndrome.

Diagnosis

Turner syndrome may be diagnosed by amniocentesis during pregnancy. Sometimes, fetuses with Turner syndrome are identified by abnormal ultrasound findings (i.e. heart defect, kidney abnormality, cystic hygroma, ascites). Although the recurrence risk is not increased, genetic counseling is often recommended for families who have had a pregnancy or child with Turner syndrome.

A test, called a karyotype or a chromosome analysis, analyzes the chromosomal composition of the individual. This is the test of choice to diagnose Turner syndrome.

Prognosis

While most of the physical findings in Turner syndrome are harmless, there can be significant medical problems associated with the syndrome.

Cardiovascular

Price et al. (1986 study of 156 female patients with Turner syndrome) showed a significantly greater number of deaths from diseases of the circulatory system than expected, half of them due to congenital heart disease—mostly preductal coarctation of the aorta. When patients with congenital heart disease were omitted from the sample of the study, the mortality from circulatory disorders was not significantly increased.

Cardiovascular malformations are a serious concern as it is the most common cause of death in adults with Turner syndrome. It takes an important part in the 3-fold increase in overall mortality and the reduced life expectancy (up to 13 years) associated with Turner syndrome.

Cause

According to Sybert, 1998 the data is inadequate to allow conclusions about phenotype-karyotype correlations in regard to cardiovascular malformations in Turner syndrome because the number of individuals studied within the less common karyotype groups is too small. Other studies also suggest the presence of hidden mosaicisms that are not diagnosed on usual karyotypic analyses in some patients with 45,X karyotype.

In conclusion, the associations between karyotype and phenotypic characteristics, including cardiovascular malformations, remain questionable.

Prevalence of cardiovascular malformations

The prevalence of cardiovascular malformations among patients with Turner syndrome ranges from 17% (Landin-Wilhelmsen et al., 2001) to 45% (Dawson-Falk et al., 1992).

The variations found in the different studies are mainly attributable to variations in non-invasive methods used for screening and the types of lesions that they can characterize (Ho et al., 2004). However Sybert, 1998 suggests that it could be simply attributable to the small number of subjects in most studies.

Different karyotypes may have differing prevalence of cardiovascular malformations. Two studies found a prevalence of cardiovascular malformations of 30%[9] and 38%[10] in a group of pure 45,X monosomy. But considering other karyotype groups, they reported a prevalence of 24.3%[9] and 11%[10] in patients with mosaic X monosomy , and a prevalence of 11% in patients with X chromosomal structural abnormalities.[9]

The higher prevalence in the group of pure 45,X monosomy is primarily due to a significant difference in the prevalence of aortic valve abnormalities and aortic coarctation, the two most common cardiovascular malformations.

Congenital heart disease

The most commonly observed are congenital obstructive lesions of the left side of the heart, leading to reduced flow on this side of the heart. This includes bicuspid aortic valve and coarctation of the aorta. Sybert, 1998 found that more than 50% of the cardiovascular malformations observed in her study of individuals with Turner syndrome were bicuspid aortic valves or coarctation of the aorta, alone or in combination.

Other congenital cardiovascular malformations, such as partial anomalous venous drainage and aortic stenosis or aortic regurgitation, are also more common in Turner syndrome than in the general population. Hypoplastic left heart syndrome represents the most severe reduction in left-sided structures.

Bicuspid aortic valve. Up to 15% of adults with Turner syndrome have bicuspid aortic valves, meaning that there are only two, instead of three, parts to the valves in the main blood vessel leading from the heart. Since bicuspid valves are capable of regulating blood flow properly, this condition may go undetected without regular screening. However, bicuspid valves are more likely to deteriorate and later fail. Calcification also occurs in the valves,[11] which may lead to a progressive valvular dysfunction as evidenced by aortic stenosis or regurgitation.[12]

With a prevalence from 12.5%[9] to 17.5% (Dawson-Falk et al., 1992), bicuspid aortic valve is the most common congenital malformation affecting the heart in this syndrome. It is usually isolated but it may be seen in combination with other anomalies, particularly coarctation of the aorta.

Coarctation of the aorta. Between 5% and 10% of those born with Turner syndrome have coarctation of the aorta, a congenital narrowing of the descending aorta, usually just distal to the origin of the left subclavian artery and opposite to the duct (and so termed “juxtaductal”). Estimates of the prevalence of this malformation in patients with Turner syndrome ranges from 6.9%[9] to 12.5% (Dawson-Falk et al., 1992). A coarctation of the aorta in a female is suggestive of Turner syndrome, and suggests the need for further tests, such as a karyotype.

Partial anomalous venous drainage. This abnormality is a relatively rare congenital heart disease in the general population. The prevalence of this abnormality also is low (around 2.9%) in Turner syndrome. However, its relative risk is 320 in comparison with the general population. Strangely, Turner syndrome seems to be associated with unusual forms of partial anomalous venous drainage.[9][13]

In the management of a patient with Turner syndrome it is essential to keep in mind that these left-sided cardiovascular malformations in Turner syndrome result in an increased susceptibility to bacterial endocarditis. Therefore prophylactic antibiotics should be considered when procedures with high risk endocarditis are performed, such as dental cleaning.[12]

Turner syndrome is often associated with persistent hypertension, sometimes in childhood. In the majority of Turner syndrome patients with hypertension, there is no specific cause. In the remainder, it is usually associated with cardiovascular or kidney abnormalities, including coarctation of the aorta.

Aortic dilation, dissection, and rupture

Two studies have suggested aortic dilatation in Turner syndrome, typically involving the root of the ascending aorta and occasionally extending through the aortic arch to the descending aorta, or at the site of previous coarctation of the aorta repair.[14]

  • Allen et al., 1986 who evaluated 28 girls with Turner syndrome, found a significantly greater mean aortic root diameter in patients with Turner syndrome than in the control group (matched for body surface area). Nonetheless, the aortic root diameter found in Turner syndrome patients were still well within the limits.[15]
  • This has been confirmed by the study of Dawson-Falk et al., 1992 who evaluated 40 patients with Turner syndrome.[16] They presented basically the same findings: a greater mean aortic root diameter, which nevertheless remains within the normal range for body surface area.

Sybert, 1998 points out that it remains unproven that aortic root diameters that are relatively large for body surface area but still well within normal limits imply a risk for progressive dilatation.[17]

Prevalence of aortic abnormalities

The prevalence of aortic root dilatation ranges from 8.8%[14] to 42%[12] in patients with Turner syndrome. Even if not every aortic root dilatation necessarily goes on to an aortic dissection (circumferential or transverse tear of the intima), complications such as dissection, aortic rupture resulting in death may occur. The natural history of aortic root dilatation is still unknown, but it is a fact that it is linked to aortic dissection and rupture, which has a high mortality rate.[18]

Aortic dissection affects 1% to 2% of patients with Turner syndrome. As a result any aortic root dilatation should be seriously taken into account as it could become a fatal aortic dissection. Routine surveillance is highly recommended.[12]

Risk factors for aortic rupture

It is well established that cardiovascular malformations (typically bicuspid aortic valve, coarctation of the aorta and some other left-sided cardiac malformations) and hypertension predispose to aortic dilatation and dissection in the general population. At the same time it has been shown that these risk factors are common in Turner syndrome. Indeed these same risk factors are found in more than 90% of patients with Turner syndrome who develop aortic dilatation. Only a small number of patients (around 10%) have no apparent predisposing risk factors. It is important to note that the risk of hypertension is increased 3-fold in patients with Turner syndrome. Because of its relation to aortic dissection blood pressure needs to be regularly monitored and hypertension should be treated aggressively with an aim to keep blood pressure below 140/80 mmHg. It has to be noted that as with the other cardiovascular malformations, complications of aortic dilatation is commonly associated with 45,X karyotype.[12]

Pathogenesis of aortic dissection and rupture

The exact role that all these risk factors play in the process leading to such fatal complications is still quite unclear. Aortic root dilatation is thought to be due to a mesenchymal defect as pathological evidence of cystic medial necrosis has been found by several studies. The association between a similar defect and aortic dilatation is well established in such conditions such as Marfan Syndrome. Also, abnormalities in other mesenchymal tissues (bone matrix and lymphatic vessels) suggests a similar primary mesenchymal defect in patients with Turner syndrome.[14] However there is no evidence to suggest that patients with Turner syndrome have a significantly higher risk of aortic dilatation and dissection in absence of predisposing factors. So the risk of aortic dissection in Turner syndrome appears to be a consequence of structural cardiovascular malformations and hemodynamic risk factors rather than a reflection of an inherent abnormality in connective tissue (Sybert, 1998). The natural history of aortic root dilatation is unknown, but because of its lethal potential, this aortic abnormality needs to be carefully followed.

Pregnancy

As more women with Turner syndrome complete pregnancy thanks to the new modern techniques to treat infertility, it has to be noted that pregnancy may be a risk of cardiovascular complications for the mother. Indeed several studies had suggested an increased risk for aortic dissection in pregnancy.[14] Three deaths have even been reported. The influence of estrogen has been examined but remains unclear. It seems that the high risk of aortic dissection during pregnancy in women with Turner syndrome may be due to the increased hemodynamic load rather than the high estrogen rate.[12] Of course these findings are important and need to be remembered while following a pregnant patient with Turner syndrome.

Cardiovascular malformations in Turner syndrome are also very serious, not only because of their high prevalence in that particular population but mainly because of their high lethal potential and their great implication in the increased mortality found in patients with Turner syndrome. Congenital heart disease needs to be explored in every female newly diagnosed with Turner syndrome. As adults are concerned close surveillance of blood pressure is needed to avoid a high risk of fatal complications due to aortic dissection and rupture.

Skeletal

Normal skeletal development is inhibited due to a large variety of factors, mostly hormonal. The average height of a woman with Turner syndrome, in the absence of growth hormone treatment, is 4'7", about 140 cm.

The fourth metacarpal bone (fourth toe and ring finger) may be unusually short, as may the fifth.

Due to inadequate production of estrogen, many of those with Turner syndrome develop osteoporosis. This can decrease height further, as well as exacerbate the curvature of the spine, possibly leading to scoliosis. It is also associated with an increased risk of bone fractures.

Kidney

Approximately one-third of all women with Turner syndrome have one of three kidney abnormalities:

  1. A single, horseshoe-shaped kidney on one side of the body.
  2. An abnormal urine-collecting system.
  3. Poor blood flow to the kidneys.

Some of these conditions can be corrected surgically. Even with these abnormalities, the kidneys of most women with Turner syndrome function normally. However, as noted above, kidney problems may be associated with hypertension.

Thyroid

Approximately one-third of all women with Turner syndrome have a thyroid disorder. Usually it is hypothyroidism, specifically Hashimoto's thyroiditis. If detected, it can be easily treated with thyroid hormone supplements.

Diabetes

Women with Turner syndrome are at a moderately increased risk of developing type 1 diabetes in childhood and a substantially increased risk of developing type 2 diabetes by adult years. The risk of developing type 2 diabetes can be substantially reduced by maintaining a normal weight.

Cognitive

Turner syndrome does not typically cause mental retardation or impair cognition. However, learning difficulties are common among women with Turner syndrome, particularly a specific difficulty in perceiving spatial relationships, such as Nonverbal Learning Disorder. This may also manifest itself as a difficulty with motor control or with mathematics. While it is non-correctable, in most cases it does not cause difficulty in daily living.

There is also a rare variety of Turner Syndrome, known as "Ring-X Turner Syndrome", which has an approximate 60 percent association with mental retardation. This variety accounts for approximately 2 - 4% of all Turner Syndrome cases.[19]

Reproductive

Women with Turner syndrome are almost universally infertile. While some women with Turner syndrome have successfully become pregnant and carried their pregnancies to term, this is very rare and is generally limited to those women whose karyotypes are not 45,X.[20][21] Even when such pregnancies do occur, there is a higher than average risk of miscarriage or birth defects, including Turner Syndrome or Down Syndrome.[22] Some women with Turner syndrome who are unable to conceive without medical intervention may be able to use IVF or other fertility treatments.[23]

Usually estrogen replacement therapy is used to spur growth of secondary sexual characteristics at the time when puberty should onset. While very few women with Turner Syndrome menstruate spontaneously, estrogen therapy requires a regular shedding of the uterine lining ("withdrawal bleeding") to prevent its overgrowth. Withdrawal bleeding can be induced monthly, like menstruation, or less often, usually every three months, if the patient desires. Estrogen therapy does not make a woman with nonfunctional ovaries fertile, but it plays an important role in assisted reproduction; the health of the uterus must be maintained with estrogen if an eligible woman with Turner Syndrome wishes to use IVF.

Treatment

As a chromosomal condition, there is no cure for Turner syndrome. However, much can be done to minimize the symptoms. For example:[24]

  • Growth hormone, either alone or with a low dose of androgen, will increase growth and probably final adult height. Growth hormone is approved by the U.S. Food and Drug Administration for treatment of Turner syndrome and is covered by many insurance plans.[24][25] There is evidence that this is effective, even in toddlers.[26]
  • Estrogen replacement therapy has been used since the condition was described in 1938 to promote development of secondary sexual characteristics. Estrogens are crucial for maintaining good bone integrity and tissue health.[24] Women with Turner Syndrome who do not have spontaneous puberty and who are not treated with estrogen are at high risk for osteoporosis.
  • Modern reproductive technologies have also been used to help women with Turner syndrome become pregnant if they desire. For example, a donor egg can be used to create an embryo, which is carried by the Turner syndrome woman.[24]
  • Uterine maturity is positively associated with years of estrogen use, history of spontaneous menarche, and negatively associated with the lack of current hormone replacement therapy.[27]

See also

References

  1. ^ James, William; Berger, Timothy; Elston, Dirk (2005). Andrews' Diseases of the Skin: Clinical Dermatology. (10th ed.). Saunders. ISBN 0721629210.
  2. ^ Campbell, Neil. A; Brad Williamson, Robin J. Heyden (2006). Biology : Exploring Life. Boston, Massachusetts: Pearson Prentice Hall. ISBN 0-13-250882-6. 
  3. ^ "[htttp://school.eb.com Turner's Syndrome]". Encyclopedia Britannica. Encyclopedia Britannica. htttp://school.eb.com. Retrieved 2009-03-24. 
  4. ^ Sybert VP, McCauley E (September 2004). "Turner's syndrome" ([dead link]Scholar search). N. Engl. J. Med. 351 (12): 1227–38. doi:10.1056/NEJMra030360. PMID 15371580. http://content.nejm.org/cgi/pmidlookup?view=short&pmid=15371580&promo=ONFLNS19. 
  5. ^ Rovet JF (May 1993). "The psychoeducational characteristics of children with Turner syndrome". J Learn Disabil 26 (5): 333–41. doi:10.1177/002221949302600506. PMID 8492052. 
  6. ^ http://www.nytimes.com/2009/09/15/science/15chrom.html?pagewanted=1&_r=1&hpw
  7. ^ Turner HH (1938). "A syndrome of infantilism, congenital webbed neck, and cubitus valgus". Endocrinology 23: 566–74. 
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Further reading

External links

v  d  e
Pathology: chromosome abnormalities (Q90-Q99 · 758)
Autosomal
X/Y linked

Turner syndrome (XO)
Klinefelter's syndrome (47,XXY) · 48,XXYY · 48,XXXY · 49,XXXYY · 49,XXXXY

Triple X syndrome (47,XXX) · 48,XXXX · 49,XXXXX

47,XYY · 48,XYYY · 49,XYYYY

46,XX/XY
Translocations
Lymphoid
Myeloid
Other
Gonadal dysgenesis
Other


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