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Klinefelter's syndrome
Klinefelter's syndrome, 47, XXY or XXY syndrome is a condition caused by a chromosome aneuploidy. Affected males have an extra X sex chromosome. The principal effects are development of small testes and reduced fertility. A variety of other physical and behavioral differences and problems are common, though severity varies and many boys and men with the condition have few detectable symptoms. The second most common extra chromosome condition, it is named after Dr. Harry Klinefelter, an endocrinologist at Massachusetts General Hospital, Boston, Massachusetts, who first described it in 1942.[1] The condition exists in roughly 1 out of every 500 to 1,000 males.[2] Because of the extra chromosome, individuals with the condition are usually referred to as "XXY Males", or "47,XXY Males".[3] Additional recommended knowledge
Signs and symptomsAffected males are almost always effectively sterile, although advanced reproductive assistance is sometimes possible.[4] Some degree of language learning impairment may be present.[5] In adults, possible characteristics vary widely and include little to no signs of affectedness, a lanky, youthful build and facial appearance, or a rounded body type with some degree of gynecomastia (increased breast tissue).[6] Gynecomastia is present to some extent in about a third of affected individuals, a slightly higher percentage than in the XY population, but only about 10% of XXY males' gynecomastia is noticeable enough to require surgery.[7] The term "hypogonadism" in XXY symptoms is often misinterpreted to mean "small testicles" or "small penis". In fact, it means decreased testicular hormone/endocrine function. Because of this hypogonadism, patients will often have a low serum testosterone level but high serum follicle-stimulating hormone (FSH) and luteinizing hormone (LH) levels.[8] Despite this misunderstanding of the term, however, it is true that XXY men often also have "microorchidism" (i.e. small testicles).[8] The more severe end of the spectrum of symptom expression is also associated with an increased risk of germ cell tumors,[9] breast cancer,[10] and osteoporosis,[2] risks shared to varying degrees[11] with females. Additionally, extant medical literature shows some individual case studies of Klinefelter's syndrome coexisting with other disorders, such as pulmonary disease, varicose veins, diabetes mellitus, and rheumatoid arthritis, but the etiologies (understanding of any potential causation relationship) between Klinefelter's and these other conditions are not well characterized or understood. In contrast to these potentially increased risks, it is currently thought that rare X-linked recessive conditions occur even less frequently in XXY males than in normal XY males, since these conditions are transmitted by genes on the X chromosome, and people with three X chromosomes are typically only carriers rather than affected by these X-linked recessive conditions. There are many variances within the XXY population, just as in the most common 46,XY population. While it is possible to characterise 47,XXY males with certain body types, that in itself should not be the method of identification as to whether or not someone has 47,XXY. The only reliable method of identification is karyotype testing. CauseThe extra X chromosome is retained because of a nondisjunction event during meiosis (sex cell division). The XXY chromosome arrangement is one of the most common genetic variations from the XY karyotype, occurring in about 1 in 500 to 1,000 live male births.[2] In mammals with more than one X chromosome, the genes on all but one X chromosome are not expressed; this is known as X inactivation. This happens in XXY males as well as normal XX females.[12] A few genes located in the pseudoautosomal regions, however, have corresponding genes on the Y chromosome and are capable of being expressed.[13] These triploid genes in XXY males may be responsible for symptoms associated with Klinefelter's syndrome.[citation needed] The first published report of a man with a 47,XXY karyotype was by Patricia A. Jacobs and Dr. J.A. Strong at Western General Hospital in Edinburgh, Scotland in 1959.[14] This karyotype was found in a 24-year-old man who had signs of Klinefelter's syndrome. Dr. Jacobs described her discovery of this first reported human or mammalian chromosome aneuploidy in her 1981 William Allan Memorial Award address.[15] TreatmentThe genetic variation is irreversible, but its symptoms can be altered or treated in a number of ways, including the use of testosterone treatment.[citation needed] Inadequately treated hypogonadism in Klinefelter syndrome increases recognized psychosocial morbidity]].[16] At least one study indicates that planned and timed support should be provided for young men with Klinefelter syndrome, to ameliorate current poor psychosocial outcomes.[16] Kathleen o'keefe is a common example of this rare disorder VariationsThe 48, XXYY (male) syndrome occurs 1 in 17,000 births and has traditionally been considered to be a variation of Klinefelter's syndrome. XXYY is no longer generally considered a variation of KS, although it has not yet been assigned an ICD-10 code. Males with Klinefelter syndrome may have a mosaic 47,XXY/46,XY constitutional karyotype and varying degrees of spermatogenic failure. Mosaicism 47,XXY/46,XX with clinical features suggestive of Klinefelter syndrome is very rare. Thus far, only about 10 cases have been described in literature.[17] ComplicationsPatients with Klinefelter syndrome have a 50 times greater risk of germ cell tumors (GSTs).[9] In these patients, GSTs usually contain nonseminomatous elements, present at an earlier age, and seldom are testicular in location. References
See also
Categories: Genetic disorders | Syndromes |
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This article is licensed under the GNU Free Documentation License. It uses material from the Wikipedia article "Klinefelter's_syndrome". A list of authors is available in Wikipedia. |