Triple X syndrome

Triple X syndrome
Classification and external resources
ICD-10 Q97.0
DiseasesDB 13386

Triple X syndrome is a form of chromosomal variation characterized by the presence of an extra X chromosome in each cell of a human female. Triple-x is a chromosomal condition which occurs only in females. A chromosome is a rod-like structure present in the nucleus of all body cells, with the exception of the red blood cells, which stores genetic information. Normally humans have twenty-three pairs of chromosomes, forty-six chromosomes in total. The twenty-third pair,otherwise referred to as the sex chromosomes, stores genetic information which determines our sex. Females have a xx pair and males have an xy pair of chromosomes. A female affected by triple-x syndrome has an xx pair of chromosomes, as well as an additional chromosome, resulting in the formation of xxx. A mosaic form also occurs where only a percentage of of body cell contain xxx while the remainder carry xx. The extent to which an individual is affected by the condition will depend upon the proportion of xxx to xx throughout. [1] The condition is also known as triplo-X, trisomy X, XXX syndrome, and 47,XXX aneuploidy. Triple X results during division of a parent's reproductive cells and occurs about once in every 1,000 births. Unlike most other chromosomal conditions (such as Down syndrome), there is usually no distinguishable difference to the naked eye between women with triple X and the rest of the female population.

Contents

Cause

Triple X syndrome is not inherited, but usually occurs as an event during the formation of reproductive cells (ovum and sperm). An error in cell division called nondisjunction can result in reproductive cells with additional chromosomes. For example, an oocyte or sperm cell may gain an extra copy of the X chromosome as a result of the non-disjunction. If one of these cells contributes to the genetic makeup of a child, the child will have an extra X chromosome in each of her cells. In some cases, trisomy X occurs during cell division in early embryonic development.

Some females with triple X syndrome have an extra X chromosome in only some of their cells. These cases are called 46,XX/47,XXX mosaics.

Symptoms

Due to the Lyonization, inactivation and formation of a Barr body, in all female cells, only one X chromosome is active at any time in a female cell. Thus, Triple X syndrome most often causes no unusual physical features or medical problems. But there are those rare cases when a female with Triple X syndrome is affected by changes such as tall stature, behavioral problems, clumsiness, poor coordination, midfacial hypoplasia, wide-set eyes, epicanthic fold, amenorrhea, posteriorly rotated ears, small head, long head, small lower jaw, expressionless face, prominent forehead, enamel hypoplasia, widely spaced nipples, small hands, small feet, kyphosis, lordosis, reduced muscle tone, ovarian failure, mental retardation, and infertility. [2] Females with the condition may have menstrual irregularities and, although rarely exhibiting severe mental impairments, have an increased risk of learning disabilities, delayed speech, deficient language skills and delayed development of motor skills.

There are seldom any observable physical anomalies in Triple X females, other than being taller than average. Most women with Triple X have normal sexual development. Some experience an early onset of menstruation. Triple X women are rarely diagnosed, apart from pre-natal testing methods, unless they undergo amniocentesis and blood tests for medical reasons later in life. Most medical professionals do not regard the condition as a disability. However, if mild delays are present, such status can be sought by parents for early intervention treatment.

Incidence

Triple X syndrome occurs in around 1 in 1,000 girls. On average, five to ten girls with triple X syndrome are born in the United States each day.[3]

First case

The first published report of a woman with a 47,XXX karyotype was by Patricia A. Jacobs, et al. at Western General Hospital in Edinburgh, Scotland, in 1959. It was found in a 35-year-old, 5 ft. 9 in. (176 cm) tall, 128 lb. (58.2 kg) woman who had premature ovarian failure at age 19; her mother was age 41 and her father was 40 at the time of her conception.[4]

Statistics

In Denmark between 1970-1984 76% of the prenatally diagnosed fetuses with triple-x were aborted. Between 1985-1987 this figure dropped to 56%. With improved information the number of abortions diminished. The experience in the Netherlands demonstrates that during the period 1991-2000 33% (18/54) of the couples that were confronted with a prenatal diagnoses 47, xxx elected to abort. If balanced information is provided to prospective parents, pre-natally, the incidence of voluntary termination (abortion) is reduced.[5]

See also

References

  1. Medical text written August 2002 by Contact a Family. Last reviewed February 2008 by Dr R Stanhope, Consultant Paediatric Endocrinologist, Institute of Child Health, London, UK. http://www.cafamily.org.uk/medicalinformation/conditions/azlistings/t40_1.html
  2. http://www.wrongdiagnosis.com/symbol/47_xxx_syndrome/symptoms.htm
  3. National Library of Medicine (2007). "Genetics Home Reference: Triple X syndrome". http://ghr.nlm.nih.gov/condition=triplexsyndrome. Retrieved 2007-03-22. 
  4. Jacobs PA, Baikie AG, Brown WM, MacGregor TN, Maclean N, Harnden DG (September 26, 1959). "Evidence for the existence of the human "super female"". Lancet 274 (7100): 423–5. doi:10.1016/S0140-6736(59)90415-5. PMID 14406377. http://www.sciencedirect.com/science?_ob=ArticleURL&_udi=B6T1B-49JVK1P-NW&_user=10&_coverDate=09%2F26%2F1959&_rdoc=1&_fmt=&_orig=search&_sort=d&view=c&_acct=C000050221&_version=1&_urlVersion=0&_userid=10&md5=9ff3228399f35afd36bda605db23eb23. 
  5. written by Connie T.R.M. Schrander-Stumpel, MD, PhD, Professor of Clinical Genetics, Academic Hospital Maastricht, Netherlands. http://www.triple-x-syndroom.nl/document31/patient+care+article+triplexsyndrome+or+trisomy+x

External links

Pathology: chromosome abnormalities (Q90-Q99 · 758)
Autosomal
Trisomies
Down syndrome (21) · Edwards syndrome (18) · Patau syndrome (13)
Trisomy 9 · Warkany syndrome 2 (8) · Trisomy 22/Cat eye syndrome (22) · Trisomy 16
Monosomies/deletions

Wolf-Hirschhorn syndrome (4) · Cri du chat/Chromosome 5q deletion syndrome (5) · Williams syndrome (7) · Jacobsen syndrome (11) · Miller-Dieker syndrome/Smith-Magenis syndrome (17) · DiGeorge syndrome (22)
genomic imprinting (Angelman syndrome/Prader–Willi syndrome (15))

18q deletion syndrome
X/Y linked
Monosomy
Trisomy/tetrasomy,
other karyotypes/mosaics

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
Burkitt's lymphoma t(8 MYC;14 IGH) · Follicular lymphoma t(14 IGH;18 BCL2) · Mantle cell lymphoma/Multiple myeloma t(11 CCND1:14 IGH) · Anaplastic large cell lymphoma t(2 ALK;5 NPM1) · Acute lymphoblastic leukemia
Myeloid
Philadelphia chromosome t(9 ABL; 22 BCR) · Acute myeloblastic leukemia with maturation t(8 RUNX1T1;21 RUNX1) · Acute promyelocytic leukemia t(15 PML,17 RARA) · Acute megakaryoblastic leukemia t(1 RBM15;22 MKL1)
Other
Ewing's sarcoma t(11 FLI1; 22 EWS) · Synovial sarcoma t(x SYT;18 SSX) · Dermatofibrosarcoma protuberans t(17 COL1A1;22 PDGFB) · Myxoid liposarcoma t(12 DDIT3; 16 FUS) · Desmoplastic small round cell tumor t(11 WT1; 22 EWS) · Alveolar rhabdomyosarcoma t(2 PAX3; 13 FOXO1) t (1 PAX7; 13 FOXO1)
Gonadal dysgenesis
Mixed gonadal dysgenesis · XX gonadal dysgenesis
Other
Fragile X syndrome · Uniparental disomy · XX male syndrome