Background: The association of achondroplasia and Klinefelter syndrome is extremely rare. To date, five cases have
been previously reported, all of them diagnosed beyond the postnatal period, and only one was molecularly
characterized. We describe the first case of this unusual association diagnosed in the neonatal period, the clinical
findings and the molecular studies undertaken.
Case presentation: The boy was born at term with clinical and radiological features indicating the diagnosis of
achondroplasia or hypochondroplasia combined with the prenatal karyotype of Klinefelter syndrome (47,XXY).
Neonatal FGFR3 mutation screening showed that the newborn was heterozygous for the classic achondroplasia
G340R mutation. Microsatellite marker analysis showed that the sex chromosome aneuploidy had arisen from a
non-disjunction error in paternal meiosis I, with a recombination event in the pseudoautosomal region 1 (PAR1).
Conclusion: Specific mutation analysis is appropriate to confirm the clinical diagnosis of achondroplasia for
appropriate diagnosis, prognosis, and genetic counseling, especially when the karyotype does not explain the
abnormal prenatal sonographic findings. In the present case, a recombination event was observed in the PAR1
region, although recombinational events in paternally derived Klinefelter syndrome cases are much rarer than
expected

Barroso, Eva

Colino, Esmeralda

Heath, Karen Elise

Martínez-Payo, Cristina

Regidor, Francisco J.

Ros Pérez, Purificación

BMC Pediatrics

PubMed

Purificación Ros-Pérez

Francisco J Regidor

Esmeralda Colino

Cristina Martínez-Payo

Eva Barroso

Karen E Heath

Crossref

Ros-Pérez et al. BMC Pediatrics 2012, 12:88http://www.biomedcentral.com/1471-2431/12/88CASE REPORT Open AccessAchondroplasia with 47, xxy karyotype: a casereport of the neonatal diagnosis of an extremelyunusual associationPurificación Ros-Pérez1*, Francisco J Regidor1, Esmeralda Colino1, Cristina Martínez-Payo2, Eva Barroso3and Karen E Heath3AbstractBackground: The association of achondroplasia and Klinefelter syndrome is extremely rare. To date, five cases havebeen previously reported, all of them diagnosed beyond the postnatal period, and only one was molecularlycharacterized. We describe the first case of this unusual association diagnosed in the neonatal period, the clinicalfindings and the molecular studies undertaken.Case presentation: The boy was born at term with clinical and radiological features indicating the diagnosis ofachondroplasia or hypochondroplasia combined with the prenatal karyotype of Klinefelter syndrome (47,XXY).Neonatal FGFR3 mutation screening showed that the newborn was heterozygous for the classic achondroplasiaG340R mutation. Microsatellite marker analysis showed that the sex chromosome aneuploidy had arisen from anon-disjunction error in paternal meiosis I, with a recombination event in the pseudoautosomal region 1 (PAR1).Conclusion: Specific mutation analysis is appropriate to confirm the clinical diagnosis of achondroplasia forappropriate diagnosis, prognosis, and genetic counseling, especially when the karyotype does not explain theabnormal prenatal sonographic findings. In the present case, a recombination event was observed in the PAR1region, although recombinational events in paternally derived Klinefelter syndrome cases are much rarer thanexpected.Keywords: Klinefelter syndrome, Achondroplasia, Mutation, Karyotype, Prenatal diagnosisBackgroundThe association of achondroplasia and Klinefelter syndromeis extremely rare. To our knowledge, only five cases havebeen reported previously [1-5], all well beyond the immedi-ate postnatal period, and mutation analysis was performedin only one case [5]. In all cases the achondroplasia FGFR3gene defect dominated the clinical picture, even prenatally,and the Klinefelter syndrome is not able to counter theachondroplasia’s effects on height. Klinefelter syndrome isreadily diagnosed by karyotype analysis, but the diagnosticconfirmation of the skeletal dysplasia requires a specificmutation analysis, necessary for genetic counseling andprognosis, and to determine perinatal lethality.* Correspondence: prosmon@hotmail.com1Department of Pediatrics, Hospital Universitario Puerta de Hierro-Majadahonda, C/Manuel de Falla 1, Majadahonda, 28222, Madrid, SpainFull list of author information is available at the end of the article© 2012 Ros-Pérez et al.; licensee BioMed CentCommons Attribution License (http://creativecreproduction in any medium, provided the orWe clinically and molecularly describe here the firstcase of this extremely unusual association that wasdiagnosed in the neonatal period, and emphasize the im-portance of performing specific genetic studies whenthere are prenatal ultrasound findings suggestive of skel-etal dysplasia. It is noteworthy that in our case a recom-bination event was observed in the PAR1, although ahighly significant reduction in recombination has beenobserved in paternally derived Klinefelter syndromecases.Case presentationThe boy was born at term (41 weeks according to gesta-tional age) after an uneventful pregnancy. Birth weightwas 3000 g (-0.77 standard deviations, SD), birth length47 cm (-1.76 SD) and head circumference 36 cm (+ 0.6SD), according to Spanish neonatal standards [6,7]. Heral Ltd. This is an Open Access article distributed under the terms of the Creativeommons.org/licenses/by/2.0), which permits unrestricted use, distribution, andiginal work is properly cited.Ros-Pérez et al. BMC Pediatrics 2012, 12:88 Page 2 of 4http://www.biomedcentral.com/1471-2431/12/88was the second child of healthy parents of normal height(mother -0.6 SD, father - 1 SD). The mother was 37 yearsold and the father was 43 years old at the time of con-ception. There was no history of consanguinity. Onebrother was healthy. During pregnancy, a routine sonog-raphy was carried out at a different institution at27 + 2 weeks and the fetus was detected to have abnor-mal head morphology with small body and limbs withno other significant abnormalities. Prenatal analysis wasundertaken, revealing a 47,XXY karyotype, correspond-ing to Klinefelter syndrome. Genetic counseling wasgiven accordingly and no further studies were under-taken at that time.On physical examination at birth, the newborn had rhizo-melic shortening, a large head with protruding forehead,mid-facial hypoplasia, depressed nasal bridge, hypoplasticchin, low set ears, and short neck (Figure 1A). The abdo-men was protruding and there was evidence of decreasinganterior-posterior chest diameter, and lumbar lordosis.Signs of trident hand were present (Figure 1B). The exter-nal genitalia were unremarkable, with testes present in thescrotum that appeared normal (Figure 1C).Radiological studies revealed decreased interpediculardistances, anterior beaking and posterior scalloping of thelumbar vertebrae (Figure 1D). The sacro-coccyx was curvedposteriorly with small square iliac wing and the horizontalDBACFigure 1 Clinical and radiological findings. A. Patients general appearanforehead, mid facial hypoplasia, depressed nasal bridge, hypoplasic chin, shshortness of legs with metaphyseal flaring.acetabulum roof had champagne glass appearance. Theneonate had bilateral short humeri, radii and ulnae withmetaphyseal flaring, as well as a short tibia and fibula withmetaphyseal flaring, mildly increased fibular length and ageneralized brachydactylia with bullet shaped proximal andmiddle phalanges. The clinical and radiological featuresindicated a diagnosis of achondroplasia or hypochondropla-sia combined with the prenatal karyotype of Klinefelter syn-drome. Hormonal analysis was also undertaken at day 3.LH (< 0.1 UI/L), FSH (< 0.3 UI/L) and testosterone(89.5 ng/dl) levels were within the normal range for age.Mutation screening of exons 8 and 11 of FGFR3(NM_000142) was undertaken by PCR and direct sequen-cing. Mutations in these two exons account for >98% ofachondroplasia and >70% of hypochondroplasia cases, in-cluding the most frequently observed mutations in achon-droplasia (p.G380R) and hypochondroplasia (p.N540K).The patient was shown to be heterozygous for the classicalc.1138 G>A mutation which results in a Glycine to Argin-ine substitution at position 380 (p.G380R) within the trans-membrane domain of the mature protein.The 47,XXY karyotype was confirmed postnatally in30 metaphases. Analysis of microsatellite markers loca-lized along the X chromosome, including the pseudoau-tosomal region 1 (PAR1), was carried out as previouslydescribed [8,9] and in accordance to the kit (Devyserce with rhizomelic limb shortening. B. A large head with protrudingort neck. C. Short trident hands. D. Radiograph showing bowing andRos-Pérez et al. BMC Pediatrics 2012, 12:88 Page 3 of 4http://www.biomedcentral.com/1471-2431/12/88Compact). The aneuploidy was shown to be of paternalorigin with a recombination event present between mar-kers DXYS10082 and DXYS10097 (Figure 2).At the age of one year, the patient presented typicalachondroplastic body proportions, normal neurologicaldevelopment except for axial hypotonia, and the height,weight and head circumference were -4.9 SD and -3.8SD and -0.34 SD respectively, according to the Spanishpopulation [6,7]. The patient developed a severe kyphos-coliotic deformity affecting the lower thoracic and upperlumbar spine.DiscussionTo our knowledge, this is the first report of the extremelyunusual association of achondroplasia and Klinefeltersyndrome that was diagnosed in the neonatal period.Only five cases have been previously reported, includinga 28 month old boy [4], one child [1], one teenager [5],and two adults [2,3]. The incidence of Klinefelter syn-drome and achondroplasia occurring together is esti-mated at 1 in 25 million births using recent data for therespective disorders [10,11].In previuously reported cases (1-5) the initial diagnosiswas achondroplasia, based on the clinical findings of fa-cial appearance, severe short stature and body propor-tions. Similarly, in our case, height was dominated bythe effect of the FGFR3 mutation rather than by theXXY aneuploidy.Figure 2 Analysis of PAR1 and X-chromosome specific microsatellitechromosome is of paternal origin. A recombination is observed in PAR1 benot informative. X1, X2 and X4 are X-chromosome markers included in theBased on the karyotype analysis ordered because of ab-normal sonographic findings, our case was initially diag-nosed prenatally in a different institution of non-mosaicKlinefelter syndrome. At birth, achondroplasia was clin-ically suspected and mutation analysis confirmed thesuspicion. Our case is of great clinical interest, as itdocuments the interest of mutation screening when son-ography during pregnancy reveals findings suggestive ofa skeletal dysplasia, especially when the karyotype doesnot explain the abnormal sonographic findings.The p.G380R substitution in the transmembrane domainof the FGFR3 protein, as identified in this case, is present in>98% of achondroplasia patients, and may either havearisen sporadically or be due to germline mosaicism. Morethan 90% of achondroplasia cases are sporadic and there isan association of increased incidence with advancing pater-nal age at the time of conception of affected individuals, asin this case, suggesting that de novo mutations are of pater-nal origin [10]. Recently, Almeida et al. [12] emphasized theclinical heterogeneity of skeletal dysplasias (achondroplasiaand hypochondroplasia) associated with FGFR3 mutations,and the importance of undertaking mutation analysis toconfirm the clinical diagnosis and to establish an appropri-ate prognosis and genetic counseling [12].Analysis of PAR1 microsatellite markers revealed thatthe extra sex chromosome was of paternal origin, arisingfrom the fusion of an XY spermatozoon and an X ovum.The frequency of XY sperm increases with paternal agemarkers in the studied family. The markers show that the extra Xtween markers DXYS10085 and DXYS10087. Marker DXYS10084 wasDevyser Compact kit.Ros-Pérez et al. BMC Pediatrics 2012, 12:88 Page 4 of 4http://www.biomedcentral.com/1471-2431/12/88[13], thus increasing the risk of fathering boys withKlinefelter syndrome. Interestingly, in our case a recom-bination event was observed in PAR1, although a highlysignificant reduction in recombination has beenobserved in paternally derived cases of Klinefelter syn-drome and in diploid 24, XY spermatozoa reviewed in[14].Fertility prognosis in these cases is unclear. Thereis one report of preserved fertility in a non-mosaicKlinefelter patient with a mutation in FGFR3 (5). Theauthors speculate that the classical FGFR3 mutation(p.G380R) found in this patient may stimulate spermato-gonial proliferation and/or prevent apoptosis, givinggerm cells a selective advantage. In our case the LH,FSH and testosterone levels were in the normal range atthe third day of life. However, a more prolonged followup is necessary to determine the function of thehypothalamic-pituitary-gonadal axis and the potentialfor fertility.ConclusionsIn summary, mutation screening is appropriate whensonography during pregnancy reveals findings suggestiveof a skeletal dysplasia, especially when the karyotypedoes not explain the abnormal sonographic findings.The presence of FGFR3 mutations dominates the clinicalpicture and its identification is important not only forgenetic counseling and recurrence risk, but also to deter-mine perinatal lethality, the severity of the dysplasia andprognosis. The coordinated collaboration between gyne-cologists, pediatricians and geneticists is appropriate.ConsentWritten informed consent was obtained from bothparents for publication of this Case report and anyaccompanying images. A copy of the informed con-sent is available for review by the Series Editor ofBMC Pediatrics.Ethical approvalThe genetic analysis was approved by the local ethicalcommittee, Hospital Universitario La Paz. All studieswere in compliance with the Helsinki Declaration.Competing interestsThe authors declare that there are no competing interests, either financial ornon-financial, that could be perceived as prejudicing the impartiality of theresearch reported.Authors’ contributionsPRP conceived the report. PRP, FJR, EC and CMP carried out clinicalexaminations and diagnostic interpretations. EB and KEH: designed,performed and interpreted the genetic studies. PRP, FJR, EC, CMP and KEHwrote and revised the manuscript. All authors read and approved the finalmanuscript.Author details1Department of Pediatrics, Hospital Universitario Puerta de Hierro-Majadahonda, C/Manuel de Falla 1, Majadahonda, 28222, Madrid, Spain.2Department of Gynecology and Obstetrics, Hospital Universitario Puerta deHierro-Majadahonda, Madrid, Spain. 3Institute for Medical and MolecularGenetics (INGEMM), Hospital Universitario La Paz and Instituto para laInvestigación de La Paz (IdiPAZ), and CIBERER, ISCIII, Madrid, Spain.Received: 10 March 2012 Accepted: 18 June 2012Published: 29 June 2012References1. Sendrail M, Gleizes M, Sendrail-Pesqué M, Colombiés P: PolygonosomieKlinefeltérienne et achondroplasie. Sem Hop París 1967, 43:1217–1225.2. Kulakova TA: Ignat’ev luT, Achondroplasia associated with Klinefelter’ssyndrome. Klin Med (Mosk) 1986, 64:126–128.3. Sayli BS, Gül D, Cakirbay H: Letter to editor: Achondroplasia with XXYkaryotype. Clin Genet 1994, 45:217–218.4. Soltanzadeh MH, Nabavi SS: Achondroplasia with Klinefelter’s syndrome.Med J Iran Hosp 2000, 3:59–60.5. Juul A, Aksglaede L, Lund AM, Duno M, Skakkbaek NE, Rajpert-De Meyts:Preserved fertility in a non-mosaic Klinefelter patient with a mutation inthe fibroblast growth factor receptor 3 gene: Case report. Hum Reprod2007, 22:1907–1911.6. Carrascosa Lezcano A, Ferrández Longás, Yeste Fernández D, García-DihinxVillanova Jy, Romo Montejo A: Estudio trasversal Español de crecimiento2008. Parte I: valores de peso y longitud en recién nacidos de 26 -42semanas de edad gestacional. An Pediatr 2008, 68:544–551.7. Carrascosa Lezcano A, Fernández García JM, Fernández Ramos C, FerrándezLongás A, López-Siguero JP, Sánchez González E, Sobradillo B, Ruiz D, YesteFernández: Estudio trasversal Español de crecimiento 2008. Parte II:valores de talla, peso e índice de masa corporal desde el nacimientohasta la talla adulta. An Pediatr 2008, 68:552–569.8. Benito-Sanz S, Thomas NS, Huber C, Gorbenko Del Blanco D, Aza-CarmonaM, Crolla JA, Maloney V, Argente J, Campos-Barros A, Cormier-Daire V, HeathKE: A novel class of pseudoautosomal region 1 (PAR1) deletionsdownstream of SHOX is associated with Léri-Weill dyschondrosteosis(LWD). Am J Hum Genet 2005, 77:533–544.9. Benito-Sanz S, Gorbenko Del Blanco D, Huber C, Thomas NS, Aza-CarmonaM, Bunyan D, Maloney V, Argente J, Cormier-Daire V, Campos-Barros A,Heath KE: Characterization of SHOX deletions in Leri-Weilldyschondrosteosis (LWD) reveals genetic heterogeneity and norecombination hotspots. Am J Hum Genet 2006, 79:409–414.10. Martínez-Frías ML, de Frutos CA, Bermejo E: ECEMC Working Group, NietoM.A, Review of the recently defined molecular mechanisms underlyingthanatophoric dysplasia and their potencial therapeutic implications foracondroplasia, Part A. Am J Med Genet 2010, 152:A242–A255.11. Morris JK, Alberman E, Scott C, Jacobs P: Is the prevalence of Klinefeltersyndrome increasing? Eur J Hum Genet 2008, 16:163–170.12. Almeida MR, Campos Xavier AB, Medeira A, Cordeiro I, Sousa AB, Lima M,Soares G, Rocha M, Saraiva J, Ramos L, Sousa S, Marcelino JP, Correia A,Santos HG: Clinical and Molecular diagnosis of the skeletal dysplasiaassociated with mutations in the gene encoding Fibroblast GrowthFactor Receptor 3 (FGFR3) in Portugal. Clin Genet 2009, 75:150–156.13. Lowe X, Eskenazi B, Nelson DO, Kidd S, Alme A, Wyrobek AJ: Frequency ofXY sperm increases with age in fathers of boys with Klinefeltersyndrome. Am J Hum Genet 2001, 69:1046–1054.14. Thomas NS, Hassold TJ: Aberrant recombination and the origin ofKlinefelter syndrome. Hum Reprod Updat 2003, 9:309–317.doi:10.1186/1471-2431-12-88Cite this article as: Ros-Pérez et al.: Achondroplasia with 47, xxykaryotype: a case report of the neonatal diagnosis of an extremelyunusual association. BMC Pediatrics 2012 12:88.

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Achondroplasia with 47, xxy karyotype: a case report of the neonatal diagnosis of an extremely unusual association

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Ros-Pérez et al. BMC Pediatrics 2012, 12:88
http://www.biomedcentral.com/1471-2431/12/88CASE REPORT Open AccessAchondroplasia with 47, xxy karyotype: a case
report of the neonatal diagnosis of an extremely
unusual association
Purificación Ros-Pérez1*, Francisco J Regidor1, Esmeralda Colino1, Cristina Martínez-Payo2, Eva Barroso3
and Karen E Heath3Abstract
Background: The association of achondroplasia and Klinefelter syndrome is extremely rare. To date, five cases have
been previously reported, all of them diagnosed beyond the postnatal period, and only one was molecularly
characterized. We describe the first case of this unusual association diagnosed in the neonatal period, the clinical
findings and the molecular studies undertaken.
Case presentation: The boy was born at term with clinical and radiological features indicating the diagnosis of
achondroplasia or hypochondroplasia combined with the prenatal karyotype of Klinefelter syndrome (47,XXY).
Neonatal FGFR3 mutation screening showed that the newborn was heterozygous for the classic achondroplasia
G340R mutation. Microsatellite marker analysis showed that the sex chromosome aneuploidy had arisen from a
non-disjunction error in paternal meiosis I, with a recombination event in the pseudoautosomal region 1 (PAR1).
Conclusion: Specific mutation analysis is appropriate to confirm the clinical diagnosis of achondroplasia for
appropriate diagnosis, prognosis, and genetic counseling, especially when the karyotype does not explain the
abnormal prenatal sonographic findings. In the present case, a recombination event was observed in the PAR1
region, although recombinational events in paternally derived Klinefelter syndrome cases are much rarer than
expected.
Keywords: Klinefelter syndrome, Achondroplasia, Mutation, Karyotype, Prenatal diagnosisBackground
The association of achondroplasia and Klinefelter syndrome
is extremely rare. To our knowledge, only five cases have
been reported previously [1-5], all well beyond the immedi-
ate postnatal period, and mutation analysis was performed
in only one case [5]. In all cases the achondroplasia FGFR3
gene defect dominated the clinical picture, even prenatally,
and the Klinefelter syndrome is not able to counter the
achondroplasia’s effects on height. Klinefelter syndrome is
readily diagnosed by karyotype analysis, but the diagnostic
confirmation of the skeletal dysplasia requires a specific
mutation analysis, necessary for genetic counseling and
prognosis, and to determine perinatal lethality.* Correspondence: prosmon@hotmail.com
1Department of Pediatrics, Hospital Universitario Puerta de Hierro-
Majadahonda, C/Manuel de Falla 1, Majadahonda, 28222, Madrid, Spain
Full list of author information is available at the end of the article
© 2012 Ros-Pérez et al.; licensee BioMed Cent
Commons Attribution License (http://creativec
reproduction in any medium, provided the orWe clinically and molecularly describe here the first
case of this extremely unusual association that was
diagnosed in the neonatal period, and emphasize the im-
portance of performing specific genetic studies when
there are prenatal ultrasound findings suggestive of skel-
etal dysplasia. It is noteworthy that in our case a recom-
bination event was observed in the PAR1, although a
highly significant reduction in recombination has been
observed in paternally derived Klinefelter syndrome
cases.
Case presentation
The boy was born at term (41 weeks according to gesta-
tional age) after an uneventful pregnancy. Birth weight
was 3000 g (-0.77 standard deviations, SD), birth length
47 cm (-1.76 SD) and head circumference 36 cm (+ 0.6
SD), according to Spanish neonatal standards [6,7]. Heral Ltd. This is an Open Access article distributed under the terms of the Creative
ommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and
iginal work is properly cited.
Ros-Pérez et al. BMC Pediatrics 2012, 12:88 Page 2 of 4
http://www.biomedcentral.com/1471-2431/12/88was the second child of healthy parents of normal height
(mother -0.6 SD, father - 1 SD). The mother was 37 years
old and the father was 43 years old at the time of con-
ception. There was no history of consanguinity. One
brother was healthy. During pregnancy, a routine sonog-
raphy was carried out at a different institution at
27 + 2 weeks and the fetus was detected to have abnor-
mal head morphology with small body and limbs with
no other significant abnormalities. Prenatal analysis was
undertaken, revealing a 47,XXY karyotype, correspond-
ing to Klinefelter syndrome. Genetic counseling was
given accordingly and no further studies were under-
taken at that time.
On physical examination at birth, the newborn had rhizo-
melic shortening, a large head with protruding forehead,
mid-facial hypoplasia, depressed nasal bridge, hypoplastic
chin, low set ears, and short neck (Figure 1A). The abdo-
men was protruding and there was evidence of decreasing
anterior-posterior chest diameter, and lumbar lordosis.
Signs of trident hand were present (Figure 1B). The exter-
nal genitalia were unremarkable, with testes present in the
scrotum that appeared normal (Figure 1C).
Radiological studies revealed decreased interpedicular
distances, anterior beaking and posterior scalloping of the
lumbar vertebrae (Figure 1D). The sacro-coccyx was curved
posteriorly with small square iliac wing and the horizontalD
BA
C
Figure 1 Clinical and radiological findings. A. Patients general appearan
forehead, mid facial hypoplasia, depressed nasal bridge, hypoplasic chin, sh
shortness of legs with metaphyseal flaring.acetabulum roof had champagne glass appearance. The
neonate had bilateral short humeri, radii and ulnae with
metaphyseal flaring, as well as a short tibia and fibula with
metaphyseal flaring, mildly increased fibular length and a
generalized brachydactylia with bullet shaped proximal and
middle phalanges. The clinical and radiological features
indicated a diagnosis of achondroplasia or hypochondropla-
sia combined with the prenatal karyotype of Klinefelter syn-
drome. Hormonal analysis was also undertaken at day 3.
LH (< 0.1 UI/L), FSH (< 0.3 UI/L) and testosterone
(89.5 ng/dl) levels were within the normal range for age.
Mutation screening of exons 8 and 11 of FGFR3
(NM_000142) was undertaken by PCR and direct sequen-
cing. Mutations in these two exons account for >98% of
achondroplasia and >70% of hypochondroplasia cases, in-
cluding the most frequently observed mutations in achon-
droplasia (p.G380R) and hypochondroplasia (p.N540K).
The patient was shown to be heterozygous for the classical
c.1138 G>A mutation which results in a Glycine to Argin-
ine substitution at position 380 (p.G380R) within the trans-
membrane domain of the mature protein.
The 47,XXY karyotype was confirmed postnatally in
30 metaphases. Analysis of microsatellite markers loca-
lized along the X chromosome, including the pseudoau-
tosomal region 1 (PAR1), was carried out as previously
described [8,9] and in accordance to the kit (Devyserce with rhizomelic limb shortening. B. A large head with protruding
ort neck. C. Short trident hands. D. Radiograph showing bowing and
Ros-Pérez et al. BMC Pediatrics 2012, 12:88 Page 3 of 4
http://www.biomedcentral.com/1471-2431/12/88Compact). The aneuploidy was shown to be of paternal
origin with a recombination event present between mar-
kers DXYS10082 and DXYS10097 (Figure 2).
At the age of one year, the patient presented typical
achondroplastic body proportions, normal neurological
development except for axial hypotonia, and the height,
weight and head circumference were -4.9 SD and -3.8
SD and -0.34 SD respectively, according to the Spanish
population [6,7]. The patient developed a severe kyphos-
coliotic deformity affecting the lower thoracic and upper
lumbar spine.
Discussion
To our knowledge, this is the first report of the extremely
unusual association of achondroplasia and Klinefelter
syndrome that was diagnosed in the neonatal period.
Only five cases have been previously reported, including
a 28 month old boy [4], one child [1], one teenager [5],
and two adults [2,3]. The incidence of Klinefelter syn-
drome and achondroplasia occurring together is esti-
mated at 1 in 25 million births using recent data for the
respective disorders [10,11].
In previuously reported cases (1-5) the initial diagnosis
was achondroplasia, based on the clinical findings of fa-
cial appearance, severe short stature and body propor-
tions. Similarly, in our case, height was dominated by
the effect of the FGFR3 mutation rather than by the
XXY aneuploidy.Figure 2 Analysis of PAR1 and X-chromosome specific microsatellite
chromosome is of paternal origin. A recombination is observed in PAR1 be
not informative. X1, X2 and X4 are X-chromosome markers included in theBased on the karyotype analysis ordered because of ab-
normal sonographic findings, our case was initially diag-
nosed prenatally in a different institution of non-mosaic
Klinefelter syndrome. At birth, achondroplasia was clin-
ically suspected and mutation analysis confirmed the
suspicion. Our case is of great clinical interest, as it
documents the interest of mutation screening when son-
ography during pregnancy reveals findings suggestive of
a skeletal dysplasia, especially when the karyotype does
not explain the abnormal sonographic findings.
The p.G380R substitution in the transmembrane domain
of the FGFR3 protein, as identified in this case, is present in
>98% of achondroplasia patients, and may either have
arisen sporadically or be due to germline mosaicism. More
than 90% of achondroplasia cases are sporadic and there is
an association of increased incidence with advancing pater-
nal age at the time of conception of affected individuals, as
in this case, suggesting that de novo mutations are of pater-
nal origin [10]. Recently, Almeida et al. [12] emphasized the
clinical heterogeneity of skeletal dysplasias (achondroplasia
and hypochondroplasia) associated with FGFR3 mutations,
and the importance of undertaking mutation analysis to
confirm the clinical diagnosis and to establish an appropri-
ate prognosis and genetic counseling [12].
Analysis of PAR1 microsatellite markers revealed that
the extra sex chromosome was of paternal origin, arising
from the fusion of an XY spermatozoon and an X ovum.
The frequency of XY sperm increases with paternal agemarkers in the studied family. The markers show that the extra X
tween markers DXYS10085 and DXYS10087. Marker DXYS10084 was
Devyser Compact kit.
Ros-Pérez et al. BMC Pediatrics 2012, 12:88 Page 4 of 4
http://www.biomedcentral.com/1471-2431/12/88[13], thus increasing the risk of fathering boys with
Klinefelter syndrome. Interestingly, in our case a recom-
bination event was observed in PAR1, although a highly
significant reduction in recombination has been
observed in paternally derived cases of Klinefelter syn-
drome and in diploid 24, XY spermatozoa reviewed in
[14].
Fertility prognosis in these cases is unclear. There
is one report of preserved fertility in a non-mosaic
Klinefelter patient with a mutation in FGFR3 (5). The
authors speculate that the classical FGFR3 mutation
(p.G380R) found in this patient may stimulate spermato-
gonial proliferation and/or prevent apoptosis, giving
germ cells a selective advantage. In our case the LH,
FSH and testosterone levels were in the normal range at
the third day of life. However, a more prolonged follow
up is necessary to determine the function of the
hypothalamic-pituitary-gonadal axis and the potential
for fertility.
Conclusions
In summary, mutation screening is appropriate when
sonography during pregnancy reveals findings suggestive
of a skeletal dysplasia, especially when the karyotype
does not explain the abnormal sonographic findings.
The presence of FGFR3 mutations dominates the clinical
picture and its identification is important not only for
genetic counseling and recurrence risk, but also to deter-
mine perinatal lethality, the severity of the dysplasia and
prognosis. The coordinated collaboration between gyne-
cologists, pediatricians and geneticists is appropriate.
Consent
Written informed consent was obtained from both
parents for publication of this Case report and any
accompanying images. A copy of the informed con-
sent is available for review by the Series Editor of
BMC Pediatrics.
Ethical approval
The genetic analysis was approved by the local ethical
committee, Hospital Universitario La Paz. All studies
were in compliance with the Helsinki Declaration.
Competing interests
The authors declare that there are no competing interests, either financial or
non-financial, that could be perceived as prejudicing the impartiality of the
research reported.
Authors’ contributions
PRP conceived the report. PRP, FJR, EC and CMP carried out clinical
examinations and diagnostic interpretations. EB and KEH: designed,
performed and interpreted the genetic studies. PRP, FJR, EC, CMP and KEH
wrote and revised the manuscript. All authors read and approved the final
manuscript.Author details
1Department of Pediatrics, Hospital Universitario Puerta de Hierro-
Majadahonda, C/Manuel de Falla 1, Majadahonda, 28222, Madrid, Spain.
2Department of Gynecology and Obstetrics, Hospital Universitario Puerta de
Hierro-Majadahonda, Madrid, Spain. 3Institute for Medical and Molecular
Genetics (INGEMM), Hospital Universitario La Paz and Instituto para la
Investigación de La Paz (IdiPAZ), and CIBERER, ISCIII, Madrid, Spain.
Received: 10 March 2012 Accepted: 18 June 2012
Published: 29 June 2012
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Cite this article as: Ros-Pérez et al.: Achondroplasia with 47, xxy
karyotype: a case report of the neonatal diagnosis of an extremely
unusual association. BMC Pediatrics 2012 12:88.


Cakirbay H: Letter to editor:

Characterization of SHOX deletions in Leri-Weill dyschondrosteosis (LWD) reveals genetic heterogeneity and no recombination hotspots.

Colombiés P: Polygonosomie Klinefeltérienne et achondroplasie. Sem Hop París

E: ECEMC Working Group, Nieto M.A, Review of the recently defined molecular mechanisms underlying thanatophoric dysplasia and their potencial therapeutic implications for acondroplasia, Part A. Am J Med Genet

Ferrández Longás, Yeste Fernández D, García-Dihinx Villanova Jy, Romo Montejo A: Estudio trasversal Español de crecimiento

HG: Clinical and Molecular diagnosis of the skeletal dysplasia associated with mutations in the gene encoding Fibroblast Growth Factor Receptor 3 (FGFR3) in Portugal. Clin Genet

Ignat’ev luT, Achondroplasia associated with Klinefelter’s syndrome. Klin Med (Mosk)

Is the prevalence of Klinefelter syndrome increasing?

KE: A novel class of pseudoautosomal region 1 (PAR1) deletions downstream of SHOX is associated with Léri-Weill dyschondrosteosis (LWD).

Nabavi SS: Achondroplasia with Klinefelter’s syndrome.

Rajpert-De Meyts: Preserved fertility in a non-mosaic Klinefelter patient with a mutation in the fibroblast growth factor receptor 3 gene: Case report. Hum Reprod

valores de peso y longitud en recién nacidos de 26 -42 semanas de edad gestacional. An Pediatr

Wyrobek AJ: Frequency of XY sperm increases with age in fathers of boys with Klinefelter syndrome.

Yeste Fernández: Estudio trasversal Español de crecimiento 2008. Parte II: valores de talla, peso e índice de masa corporal desde el nacimiento hasta la talla adulta. An Pediatr

file:///data/remote/core/dit/data/Springer-OA/pdf/38e/aHR0cDovL2xpbmsuc3ByaW5nZXIuY29tLzEwLjExODYvMTQ3MS0yNDMxLTEyLTg4LnBkZg==.pdf

Achondroplasia with 47, xxy karyotype: a case report of the neonatal diagnosis of an extremely unusual association

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