Interstitial and terminal deletions of the long arm of chromosome 4: Further delineation of phenotypes

Lin, Angela E.; Garver, Kenneth L.; Diggans, Gerard R.; Clemens, Michele; Wenger, Sharon L.; Steele, Mark W.; Jones, Marilyn C.; Israel, Jamie

doi:10.1002/ajmg.1320310308

Cited by 102 publications

(113 citation statements)

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“…The reported terminal 4q deletions mostly involved breakpoints at 4q31 (22 patients) [4, 5, 6, 7, 8], 4q32 (4 patients) [5, 9], 4q33 (12 patients) [10, 11, 12]and 4q34 (5 patients) [4, 5, 13]. Most interstitial deletions of the long arm of the chromosome 4 involve the q11–q31 segments.…”

Section: Discussionmentioning

confidence: 99%

A New Inherited Interstitial Deletion of the Distal Long Arm of Chromosome 4,

Aladhami

Gould²,

Muhammad³

1999

Hum Hered

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A 12-year-old boy showed mild dysmorphic features, late presentation of learning difficulties and behaviour problems, obesity, breast hypertrophy and bilateral slipped capital femoral epiphysis. His mother also has mild dysmorphic features, obesity, and a similar history of late presentation of learning difficulties and behaviour problems. Cytogenetic analysis demonstrated an inherited distal long arm deletion of one chromosome 4. The boy’s karyotype was interpreted as 46,XY,del(4)(q32 q33)mat and the mother’s karyotype as 46,XX,del(4)(q32 q33). This is the second report of an inherited distal 4q deletion and the first report of interstitial chromosome 4 deletion involving q32 q33 segments.

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Section: Discussionmentioning

confidence: 99%

A New Inherited Interstitial Deletion of the Distal Long Arm of Chromosome 4,

Aladhami

Gould²,

Muhammad³

1999

Hum Hered

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“…In order to establish a genotype-phenotype correlation, the severity of the phenotype is correlated with the size of the deletion. Thus, several reports suggested that small terminal, or interstitial, distal Cr4q del involving bands 4q34 and 4q35 seems to have little clinical impact, consisting in little facial dysmorphism and mild, or absent, intellectual disability (ID) 4 , and Yakut et al 5 reported a case of a familial interstitial 4q35 deletion with no discernible phenotypic effects. On the other hand, a relatively constant phenotype can be recognised in 4q31 to qter deletion.…”

Section: Introductionmentioning

confidence: 99%

Pain insensitivity in a child with a de novo interstitial deletion of the long arm of the chromosome 4: Case report

Cascella

Muzio

2017

Rev. chil. pediatr.

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Introduction. Terminal and interstitial deletions of the distal segment of the long arm of chromosome 4 (Cr4q del) are not common genetic disorders. The severity of the phenotype is correlated with the size of the deletion because small deletions have little clinical impact, whereas large deletions are usually associated with multiple congenital anomalies, postnatal growth failure, and moderate to severe intellectual disability. Alteration in pain tolerance has not been included among these features, also in case of large deletions. The purpose of this report is to document a case of a child affected by interstitial Cr4q del, expressing pain insensitivity as clinical feature not previously described. We also offer a discussion on genetic disorders featuring pain insensitivity/indifference. Case report. A Caucasian girl aged 12 came to our observation for a developmental delay with multiple congenital abnormalities and moderate intellectual disability (IQ 47). A de novo interstitial Cr4 del between band q31.3 and q32.2 (Cr4 del q31.3 to q32.2) was found. The child also expresses no evidence of pain perception to injures which normally evoke pain. Consequently, she is affected by severe disability caused by painless injuries and self-injurious behaviours, such as excessive self-rubbing and scratching. The neurological examination manifested high pain threshold with preserved tactile sensitivity. Conclusions. This is the first report of pain insensitivity in a patient with a specific genetic deletion involving the interstitial region of the distal long arm of Cr4. Moreover, this report could serve as a useful model to better understand mechanisms of pain perception and its modulation.

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“…1,14,15 In particular, there appears to be a karyotypephenotype correlation because CVM has been noted in almost two thirds of patients with the terminal deletions at 4q31, whereas only about a quarter of patients with the more distal deletions at 4q34 or q35 have CVM. It has been postulated that genes distal to 4q34 may play a critical role in producing a CVM, 14 though the molecular basis is unknown.…”

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confidence: 99%

“…Over the past 30 years, 50 cases have been reported, 23 (41%) of which have had a cardiovascular malformation (CVM). [1][2][3][4][5][6][7][8][9][10][11][12][13][14] Compared with the 10% frequency in the Baltimore-Washington Infant Study, a case-control study of liveborn infants with a confirmed CVM in 1981-1989, 14 right ventricular outflow tract obstructive defects are more common (35%) in patients with 4q deletion.…”

mentioning

confidence: 99%