A Novel Heterozygous Intragenic Sequence Variant in DLX6 Probably Underlies First Case of Autosomal Dominant Split-Hand/Foot Malformation Type 1

Ullah, Asmat; Hammid, Anam; Umair, Muhammad; Ahmad, Farooq

doi:10.1159/000453350

Cited by 23 publications

(26 citation statements)

References 32 publications

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“…Data presented in these 3 reports and identification of the frameshift mutation (p.Ser137Alafs*19) in the family, presented here, supported the involvement of the EPS15L1 gene on chromosome 19p13.3‐p12 in causing SHFM phenotype. It is pertinent to report here that associated features reported with SHFM1, SHFM5, and SHFM6 such as polydactyly, cardiovascular anomalies, deafness, and nail clubbing were not observed in the affected individuals of our family.…”

Section: Discussionmentioning

confidence: 77%

“…Karyotype analysis was performed on peripheral blood lymphocytes collected from the proband (IV‐2) using the G‐banding technique …”

Section: Methodsmentioning

confidence: 99%

“…This included SHFM1 on chromosome 7q21 (MIM 183600), SHFM2 on Xq32 (MIM 313350), SHFM3 on 10q24 (MIM 246560), SHFM4 on 3q27 (MIM 605289), SHFM5 on 2q31 (MIM 606708), SHFM6 on 12q13.11‐q13 (MIM 183600), and a chromosomal region 8q21.11‐q22.3 . For these 7 loci, 5 genes including DLX5 (MIM 600028) and DLX6 for SHFM1, TP63 (MIM 603273) for SHFM4, WNT10B (MIM 601906) for SHFM6 and ZAK (MIM 616890) for split‐foot malformation with mesoaxial polydactyly have been identified. Three other types of SHFM associated with long‐bone deficiency (SHFLD), have been mapped.…”

Section: Introductionmentioning

confidence: 99%

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First direct evidence of involvement of a homozygous loss‐of‐function variant in the EPS15L1 gene underlying split‐hand/split‐foot malformation

et al. 2018

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Split‐hand/split‐foot malformation (SHFM) is a severe form of congenital limb deformity characterized by the absence of 1 or more digits and/or variable degree of median clefts of hands and feet. The present study describes an investigation of a consanguineous family of Pakistani origin segregating SHFM in an autosomal recessive manner. Human genome scan using SNP markers followed by whole exome sequencing revealed a frameshift deletion (c.409delA, p.Ser137Alafs*19) in the EPS15L1 gene located on chromosome 19p13.11. This is the first biallelic variant identified in the EPS15L1 gene underlying SHFM. Our findings report the first direct involvement of EPS15L1 gene in the development of human limbs.

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Section: Discussionmentioning

confidence: 77%

“…Karyotype analysis was performed on peripheral blood lymphocytes collected from the proband (IV‐2) using the G‐banding technique …”

Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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First direct evidence of involvement of a homozygous loss‐of‐function variant in the EPS15L1 gene underlying split‐hand/split‐foot malformation

et al. 2018

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“…SHFM has been reported to be associated with ectrodactyly‐ectodermal dysplasia‐clefting syndrome (EEC; MIM #129900), brachydactyly‐ectrodactyly with fibular aplasia or hypoplasia (MIM #113310), autosomal recessive DLX5 ‐associated SHFM, autosomal dominant DLX5 ‐associated SHFM, autosomal dominant DLX6 ‐associated SHFM, FGFR1 ‐associated congenital hypogonadotropic hypogonadism with SHFM (MIM #147950), BHLHA9 ‐associated SHFM with long‐bone deficiency (SHFMLD: MIM #119100), and autosomal recessive WNT10B ‐associated SHFM (SHFM6; MIM #225300) . A patient with Kabuki syndrome with SHFM has been reported, but molecular testing was not performed .…”

Section: Shfm‐associated Syndromesmentioning

confidence: 99%

Genetic regulatory pathways of split‐hand/foot malformation

Kantaputra

Carlson

2018

Clinical Genetics

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Split-hand/foot malformation (SHFM) is caused by mutations in TP63, DLX5, DLX6, FGF8, FGFR1, WNT10B, and BHLHA9. The clinical features of SHFM caused by mutations of these genes are not distinguishable. This implies that in normal situations these SHFM-associated genes share an underlying regulatory pathway that is involved in the development of the central parts of the hands and feet. The mutations in SHFM-related genes lead to dysregulation of Fgf8 in the central portion of the apical ectodermal ridge (AER) and subsequently lead to misexpression of a number of downstream target genes, failure of stratification of the AER, and thus SHFM. Syndactyly of the remaining digits is most likely the effects of dysregulation of Fgf-Bmp-Msx signaling on apoptotic cell death. Loss of digit identity in SHFM is hypothesized to be the effects of misexpression of HOX genes, abnormal SHH gradient, or the loss of balance between GLI3A and GLI3R. Disruption of canonical and non-canonical Wnt signaling is involved in the pathogenesis of SHFM. Whatever the causative genes of SHFM are, the mutations seem to lead to dysregulation of Fgf8 in AER cells of the central parts of the hands and feet and disruption of Wnt-Bmp-Fgf signaling pathways in AER.

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“… Shamseldin et al (2012) reported a mutation in the gene DLX5 responsible for the SHFM-1 phenotype in a consanguineous family. We reported intragenic variants in the DLX5 and DLX6 genes that caused the SHFM-1 phenotype in two different families ( Ullah et al , 2016a , b ). Goodman et al (2002) proposed that SHFM-5 and other digit defects may be caused by haploinsufficiency of genes ( EVX2 , DLX1 , DLX2 ) located at the 5′ end of the HOXD cluster.…”

Section: Introductionmentioning

confidence: 99%

Homozygous sequence variants in the WNT10B gene underlie split hand/foot malformation

et al. 2018

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Split-hand/split-foot malformation (SHFM), also known as ectrodactyly is a rare genetic disorder. It is a clinically and genetically heterogeneous group of limb malformations characterized by absence/hypoplasia and/or median cleft of hands and/or feet. To date, seven genes underlying SHFM have been identified. This study described four consanguineous families (A-D) segregating SHFM in an autosomal recessive manner. Linkage in the families was established to chromosome 12p11.1–q13.13 harboring WNT10B gene. Sequence analysis identified a novel homozygous nonsense variant (p.Gln154*) in exon 4 of the WNT10B gene in two families (A and B). In the other two families (C and D), a previously reported variant (c.300_306dupAGGGCGG; p.Leu103Argfs*53) was detected. This study further expands the spectrum of the sequence variants reported in the WNT10B gene, which result in the split hand/foot malformation.

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A Novel Heterozygous Intragenic Sequence Variant in DLX6 Probably Underlies First Case of Autosomal Dominant Split-Hand/Foot Malformation Type 1

Cited by 23 publications

References 32 publications

First direct evidence of involvement of a homozygous loss‐of‐function variant in the EPS15L1 gene underlying split‐hand/split‐foot malformation

First direct evidence of involvement of a homozygous loss‐of‐function variant in the EPS15L1 gene underlying split‐hand/split‐foot malformation

Genetic regulatory pathways of split‐hand/foot malformation

Homozygous sequence variants in the WNT10B gene underlie split hand/foot malformation

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