TGIF Mutations in Human Holoprosencephaly: Correlation between Genotype and Phenotype | Zendy

Amelia A. Keaton | Zendy; Ben Solomon | Zendy; Emily F. Kauvar | Zendy; Kênia Balbi El-Jaick | Zendy; Andrea Gropman | Zendy; Y. Zafer | Zendy; Jeanne Meck | Zendy; Sherri J. Bale | Zendy; Dorothy K. Grange | Zendy; Bassem R. Haddad | Zendy; Gordon C. Gowans | Zendy; Nancy J. Clegg | Zendy; Mauricio R. Delgado | Zendy; Jin S. Hahn | Zendy; Daniel PinedaAlvarez | Zendy; Felicitas Lacbawan | Zendy; Jorge I. Vélez | Zendy; Erich Roessler | Zendy; Maximilian Muenke | Zendy

AI Assistant Blog Pricing

Home ZAIA Blog

Open Access

TGIF Mutations in Human Holoprosencephaly: Correlation between Genotype and Phenotype

Author(s) -

Amelia A. Keaton,

Ben Solomon,

Emily F. Kauvar,

Kênia Balbi El-Jaick,

Andrea Gropman,

Y. Zafer,

Jeanne Meck,

Sherri J. Bale,

Dorothy K. Grange,

Bassem R. Haddad,

Gordon C. Gowans,

Nancy J. Clegg,

Mauricio R. Delgado,

Jin S. Hahn,

Daniel PinedaAlvarez,

Felicitas Lacbawan,

Jorge I. Vélez,

Erich Roessler,

Maximilian Muenke

Publication year - 2010

Publication title -

molecular syndromology

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 0.609

H-Index - 36

eISSN - 1661-8777

pISSN - 1661-8769

DOI - 10.1159/000328203

Subject(s) - holoprosencephaly , genetics , phenotype , haploinsufficiency , biology , craniofacial , gene , mutation , bioinformatics , fetus , pregnancy

Holoprosencephaly (HPE), which results from failed or incomplete midline forebrain division early in gestation, is the most common forebrain malformation. The etiology of HPE is complex and multifactorial. To date, at least 12 HPE-associated genes have been identified, including TGIF (transforming growth factor beta-induced factor), located on chromosome 18p11.3. TGIF encodes a transcriptional repressor of retinoid responses involved in TGF-β signaling regulation, including Nodal signaling. TGIF mutations are reported in approximately 1-2% of patients with non-syndromic, non-chromosomal HPE. We combined data from our comprehensive studies of HPE with a literature search for all individuals with HPE and evidence of mutations affecting TGIF in order to establish the genotypic and phenotypic range. We describe 2 groups of patients: 34 with intragenic mutations and 21 with deletions of TGIF. These individuals, which were ascertained from our research group, in collaboration with other centers, and through a literature search, include 38 probands and 17 mutation-positive relatives. The majority of intragenic mutations occur in the TGIF homeodomain. Patients with mutations affecting TGIFrecapitulate the entire phenotypic spectrum observed in non-chromosomal, non-syndromic HPE. We identified a statistically significant difference between the 2 groups with respect to inheritance, as TGIF deletions were more likely to be de novo in comparison to TGIF mutations (χ(2) ((2)) = 6.97, p(permutated) = 0.0356). In addition, patients with TGIF deletions were also found to more commonly present with manifestations beyond the craniofacial and neuroanatomical features associated with HPE (p = 0.0030). These findings highlight differences in patients with intragenic mutations versus deletions affecting TGIF, and draw attention to the homeodomain region, which appears to be particularly relevant to HPE. These results may be useful for genetic counseling of affected patients.

The content you want is available to Zendy users.

Already have an account? Click here to sign in.

Having issues? You can contact us here

Accelerating Research