Focal Facial Dermal Dysplasia 3, Setleis Type; Ffdd3
Description
The focal dermal dysplasias (FFDDs) are a group of related developmental defects characterized by bitemporal or preauricular skin lesions resembling aplasia cutis congenita. FFFD3 is an autosomal recessive disorder characterized by bitemporal skin lesions with variable facial findings, including thin and puckered periorbital skin, distichiasis and/or absent eyelashes, upslanting palpebral fissures, a flat nasal bridge with a broad nasal tip, large lips, and redundant facial skin (summary by Slavotinek et al., 2013).FFDD2 (OMIM ) is characterized by the same facial features as FFDD3, but the inheritance is autosomal dominant.For a classification and a discussion of genetic heterogeneity of FFDD, see FFDD1 (OMIM ).
Genes related to Focal Facial Dermal Dysplasia 3, Setleis Type; Ffdd3
- TWIST2
Clinical Features
Top most frequent phenotypes and symptoms related to Focal Facial Dermal Dysplasia 3, Setleis Type; Ffdd3
- Global developmental delay
- Depressed nasal bridge
- Upslanted palpebral fissure
- Sparse hair
- Scarring
- Pectus carinatum
- Anal atresia
- Bulbous nose
- Thick vermilion border
- Single transverse palmar crease
And another 14 symptoms. If you need more information about this disease we can help you.
Incidence and onset information
— Currently we don't have prevalence information about this disease (Not enough data available about incidence and published cases.)— No data available about the known clinical features onset.
Alternative names
Focal Facial Dermal Dysplasia 3, Setleis Type; Ffdd3 Is also known as focal facial dermal dysplasia, type ii, formerly, bitemporal forceps marks syndrome, facial ectodermal dysplasia, setleis syndrome.
Researches and researchers
Currently, we don't have any information about doctors, researches or researchers related to this disease. Please contact us if you would like to appear here.Focal Facial Dermal Dysplasia 3, Setleis Type; Ffdd3 Recommended genes panels
Panel Name, Specifity and genes Tested/covered |
---|
TWIST2. Complete sequencing.
By Instituto de Medicina Genomica Instituto de Medicina Genomica (Spain).
TWIST2
Specificity
100 %
Genes
100 % |
Disorders of Sex Development (DSD) and Infertility Sequencing Panel with CNV Detection.
By PreventionGenetics PreventionGenetics (United States).
ROR2, SALL1, BMP15, BMP4, SEMA3A, SEMA3E, BMP7, FOXL2, BRDT, SOS1, SOX10, SOX2, SOX3, SOX9, SRA1, SRD5A2, SRY, STAG3, STAR, AURKC , (...)
View the complete list with 187 more genes
Specificity
1 %
Genes
100 % |
Disorders of Sex Development (DSD) Sequencing Panel with CNV Detection.
By PreventionGenetics PreventionGenetics (United States).
ROR2, SALL1, BMP15, BMP4, SEMA3A, BMP7, FOXL2, SOS1, SOX10, SOX2, SOX3, SOX9, SRD5A2, SRY, STAR, TAC3, TACR3, TBX15, HNF1B, MED12 , (...)
View the complete list with 138 more genes
Specificity
1 %
Genes
100 % |
Ambiguous Genitalia Sequencing Panel with CNV Detection.
By PreventionGenetics PreventionGenetics (United States).
ROR2, SALL1, BMP4, SEMA3A, SOS1, SOX10, SOX2, SOX3, SOX9, SRD5A2, SRY, STAR, TBX15, CEP41, TSPYL1, WNT4, WNT5A, WNT7A, WT1, WWOX , (...)
View the complete list with 65 more genes
Specificity
2 %
Genes
100 % |
Barber-Say syndrome Comprehensive test.
By Connective Tissue Gene Tests (United States).
TWIST2
Specificity
100 %
Genes
100 % |
Ablepharon-macrostomia syndrome Comprehensivetest.
By Connective Tissue Gene Tests (United States).
TWIST2
Specificity
100 %
Genes
100 % |
Barber-Say syndrome Deletion / Duplication test.
By Connective Tissue Gene Tests (United States).
TWIST2
Specificity
100 %
Genes
100 % |
Ablepharon-macrostomia syndrome Deletion / Duplication test.
By Connective Tissue Gene Tests (United States).
TWIST2
Specificity
100 %
Genes
100 % |
You can get up to 10 more panels with our dedicated tool
Learn moreSources and references
You can check the following sources for additional information.
OMIM Rare Disease Symptoms CheckerIf you liked this article maybe you will also find interesting the following in-depth articles about other rare diseases, like PYROPOIKILOCYTOSIS, HEREDITARY; HPP EMANUEL SYNDROME PIGMENTED PARAVENOUS CHORIORETINAL ATROPHY; PPCRA RETINAL CONE DYSTROPHY 3B; RCD3B