2019
DOI: 10.3390/genes10120967
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Novel TNXB Variants in Two Italian Patients with Classical-Like Ehlers-Danlos Syndrome

Abstract: TNXB-related classical-like Ehlers-Danlos syndrome (TNXB-clEDS) is an ultrarare type of Ehlers-Danlos syndrome due to biallelic null variants in TNXB, encoding tenascin-X. Less than 30 individuals have been reported to date, mostly of Dutch origin and showing a phenotype resembling classical Ehlers-Danlos syndrome without atrophic scarring. TNXB-clEDS is likely underdiagnosed due to the complex structure of the TNXB locus, a fact that complicates diagnostic molecular testing. Here, we report two unrelated Ital… Show more

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Cited by 11 publications
(12 citation statements)
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“…TNXB deficiency [51], and the recently defined clEDS type 2 caused by biallelic variants in AEBP1 [52]. The clEDS type 1 is generally distinguishable from cEDS for the absence of atrophic scarring [28,45,[53][54][55][56][57], whereas a more severe multisystemic presentation in clEDS type 2 should assist the differential diagnosis with cEDS [43,52,[58][59][60]. The dermatosparaxis (ADAMTS2) [61], cardiac-valvular (COL1A2) [62][63][64], kyphoscoliotic (PLOD1, FKBP14) [65,66], and arthrochalasia (COL1A1, COL1A2) [67,68] EDS subtypes, also sharing with cEDS several cutaneous and articular issues, are mostly distinguishable for the presence of specific hallmarks [1,9,16].…”
Section: Discussionmentioning
confidence: 99%
“…TNXB deficiency [51], and the recently defined clEDS type 2 caused by biallelic variants in AEBP1 [52]. The clEDS type 1 is generally distinguishable from cEDS for the absence of atrophic scarring [28,45,[53][54][55][56][57], whereas a more severe multisystemic presentation in clEDS type 2 should assist the differential diagnosis with cEDS [43,52,[58][59][60]. The dermatosparaxis (ADAMTS2) [61], cardiac-valvular (COL1A2) [62][63][64], kyphoscoliotic (PLOD1, FKBP14) [65,66], and arthrochalasia (COL1A1, COL1A2) [67,68] EDS subtypes, also sharing with cEDS several cutaneous and articular issues, are mostly distinguishable for the presence of specific hallmarks [1,9,16].…”
Section: Discussionmentioning
confidence: 99%
“…Due to the complex structure of the TNXB locus, EDS molecular diagnostic workflow should include NGS for the non-homologous TNXB sequence, long PCR/Sanger sequencing for the TNXA/TNXB homology region and TNXB deletion/duplication analysis (Demirdas et al, 2017;Micale et al, 2019). The last two molecular diagnostic steps have not been performed because TNXB-related classical-like EDS (TNXB-clEDS), the ultrarare type of EDS due to biallelic null variants in TNXB, has been excluded by the proband's physical examination that revealed the presence of atrophic scarring.…”
Section: Molecular Findingsmentioning
confidence: 99%
“…229 The Tenascin X deficient patients were found to have truncating mutations or deletions in TNXB. 229,230 This has since been reclassified as classic-like EDS, a rare, autosomal recessive type of EDS. 231 Some other point mutations in TNXB have also been suggested to cause hEDS or classiclike EDS (clEDS).…”
Section: Geneticsmentioning
confidence: 99%
“…Tenascin X deficiency has been indicated in a recessive form of EDS in which patients meet major and minor diagnostic criteria of classical EDS 229 . The Tenascin X deficient patients were found to have truncating mutations or deletions in TNXB 229,230 . This has since been reclassified as classic‐like EDS, a rare, autosomal recessive type of EDS 231 .…”
Section: Geneticsmentioning
confidence: 99%