Confirmation that RIPK4 mutations cause not only Bartsocas‐Papas syndrome but also CHAND syndrome

CHAND syndrome is an autosomal recessive disorder characterized by curly hair, ankyloblepharon, and nail dysplasia. Only few patients were reported to date. A homozygous RIPK4 mutation was recently identified by homozygosity mapping and whole exome sequencing in three patients from an expanded consanguineous kindred with a clinical diagnosis of CHAND syndrome. RIPK4 was previously known to be implicated in Bartsocas‐Papas syndrome, the autosomal recessive form of popliteal pterygium syndrome. We report here two cases of RIPK4 homozygous mutations in a fetus with severe Bartsocas‐Papas syndrome and a patient with CHAND syndrome. The patient with CHAND syndrome harbored the same mutation as the one identified in the family previously reported. We thus confirm the implication of RIPK4 gene in CHAND syndrome in addition to Bartsocas‐Papas syndrome and discuss genotype/phenotype correlations.

[1]  P. Nürnberg,et al.  Identification of a novel mutation in RIPK4 in a kindred with phenotypic features of Bartsocas‐Papas and CHAND syndromes , 2015, American journal of medical genetics. Part A.

[2]  S. Kapoor,et al.  Expanding the genetic and phenotypic spectrum of popliteal pterygium disorders , 2015, American journal of medical genetics. Part A.

[3]  K. Gripp,et al.  Exome Analysis in Clinical Practice: Expanding the Phenotype of Bartsocas–Papas Syndrome , 2013, American journal of medical genetics. Part A.

[4]  S. Bhaskar,et al.  Exome sequence identifies RIPK4 as the Bartsocas-Papas syndrome locus. , 2012, American journal of human genetics.

[5]  H. Kayserili,et al.  Mutations in RIPK4 cause the autosomal-recessive form of popliteal pterygium syndrome. , 2012, American journal of human genetics.

[6]  B. Marinari,et al.  A regulatory feedback loop involving p63 and IRF6 links the pathogenesis of 2 genetically different human ectodermal dysplasias. , 2010, The Journal of clinical investigation.

[7]  H. Dinh,et al.  RIP4 regulates epidermal differentiation and cutaneous inflammation. , 2010, The Journal of investigative dermatology.

[8]  T. Rinne,et al.  Spectrum of p63 mutations in a selected patient cohort affected with ankyloblepharon‐ectodermal defects‐cleft lip/palate syndrome (AEC) , 2009, American journal of medical genetics. Part A.

[9]  S. Kondo,et al.  Prevalence and nonrandom distribution of exonic mutations in interferon regulatory factor 6 in 307 families with Van der Woude syndrome and 37 families with popliteal pterygium syndrome , 2009, Genetics in Medicine.

[10]  S. Werner,et al.  Regulation of NF-kappaB activity and keratinocyte differentiation by the RIP4 protein: implications for cutaneous wound repair. , 2007, The Journal of investigative dermatology.

[11]  J. Derry,et al.  RIP4 Is an Ankyrin Repeat-Containing Kinase Essential for Keratinocyte Differentiation , 2002, Current Biology.

[12]  D. Bertola,et al.  AEC Syndrome and CHAND Syndrome: Further Evidence of Clinical Overlapping in the Ectodermal Dysplasias , 2000, Pediatric dermatology.

[13]  J. Arimany,et al.  Two sibs with cleft palate, ankyloblepharon, alveolar synechiae, and ectodermal defects: a new recessive syndrome? , 1993, Journal of medical genetics.

[14]  S. Ozeki,et al.  Alveolar synechia, ankyloblepharon, and ectodermal disorders: an autosomal recessive disorder? , 1991, American journal of medical genetics.

[15]  H. Toriello,et al.  Re-evaluation of CHANDS. , 1979, Journal of medical genetics.

[16]  Baughman Fa CHANDS: the curly hair-ankyloblepharon-nail dysplasia syndrome. , 1971 .

[17]  F. Baughman CHANDS: the curly hair-ankyloblepharon-nail dysplasia syndrome. , 1971, Birth defects original article series.