Oculoectodermal syndrome is a mosaic RASopathy associated with <i>KRAS</i> alterations

Peacock, Jacqueline D.; Dykema, Karl; Toriello, Helga V.; Mooney, Marie R.; Scholten, Donald J.; Winn, Mary E.; Borgman, Andrew; Duesbery, Nicholas S.; Hiemenga, Judith A.; Liu, Cong; Campbell, S J; Nickoloff, Brian P.; Williams, Bart O.; Steensma, Matthew R.

doi:10.1002/ajmg.a.37048

Cited by 51 publications

(54 citation statements)

References 42 publications

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“…Until recently, somatic cutaneous mosaicism was considered as a rare event with little or any clinical consequences. Recent genomic studies have recognized mutational somatic mosaicism in skin lesions with abnormal pigmentation, especially in those following the Blaschko lines (Amary et al, ; Groesser et al, ; Kurek et al, ; Peacock et al, ; Rivière et al, ; Shirley et al, ; Weinstein et al, ). The OES, ECCL, and SFMS syndromes are a group of oculocutaneous developmental mosaic RASopathies which exhibit common anomalies including focal scalp lesions, linear cutaneous hyperpigmentation, arachnoid cyst, and cardiac defects (Ardinger, Horii, & Begleiter, ; Ernst, Quinn, & Alawi, ; Moog, ).…”

Section: Discussionmentioning

confidence: 99%

“…The OES, ECCL, and SFMS syndromes are a group of oculocutaneous developmental mosaic RASopathies which exhibit common anomalies including focal scalp lesions, linear cutaneous hyperpigmentation, arachnoid cyst, and cardiac defects (Ardinger, Horii, & Begleiter, ; Ernst, Quinn, & Alawi, ; Moog, ). At the molecular level, these entities are caused by somatic mosaicism for mutations in genes encoding components of the RAS signaling pathway (Bennett et al, ; Boppudi et al, ; Groesser et al, ; Peacock et al, ). OES is a very rare disease characterized for a consistent combination of scalp lesions and epibulbar dermoids (Toriello, Lacassie, Droste, & Higgins, ).…”

Section: Discussionmentioning

confidence: 99%

“…The identification of somatic mutations in KRAS and FGFR1 genes in patients with cutaneous mosaic disorders could provide a tool for early diagnosis and surveillance of associated disorders. Non‐ossifying fibromas resulting in long bones stress fractures (Ardinger et al, ; Boppudi et al, ; Fickie & Stoler, ; Mermer, Kayhan, Karacelebi, & Percin, ; Peacock et al, ), giant cell granuloma of the mandibule and maxilla (Ardinger et al, ; Boppudi et al, ; Federici et al, ; Mermer et al, ; Peacock et al, ; Toriello et al, ), rhabdomyosarcoma (Ardinger et al, ), craniofacial, intracranial or intraspinal lipomas (Hunter, ), jaw osteomas (Zielinska‐Kazmierska, Grodecka, Jablonska‐Polakowska, & Arkuszewski, ), odontomas (Andreadis, Rizos, Belazi, Peneva, & Antoniades, ; Hauber, Warmuth‐Metz, Rose, Bröcker, & Hamm, ), ossifying fibromas (Moog et al, ), pilocytic‐low grade astrocytoma (Bieser et al, ; Brassesco et al, ; Valera et al, ), papillary glioneural tumor (Phi et al, ), dysembryoplastic neuroepithelial tumor (Bavle et al, ), and optic glioma (Kocak et al, ) can occur in these three oculocutaneous syndromes. In addition, malignant secondary tumors can arise from the nevi sebaceous in SFMS patients, including basal cell carcinoma and squamous carcinoma (Eisen & Michael; Idriss & Elston, ).…”

Section: Discussionmentioning

confidence: 99%

“…Three additional syndromes with overlapping clinical findings in eye, heart, skin, and hair have been recently shown to result from somatic mosaicism for mutations in the genes involved in the Ras pathway, including KRAS [OMIM *190070], HRAS [OMIM *190020], NRAS [OMIM *164790], and FGFR1 [OMIM *136350]. These entities are the oculoectodermal (OES, OMIM %600268) and Schimmelpenning‐Feuerstein‐Mims syndromes (SFMS, OMIM #163200), as well as encephalocraniocutaneous lipomatosis (ECCL, OMIM #613001), oculocutaneous disorders exhibiting pleiotropic anomalies that include scalp lesions, epilepsy, epibulbar dermoids, cloudy cornea, eyelid coloboma, coarctation of the aorta, and skin pigmentation abnormalities (Boppudi et al, ; Groesser et al, ; Kuroda et al, ; Peacock et al, ). Somatic mutations causing oculocutaneous mosaic RASopathies are recurrent and have been identified at KRAS codons 13, 19, and 146 in OES patients (4 subjects reported to date) (Boppudi et al, ; Peacock et al, ), KRAS codon 146 and FGFR1 codons 546 and 656 in ECCL (six reported patients) (Bennett et al, ; Boppudi et al, ), and HRAS codon 13 (2 patients), KRAS codon 12 (3 subjects), and NRAS codon 61 (1 subject) in individuals with a SFMS diagnosis (Groesser et al, ; Igawa et al, ; Kuroda et al, ; Lihua, Feng, Shanshan, Jialu, & Kewen, ; Sun et al, ; Wang, Qian, Zhang, & Zhou, ).…”

Section: Introductionmentioning

confidence: 99%

“…These entities are the oculoectodermal (OES, OMIM %600268) and Schimmelpenning‐Feuerstein‐Mims syndromes (SFMS, OMIM #163200), as well as encephalocraniocutaneous lipomatosis (ECCL, OMIM #613001), oculocutaneous disorders exhibiting pleiotropic anomalies that include scalp lesions, epilepsy, epibulbar dermoids, cloudy cornea, eyelid coloboma, coarctation of the aorta, and skin pigmentation abnormalities (Boppudi et al, ; Groesser et al, ; Kuroda et al, ; Peacock et al, ). Somatic mutations causing oculocutaneous mosaic RASopathies are recurrent and have been identified at KRAS codons 13, 19, and 146 in OES patients (4 subjects reported to date) (Boppudi et al, ; Peacock et al, ), KRAS codon 146 and FGFR1 codons 546 and 656 in ECCL (six reported patients) (Bennett et al, ; Boppudi et al, ), and HRAS codon 13 (2 patients), KRAS codon 12 (3 subjects), and NRAS codon 61 (1 subject) in individuals with a SFMS diagnosis (Groesser et al, ; Igawa et al, ; Kuroda et al, ; Lihua, Feng, Shanshan, Jialu, & Kewen, ; Sun et al, ; Wang, Qian, Zhang, & Zhou, ). Such pathogenic mutations also confer an elevated risk for developing a variety of tumors commonly associated with these oculocutaneos disorders (Aslan et al, ; Eisen & Michael; ; Kocak, Yarar, & Carman, ; Moog, ; Peacock et al, ; Toriello et al, ; Valera et al, ).…”

Section: Introductionmentioning

confidence: 99%

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Expansion of the phenotypic spectrum and description of molecular findings in a cohort of patients with oculocutaneous mosaic RASopathies

Chacón‐Camacho

López-Moreno

Morales‐Sanchez³

et al. 2019

Molec Gen & Gen Med

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Background Postzygotic KRAS , HRAS , NRAS , and FGFR1 mutations result in a group of mosaic RASopathies characterized by related developmental anomalies in eye, skin, heart, and brain. These oculocutaneous disorders include oculoectodermal syndrome (OES) encephalo‐cranio‐cutaneous lipomatosis (ECCL), and Schimmelpenning‐Feuerstein‐Mims syndrome (SFMS). Here, we report the results of the clinical and molecular characterization of a novel cohort of patients with oculocutaneous mosaic RASopathies. Methods Two OES, two ECCL, and two SFMS patients were ascertained in the study. In addition, two subjects with unilateral isolated epibulbar dermoids were also enrolled. Molecular analysis included PCR amplification and Sanger sequencing of KRAS , HRAS , NRAS , and FGFR1 genes in DNA obtained from biopsies (skin/epibulbar dermoids), buccal mucosa, and blood leukocytes. Massive parallel sequencing was employed in two cases with low‐level mosaicism. Results In DNA from biopsies, mosaicism for pathogenic variants, including KRAS p.Ala146Thr in two OES subjects, FGFR1 p.Asn546Lys and KRAS p.Ala146Val in ECCL patients, and KRAS p.Gly12Asp in both SFMS patients, was demonstrated. No mutations were shown in DNA from conjunctival lesions in two subjects with isolated epibubar dermoids. Conclusion Our study allowed the expansion of the clinical spectrum of mosaic RASopathies and supports that mosaicism for recurrent mutations in KRAS and FGFR1 is a commonly involved mechanism in these rare oculocutaneous anomalies.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

Expansion of the phenotypic spectrum and description of molecular findings in a cohort of patients with oculocutaneous mosaic RASopathies

Chacón‐Camacho

López-Moreno

Morales‐Sanchez³

et al. 2019

Molec Gen & Gen Med

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The categories of cutaneous mosaicism: A proposed classification

Happle

2015

American J of Med Genetics Pt A

112

119

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Mosaic disorders can most easily be studied in the skin. This article presents a comprehensive overview of the different forms of cutaneous mosaicism. Major categories are genomic versus epigenetic mosaicism and nonsegmental versus segmental mosaicism. The class of nonsegmental mosaics includes single point mosaicism as exemplified by solitary benign or malignant skin tumors; disseminated mosaicism as noted in autosomal dominant tumor syndromes such as neurofibromatosis 1; and patchy mosaicism without midline separation as found in giant melanocytic nevus. The class of segmental mosaics includes segmental manifestation of lethal genes surviving by mosaicism as noted in Proteus syndrome; type 1 segmental mosaicism of autosomal dominant skin disorders reflecting heterozygosity for a postzygotic new mutation; type 2 segmental mosaicism of autosomal dominant skin disorders reflecting loss of heterozygosity that occurred at an early developmental stage in a heterozygous embryo; and isolated or superimposed segmental mosaicism of common polygenic skin disorders such as psoriasis or atopic dermatitis. A particular form of genomic mosaicism is didymosis (twin spotting). Revertant mosaicism is recognizable as one or more areas of healthy skin in patients with epidermolysis bullosa or other serious genodermatoses. The category of epigenetic mosaicism includes several X-linked, male lethal disorders such as incontinentia pigmenti, and the patterns of lyonization as noted in X-linked non-lethal disorders such as hypohidrotic ectodermal dysplasia of the Christ-Siemens-Touraine type. An interesting field of future research will be the concept of epigenetic autosomal mosaicism that may explain some unusual cases of autosomal transmission of linear hypo- or hypermelanosis.

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