Cleidocranial dysplasia and novel RUNX2 variants: dental, craniofacial, and osseous manifestations

Sermporn Thaweesapphithak; Jirawat Saengsin; Wuttichart Kamolvisit; Thanakorn Theerapanon; Thantrira Porntaveetus; Vorasuk Shotelersuk

doi:10.1590/1678-7757-2022-0028

Cleidocranial dysplasia and novel RUNX2 variants: dental, craniofacial, and osseous manifestations

J Appl Oral Sci. 2022 Jun 6:30:e20220028. doi: 10.1590/1678-7757-2022-0028. eCollection 2022.

Authors

Sermporn Thaweesapphithak¹, Jirawat Saengsin², Wuttichart Kamolvisit^{3

4}, Thanakorn Theerapanon¹, Thantrira Porntaveetus¹, Vorasuk Shotelersuk^{3

4}

Affiliations

¹ Chulalongkorn University , Faculty of Dentistry , Department of Physiology , Center of Excellence in Genomics and Precision Dentistry, Bangkok , Thailand .
² Chiang Mai University , Faculty of Medicine , Department of Orthopedic Surgery , Chiang Mai , Thailand .
³ Chulalongkorn University , Faculty of Medicine , Department of Pediatrics, Medical Genomics Cluster , Center of Excellence for Medical Genomics, Bangkok , Thailand .
⁴ The Thai Red Cross Society, King Chulalongkorn Memorial Hospital , Excellence Center for Genomics and Precision Medicine , Bangkok , Thailand .

Abstract

Objectives: Cleidocranial dysplasia (CCD) is a skeletal disorder affecting cranial sutures, teeth, and clavicles, and is associated with the RUNX2 mutations. Although numerous patients have been described, a direct genotype-phenotype correlation for RUNX2 has been difficult to establish. Further cases must be studied to understand the clinical and genetic spectra of CCD. To characterize detailed phenotypes and identify variants causing CCD in five unrelated patients and their family members.

Methodology: Clinical and radiographic examinations were performed. Genetic variants were identified by exome and Sanger sequencing, data were analyzed by bioinformatics tools.

Results: Three cases were sporadic and two were familial. Exome sequencing successfully detected the heterozygous pathogenic RUNX2 variants in all affected individuals. Three were novel, comprising a frameshift c.739delA (p.(Ser247Valfs*)) in exon 6 (Patient-1), a nonsense c.901C>T (p.(Gln301*)) in exon 7 (Patient-2 and affected mother), and a nonsense c.1081C>T (p.(Gln361*)) in exon 8 (Patient-3). Two previously reported variants were missense: the c.673C>T (p.(Arg225Trp)) (Patient-4) and c.674G>A (p.(Arg225Gln)) (Patient-5) in exon 5 within the Runt homology domain. Patient-1, Patient-2, and Patient-4 with permanent dentition had thirty, nineteen, and twenty unerupted teeth, respectively; whereas Patient-3 and Patient-5, with deciduous dentition, had normally developed teeth. All patients exhibited typical CCD features, but the following uncommon/unreported phenotypes were observed: left fourth ray brachymetatarsia (Patient-1), normal clavicles (Patient-2 and affected mother), phalangeal malformations (Patient-3), and normal primary dentition (Patient-3, Patient-5).

Conclusions: The study shows that exome sequencing is effective to detect mutation across ethnics. The two p.Arg225 variants confirm that the Runt homology domain is vital for RUNX2 function. Here, we report a new CCD feature, unilateral brachymetatarsia, and three novel truncating variants, expanding the phenotypic and genotypic spectra of RUNX2 , as well as show that the CCD patients can have normal deciduous teeth, but must be monitored for permanent teeth anomalies.

MeSH terms

Cleidocranial Dysplasia* / complications
Cleidocranial Dysplasia* / diagnostic imaging
Cleidocranial Dysplasia* / genetics
Core Binding Factor Alpha 1 Subunit* / genetics
Humans
Mutation
Mutation, Missense
Phenotype

Substances

Core Binding Factor Alpha 1 Subunit
RUNX2 protein, human