Parietal aplasia and hypophosphatasia in a child harboring a novel mutation in RUNX2 and a likely pathogenic variant in TNSALP

Anna Papadopoulou; Evangelia Bountouvi; Vassiliki Sideri; Paraskevi Moutsatsou; Nikitas Spyridon Skarakis; Artemis Doulgeraki; Fotini Eleni Karachaliou

doi:10.1016/j.bone.2021.115904

Parietal aplasia and hypophosphatasia in a child harboring a novel mutation in RUNX2 and a likely pathogenic variant in TNSALP

Bone. 2021 May:146:115904. doi: 10.1016/j.bone.2021.115904. Epub 2021 Feb 27.

Authors

Anna Papadopoulou¹, Evangelia Bountouvi², Vassiliki Sideri², Paraskevi Moutsatsou³, Nikitas Spyridon Skarakis⁴, Artemis Doulgeraki⁵, Fotini Eleni Karachaliou²

Affiliations

¹ Third Department of Pediatrics, National & Kapodistrian University of Athens, University General Hospital "Attikon", Medical School, Athens, Greece; Department of Clinical Biochemistry, National & Kapodistrian University of Athens, University General Hospital "Attikon", Medical School, Athens, Greece. Electronic address: anpapado@med.uoa.gr.
² Third Department of Pediatrics, National & Kapodistrian University of Athens, University General Hospital "Attikon", Medical School, Athens, Greece.
³ Department of Clinical Biochemistry, National & Kapodistrian University of Athens, University General Hospital "Attikon", Medical School, Athens, Greece.
⁴ Department of Clinical Biochemistry, National & Kapodistrian University of Athens, University General Hospital "Attikon", Medical School, Athens, Greece; Department of Endocrinology and Diabetes Center, "G. Gennimatas", General Hospital of Athens, Athens, Greece.
⁵ Department of Bone and Mineral Metabolism, Institute of Child Health, Athens, Greece.

PMID: 33647526
DOI: 10.1016/j.bone.2021.115904

Abstract

Cleidocranial dysplasia is a dominantly inherited skeletal dysplasia resulting from inherited or spontaneous mutations of Runt-related transcription factor 2 gene (RUNX2). It represents a clinical continuum typically characterized by wide calvarial sutures, clavicular hypoplasia and dental abnormalities. CDD has been rarely associated with skeletal and biochemical features that mimic hypophosphatasia. We report clinical, biochemical and molecular profile of a 3-year-old female with CCD, presented in utero with large cranial defects. She displayed severe parietal dysplasia, wide cranial sutures, clavicular abnormalities and biochemical features of hypophospatasia (HHP). She was preliminary diagnosed with benign perinatal HHP, harboring a likely pathogenic heterozygous TNSALP variant (p.Ser181Leu) inherited by the mother, who also displayed low levels of ALP. Asfotase alfa was introduced for a six-month-period with rather positive impact on cranial ossification. Nevertheless, focal skeletal disease (cranium and clavicles) and absence of clinical symptoms in the mother, carrier of the same genetic variant, posed diagnosis into question and further genetic analysis detected the novel spontaneous frameshift mutation c.1191delC (p.Phe398Leufs*86) in RUNX2 gene, establishing the CCD diagnosis. Although genotype-phenotype correlations are difficult, p.Phe398Leufs*86 appears to be associated with a severe cranial phenotype and absence of parietal bones, similarly to other adjacent frameshift/splicing mutations. The TNSALP variant (p.Ser181Leu) may contributed to patient's final phenotype, as well as to maternal low ALP levels. However, since low ALP levels have been also reported in few CCD patients with no alterations in TNSALP gene, studies to elucidate RUNX2 and TNSALP interactions could shed more light on differential diagnosis between CCD and HHP, CCD appropriate therapy and genetic counselling. ACCESSION NUMBER: (SUB8185506).

Keywords: Asfotase alfa; C-terminous domain; Cleidocranial dysplasia; Hypophosphatasia; Novel mutation; RUNX2.

Publication types

Case Reports

MeSH terms

Child, Preschool
Cleidocranial Dysplasia* / genetics
Core Binding Factor Alpha 1 Subunit / genetics
Female
Humans
Hypophosphatasia* / genetics
Mutation / genetics
Phenotype

Substances

Core Binding Factor Alpha 1 Subunit
RUNX2 protein, human