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Literature DB >> 33846505

Septal chondrocyte hypertrophy contributes to midface deformity in a mouse model of Apert syndrome.

Woo-Jin Kim¹, Hyun-Mo Ryoo², Bong-Soo Kim³, Hye-Rim Shin³, Hyun-Jung Kim³, Heein Yoon³, Young-Dan Cho⁴, Kang-Young Choi⁵, Je-Yong Choi⁶.

Abstract

Midface hypoplasia is a major manifestation of Apert syndrome. However, the tissue component responsible for midface hypoplasia has not been elucidated. We studied mice with a chondrocyte-specific Fgfr2S252W mutation (Col2a1-cre; Fgfr2S252W/+) to investigate the effect of cartilaginous components in midface hypoplasia of Apert syndrome. In Col2a1-cre; Fgfr2S252W/+ mice, skull shape was normal at birth, but hypoplastic phenotypes became evident with age. General dimensional changes of mutant mice were comparable with those of mice with mutations in EIIa-cre; Fgfr2S252W/+, a classic model of Apert syndrome in mice. Col2a1-cre; Fgfr2S252W/+ mice showed some unique facial phenotypes, such as elevated nasion, abnormal fusion of the suture between the premaxilla and the vomer, and decreased perpendicular plate of the ethmoid bone volume, which are related to the development of the nasal septal cartilage. Morphological and histological examination revealed that the presence of increased septal chondrocyte hypertrophy and abnormal thickening of nasal septum is causally related to midface deformities in nasal septum-associated structures. Our results suggest that careful examination and surgical correction of the nasal septal cartilage may improve the prognosis in the surgical treatment of midface hypoplasia and respiratory problems in patients with Apert syndrome.

Entities: CellLine Chemical Disease Gene Mutation Species

Year: 2021 PMID： 33846505 DOI： 10.1038/s41598-021-87260-5

Source DB: PubMed Journal: Sci Rep ISSN： 2045-2322 Impact factor: 4.379

37 in total

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3. Excessive osteoclast activation by osteoblast paracrine factor RANKL is a major cause of the abnormal long bone phenotype in Apert syndrome model mice.

Authors: Hye-Rim Shin; Bong-Soo Kim; Hyun-Jung Kim; Heein Yoon; Woo-Jin Kim; Je-Yong Choi; Hyun-Mo Ryoo
Journal: J Cell Physiol Date: 2022-01-20 Impact factor: 6.513

3 in total

Septal chondrocyte hypertrophy contributes to midface deformity in a mouse model of Apert syndrome.

1. Guideline for Care of Patients With the Diagnoses of Craniosynostosis: Working Group on Craniosynostosis.

2. The nasal septum and the development of the midface. A longitudinal study of a pair of monozygotic twins.

3. Airway Analysis in Apert Syndrome.

Review 4. Cleft lip, nose, and palate: the nasal septum as the pacemaker for midfacial growth.

5. The growth of the nasal septum in the 6-9 week period of foetal development--Warfarin embryopathy offers a new insight into prenatal facial development.

6. Upper airway changes in syndromic craniosynostosis patients following midface or monobloc advancement: correlation between volume changes and respiratory outcome.

7. Loss of fibroblast growth factor receptor 2 ligand-binding specificity in Apert syndrome.

Review 8. Syndromic craniosynostosis: from history to hydrogen bonds.

9. Management of the Airway in Apert Syndrome.

10. The role of distraction osteogenesis in the management of craniofacial syndromes.

1. A dysmorphic mouse model reveals developmental interactions of chondrocranium and dermatocranium.

Review 2. Properties of the Nasal Cartilage, from Development to Adulthood: A Scoping Review.

3. Excessive osteoclast activation by osteoblast paracrine factor RANKL is a major cause of the abnormal long bone phenotype in Apert syndrome model mice.