Genetic Analysis and Functional Study of a Pedigree With Bruck Syndrome Caused by PLOD2 Variant

Wang, Ruo-Li; Ruan, Dan-Dan; Hu, Yanan; Gan, Yu-Mian; Lin, Xin-Fu; Fang, Zhu-Ting; Liao, Lisheng; Tang, Fa-Qiang; He, Wubing; Luo, Jie‐Wei

doi:10.3389/fped.2022.878172

Cited by 1 publication

(2 citation statements)

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“…A larger number of Bruck syndrome are being reported after the adoption of clinical exome sequencing in OI [21,22]. In our study most of our patients were diagnosed with clinical exome sequencing which is preferred as most of the variants are novel in our population.…”

Section: Discussionmentioning

confidence: 96%

“…A total of 87 unique public variants have been described in FKBP10 and 52 in PLOD2 (LOVD database). A large number of reports are from Chinese population [21,22,25,30]. There are three reports from the south Asian population with no overlap and no recurrent mutation [18,20,26] .A recent Egyptian series reports 13 patients from nine families with ve novel mutations [9].…”

Section: Discussionmentioning

confidence: 99%

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Clinical and genetic landscape of Bruck syndrome in the Indian population

Selina,

Kandagaddala,

Danda

et al. 2024

Preprint

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Background Bruck syndrome (BS) is a rare form of Osteogenesis imperfecta (OI) with congenital large joint contractures and bone fragility fractures. Evaluation of phenotypic and genotypic profiles of 14 children with FKBP10 and PLOD2 gene variants causing Bruck syndrome (BS) and highlighting the severe deformities in response to poor surgical treatment in the Indian cohort. Methods Patients with bone fragility were clinically evaluated. After informed consent, genotyping was done by next-generation sequencing, and the variants were validated by Sanger sequencing. These children were treated surgically and pamidronate was administered. Results Out of 14 children, 12 were with FKBP10 gene variants, and two with PLOD2 gene variants. The age at diagnosis varied from birth to four years. All were classified as type III by modified Sillence classification. twelve had joint contractures, mainly in the knees and elbows. Clubfeet was identified in seven, scoliosis in three, and severe kyphoscoliosis in three. Two had skull deformities, six with wormian bones, one with basilar invagination and another showing severe cervical compression myelopathy. Rib fractures in six, vertebral compression in nine, and protrusion acetabulae in three were noted. Surgical correction of the deformities by soft tissue release and bone shortening was partially successful, while growth modulation was unsuccessful as the implant failed. Nine of the patients were non-ambulant. Bone density was decreased in all, and the response to pamidronate was partial. This cohort had four novel FKBP10 variants and two PLOD2 variants. Conclusion The study highlights the proportionate representation of the two genes in our population, the severe deformities with poor response to surgical treatment, and novel variants in the population.

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Section: Discussionmentioning

confidence: 96%