Identification of a novel splicing mutation and genotype–phenotype correlations in rare PLS3-related childhood-onset osteoporosis

Wu, Zhichong; Feng, Zhenhua; Zhu, Xiufen; Dai, Zhicheng; Min, Kaixing; Qiu, Yong; Yi, Long; Xu, Leilei; Zhu, Zezhang

doi:10.1186/s13023-022-02380-z

Cited by 3 publications

(1 citation statement)

References 17 publications

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“…Most of these are frameshift and nonsense mutations, both likely to be followed by nonsense-mediated mRNA decay [ 1 , 6 , 7 , 11 ]. Large intragenic deletions or duplications, leading to destroyed gene structure, and splice-site mutations, resulting in altered protein length, are also common [ 1 , 12 – 16 ].…”

Section: Introductionmentioning

confidence: 99%

PLS3 Mutations in X-Linked Osteoporosis: Clinical and Genetic Features in Five New Families

Costa,

Martins,

Machado

et al. 2023

Calcif Tissue Int

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Childhood-onset osteoporosis is a rare but clinically significant condition. Studies have shown pathogenic variants in more than 20 different genes as causative for childhood-onset primary osteoporosis. The X-chromosomal PLS3, encoding Plastin-3, is one of the more recently identified genes. In this study, we describe five new families from four different European countries with PLS3-related skeletal fragility. The index cases were all hemizygous males presenting with long bone and vertebral body compression fractures. All patients had low lumbar spine bone mineral density (BMD). The age at the first clinical fracture ranged from 1.5 to 13 years old. Three of the identified PLS3 variants were stop-gain variants and two were deletions involving either a part or all exons of the gene. In four families the variant was inherited from the mother. All heterozygous women reported here had normal BMD and no bone fractures. Four patients received bisphosphonate treatment with good results, showing a lumbar spine BMD increment and vertebral body reshaping after 10 months to 2 years of treatment. Our findings expand the genetic spectrum of PLS3-related osteoporosis. Our report also shows that early treatment with bisphosphonates may influence the disease course and reduce the progression of osteoporosis, highlighting the importance of early diagnosis for prompt intervention and appropriate genetic counseling.

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Section: Introductionmentioning

confidence: 99%

PLS3 Mutations in X-Linked Osteoporosis: Clinical and Genetic Features in Five New Families

Costa,

Martins,

Machado

et al. 2023

Calcif Tissue Int

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Early-Onset Osteoporosis: Molecular Analysis in Large Cohort and Focus on the PLS3 Gene

Mancini,

Chapurlat,

Isidor

et al. 2024

Calcif Tissue Int

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The intricate mechanism of PLS3 in bone homeostasis and disease

et al. 2023

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Since our discovery in 2013 that genetic defects in PLS3 lead to bone fragility, the mechanistic details of this process have remained obscure. It has been established that PLS3 variants cause syndromic and nonsyndromic osteoporosis as well as osteoarthritis. PLS3 codes for an actin-bundling protein with a broad pattern of expression. As such, it is puzzling how PLS3 specifically leads to bone-related disease presentation. Our review aims to summarize the current state of knowledge regarding the function of PLS3 in the predominant cell types in the bone tissue, the osteocytes, osteoblasts and osteoclasts. This is related to the role of PLS3 in regulating mechanotransduction, calcium regulation, vesicle trafficking, cell differentiation and mineralization as part of the complex bone pathology presented by PLS3 defects. Considering the consequences of PLS3 defects on multiple aspects of bone tissue metabolism, our review motivates the study of its mechanism in bone diseases which can potentially help in the design of suitable therapy.

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Identification of a novel splicing mutation and genotype–phenotype correlations in rare PLS3-related childhood-onset osteoporosis

Cited by 3 publications

References 17 publications

PLS3 Mutations in X-Linked Osteoporosis: Clinical and Genetic Features in Five New Families

PLS3 Mutations in X-Linked Osteoporosis: Clinical and Genetic Features in Five New Families

Early-Onset Osteoporosis: Molecular Analysis in Large Cohort and Focus on the PLS3 Gene

The intricate mechanism of PLS3 in bone homeostasis and disease

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