BMPER variants associated with a novel, attenuated subtype of diaphanospondylodysostosis

Zong, Zheyuan; Tees, Susan; Miyanji, Firoz; Fauth, Clarissa T.; Reilly, Christopher W.; Lopez, Elena; Tredwell, Stephen J.; Goldberg, Y P; Delaney, Allen; Eydoux, Patrice; Allen, Margot Van; Lehman, Anna

doi:10.1038/jhg.2015.116

Cited by 15 publications

(24 citation statements)

References 27 publications

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“…Previous reports ascertained biallelic BMPER mutations in six patients with DSD [ 9 , 13 ] and three siblings with attenuated DSD [ 12 ]. In this report we show that ISD a disorder phenotypically similar, but much milder, than DSD is also caused by biallelic mutations in the BMPER gene.…”

Section: Discussionmentioning

confidence: 99%

“…Parental consanguinity in one patient suggested autosomal recessive inheritance, but the causative gene has been hitherto unknown [ 2 ]. Diaphanospondylodysostosis (DSD) is a lethal/semilethal skeletal dysplasia, the phenotype of which is similar to, but more severe than, that of ISD [ 5 – 12 ] (Additional file 1 : Tables S1 and Additional file 2 : Table S2). Funari et al identified mutations in the BMPER in four patients with DSD [ 13 ], and since then two additional DSD patients and three siblings with so-called attenuated form of DSD with BMPER mutations have been published [ 9 , 12 ] (Table 1 , Fig.…”

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confidence: 99%

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Extending the phenotype of BMPER-related skeletal dysplasias to ischiospinal dysostosis

Kuchinskaya

Grigelioniené

Hammarsjö

et al. 2016

Orphanet J Rare Dis

113

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Ischiospinal dysostosis (ISD) is a polytopic dysostosis characterized by ischial hypoplasia, multiple segmental anomalies of the cervicothoracic spine, hypoplasia of the lumbrosacral spine and occasionally associated with nephroblastomatosis. ISD is similar to, but milder than the lethal/semilethal condition termed diaphanospondylodysostosis (DSD), which is associated with homozygous or compound heterozygous mutations of bone morphogenetic protein-binding endothelial regulator protein (BMPER) gene. Here we report for the first time biallelic BMPER mutations in two patients with ISD, neither of whom had renal abnormalities. Our data supports and further extends the phenotypic variability of BMPER-related skeletal disorders.Electronic supplementary materialThe online version of this article (doi:10.1186/s13023-015-0380-0) contains supplementary material, which is available to authorized users.

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Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

Extending the phenotype of BMPER-related skeletal dysplasias to ischiospinal dysostosis

Kuchinskaya

Grigelioniené

Hammarsjö

et al. 2016

Orphanet J Rare Dis

113

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“…Cross talk with various BMP modulators, ECM components, and cell-surface proteins may thus provide a basis for the activities of Cv2/Bmper as agonist or antagonist of BMP ligands. Mutations in BMPER have been linked to an autosomal recessive perinatal lethal skeletal disorder, diaphanospondylodysostosis, in humans (Funari et al 2010;Ben-Neriah et al 2011;Zong et al 2015).…”

Section: Crossveinless-2 (Bmper/cv-2)mentioning

confidence: 99%

Agonists and Antagonists of TGF-β Family Ligands

Chang

2016

Cold Spring Harb Perspect Biol

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The discovery of the transforming growth factor β (TGF-β) family ligands and the realization that their bioactivities need to be tightly controlled temporally and spatially led to intensive research that has identified a multitude of extracellular modulators of TGF-β family ligands, uncovered their functions in developmental and pathophysiological processes, defined the mechanisms of their activities, and explored potential modulator-based therapeutic applications in treating human diseases. These studies revealed a diverse repertoire of extracellular and membrane-associated molecules that are capable of modulating TGF-β family signals via control of ligand availability, processing, ligand-receptor interaction, and receptor activation. These molecules include not only soluble ligand-binding proteins that were conventionally considered as agonists and antagonists of TGF-β family of growth factors, but also extracellular matrix (ECM) proteins and proteoglycans that can serve as "sink" and control storage and release of both the TGF-β family ligands and their regulators. This extensive network of soluble and ECM modulators helps to ensure dynamic and cell-specific control of TGF-β family signals. This article reviews our knowledge of extracellular modulation of TGF-β growth factors by diverse proteins and their molecular mechanisms to regulate TGF-β family signaling.

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“…Biallelic pathogenic variants in BMPER are also known to cause diaphanospondylodysostosis (DSD) (OMIM #608022), a perinatally lethal condition (Funari et al ). Attenuated DSD with features overlapping with ISD and DSD has been reported in a family with biallelic variants in BMPER (Zong et al ). All the three conditions have overlapping features and demonstrate the spectrum of severity of the BMPER related conditions.…”

mentioning

confidence: 95%

Further evidence for causation of ischiospinal dysostosis by a pathogenic variant in BMPER and expansion of the phenotype

Salian

Nampoothiri

Shukla

et al. 2018

Congenital Anomalies

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BMPER variants associated with a novel, attenuated subtype of diaphanospondylodysostosis

Cited by 15 publications

References 27 publications

Extending the phenotype of BMPER-related skeletal dysplasias to ischiospinal dysostosis

Extending the phenotype of BMPER-related skeletal dysplasias to ischiospinal dysostosis

Agonists and Antagonists of TGF-β Family Ligands

Further evidence for causation of ischiospinal dysostosis by a pathogenic variant in BMPER and expansion of the phenotype

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