Homozygous missense and nonsense mutations in BMPR1B cause acromesomelic chondrodysplasia-type Grebe

Graul‐Neumann, Luitgard; Deichsel, Alexandra; Wille, Ulrike; Kakar, Naseebullah; Koll, Randi; Bassir, C.; Ahmad, Jamil; Cormier‐Daire, Valérie; Mundlos, Stefan; Kubisch, Christian; Borck, Guntram; Klopocki, Eva; Mueller, Thomas D.; Doelken, Sandra C.; Seemann, Petra

doi:10.1038/ejhg.2013.222

Cited by 21 publications

(23 citation statements)

References 38 publications

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“…To date, twenty pathogenic mutations in the gene GDF5 including five in patients affected with AMDG have been reported (Table 2) Faiyaz-Ul-Haque et al, 2002; Al-Yahyaee Basit et al, 2008;Martinez-Garcia et al, 2015). Recently, Graul-Neumann et al (Graul-Neumann et al, 2014). have reported mutations (p.Cys53Arg; p.Try219*) in the gene BMPR1B causing AMDG in two consanguineous families of Lebanon and Pakistani origin (Table 2).…”

Section: Gdf5-bmpr1b Signalopathymentioning

confidence: 94%

“…It was localized to chromosome 20q11.22 (Thomas et al, 1996) and subsequently small mutations in the growth and differentiation factor-5 (GDF5) gene were detected in several families (Thomas et al, 1996). Recently, point mutations in bone morphogenetic protein receptor IB (BMPR1B) gene have been identified in families segregating AMDG (Graul-Neumann et al, 2014). Similarly, AMDH is characterized by severe dwarfism, lower limbs more affected than upper limbes and large joint dislocations.…”

Section: Introductionmentioning

confidence: 95%

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Genetics of human isolated acromesomelic dysplasia

Khan

Basit

Khan

et al. 2016

European Journal of Medical Genetics

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Section: Gdf5-bmpr1b Signalopathymentioning

confidence: 94%

Section: Introductionmentioning

confidence: 95%

Genetics of human isolated acromesomelic dysplasia

Khan

Basit

Khan

et al. 2016

European Journal of Medical Genetics

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“…A homozygous nonsense variant (p.Trp219*) in the same domain, in a family of Pakistani origin reported by Graul‐Neumann et al. (), caused more severe form of acromesomelic dysplasia, AMDG. It is highly likely that the nonsense variant in the kinase domain results in complete loss of function of protein through nonsense‐mediated mRNA decay and/or protein truncation.…”

Section: Discussionmentioning

confidence: 79%

A novel homozygous variant in BMPR1B underlies acromesomelic dysplasia Hunter–Thompson type

Ullah

Umair

Muhammad

et al. 2018

Annals of Human Genetics

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Acromesomelic dysplasia is genetically heterogeneous group of skeletal disorders characterized by short stature and acromelia and mesomelia of limbs. Acromesomelic dysplasia segregates in an autosomal recessive pattern and is caused by biallelic sequence variants in three genes (NPR2, GDF5, and BMPR1B). A consanguineous family of Pakistani origin segregating a subtype of acromesomelic dysplasia called Hunter–Thompson was clinically and genetically evaluated. Geno-typing of microsatellite markers and linkage analysis revealed a 7.78 Mb homozygous region on chromosome 4q22.3, which harbors BMPR1B. Sequence analysis of the gene revealed a novel homozygous missense variant (c.1190T > G, p.Met397Arg) that segregates with the disease phenotype within the family and produced a Logarithm of odds (LOD) score of 3.9 with the disease phenotype. This study reports on the first familial case of acromesomelic dysplasia Hunter–Thompson type. It is also the first report of BMPR1B underlying the etiology of acromesomelic dysplasia Hunter–Thompson type.

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“…In some but not all heterozygotes much milder forms of the traits were seen. BMPR1B is already associated with bone dysmorphologies [1][2][3], but PDHA2 has not been associated with any disease. The loci for syndromes manifesting with digit anomalies and infertility together, such as Dauwerse-Peters syndrome (MIM 611733; t(4;6)(q12;p23)), deafnessinfertility syndrome (MIM 611102; 15q15.30), and short stature, onychodysplasia, facial dysmorphism and hypotrichosis syndrome (SOFT; MIM 614813; 3p21) are all excluded by linkage analysis.…”

Section: Discussionmentioning

confidence: 99%

“…The skeletal phenotype of the patient was aplasia of the fibula, severe brachydactyly, ulnar deviation of the hands, fusion of carpal/tarsal bones and disproportionate short stature, and the variant was homozygous 8-bp deletion c.361_368delGGACCTAT (p.(Gly121Thrfs*13)). The manifestations of two other variants, namely, c.157T>C (p.(Cys53Arg)) and c.657G>A (p.(Trp219*)), are also like Grebe chondrodysplasia [2]. The last variant c.91C>T (p. (Arg31Cys)) was assessed to have a moderate impact on the protein and accordingly caused fibular hypoplasia and complex brachydactyly (du Pan dysplasia), a milder ACD [3].…”

Section: Introductionmentioning

confidence: 99%

Linked homozygous BMPR1B and PDHA2 variants in a consanguineous family with complex digit malformation and male infertility

et al. 2018

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In affected members of a consanguineous family, a syndrome, which is concurrence of set of medical signs, is often observed and commonly assumed to have arisen from pleiotropy, i.e., the phenomenon of a single gene variant affecting multiple traits. We detected six sibs afflicted with a unique combination of digit malformation that includes brachydactyly, symphalangism and zygodactyly plus infertility in males owing to azoospermia, sperm immotility or necrospermia, which we hypothesised to have arisen from a defect in a single gene. We mapped the disease locus and by exome sequencing identified in patients homozygous missense variants bone morphogenetic protein receptor type IB (BMPR1B) c.640C>T (p.(Arg214Cys)) and alpha-2 pyruvate dehydrogenase (PDHA2) c.679A>G (p.(Met227Val)). Structural protein modelling, protein sequence conservation and in silico analysis indicate that both variants affect protein function. BMPR1B is known to be responsible for autosomal dominant brachydactyly and autosomal recessive acromesomelic chondrodysplasia. Our findings show that also recessive complex digit malformation can be caused by BMPR1B variant and not all biallelic BMPR1B variants cause acromesomelic dysplasia. PDHA2 is a novel candidate gene for male infertility; the protein product is a mitochondrial enzyme with highest expression in ejaculated sperm. Our findings are a unique example of two linked variants, ~ 711 Kb apart, in different genes that together manifest as a novel syndrome. They demonstrate that exome sequencing and not candidate gene approach should be employed in disease gene hunt, defining new diseases and genetic testing, to rule out the coincidental presence of two variants contributing together to the phenotype, which may be discerned as a novel disease.

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Homozygous missense and nonsense mutations in BMPR1B cause acromesomelic chondrodysplasia-type Grebe

Cited by 21 publications

References 38 publications

Genetics of human isolated acromesomelic dysplasia

Genetics of human isolated acromesomelic dysplasia

A novel homozygous variant in BMPR1B underlies acromesomelic dysplasia Hunter–Thompson type

Linked homozygous BMPR1B and PDHA2 variants in a consanguineous family with complex digit malformation and male infertility

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