Autosomal-Recessive Mutations in MESD Cause Osteogenesis Imperfecta

Moosa, Shahida; Yamamoto, Guilherme Lopes; Garbes, Lutz; Keupp, Katharina; Beleza-Meireles, Ana; Moreno, Carolina; Valadares, Eugênia Ribeiro; Sousa, Sérgio B.; Maia, Sofia; Saraiva, Jorge; Honjo, Rachel Sayuri; Kim, Chong; Menezes, Hamilton Cabral de; Lausch, Ekkehart; Lorini, Pablo Villavicencio; Lamounier, Arsonval; Carniero, Tulio Canella Bezerra; Giunta, Cecilia; Rohrbach, Marianne; Janner, Marco; Semler, Oliver; Beleggia, Filippo; Li, Yun; Yiğit, Gökhan; Reintjes, Nadine; Altmüller, Janine; Nürnberg, Peter; Cavalcanti, Denise Pontes; Zabel, Bernhard; Warman, Matthew L.; Bertola, Débora Romeo; Wollnik, Bernd; Netzer, Christian

doi:10.1016/j.ajhg.2019.08.008

Cited by 39 publications

(57 citation statements)

References 27 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…The PLOD2 and SEC24D genes have been removed as pathological variants involved in OI 3, although PLOD2 remains listed as a pathological variant in BS type 2. Two new genes, SPARC 34 and TENT5A 35 have been identified and included as causal genes in OI 3.…”

Section: Resultsmentioning

confidence: 99%

The evolution of the nosology of osteogenesis imperfecta

Roomaney

Beighton

2020

Clinical Genetics

View full text Add to dashboard Cite

Osteogenesis imperfecta (OI) is a relatively common genetic skeletal disorder with an estimated frequency of 1 in 20 000 worldwide. The manifestations are diverse and although individually rare, the several different forms contribute to the production of a significant number of affected individuals with considerable morbidity and mortality. During the last decade, there have been extensive molecular investigations into the etiology of OI and these advances have direct relevance to the medical management of the disorder, and the purpose of this review is to document the history and evolution of the nosology of OI. The current nosology, based on molecular concepts, which are crucial in the identification of genotype-phenotype correlations in persons with OI, is also outlined. The successive revisions of the nosology and classification of OI have highlighted the importance of the nomenclature of the condition in order for it to be recognized by clinicians, scientists and patient advocacy groups. In this way, improved counseling of patients and individualized, tailored therapeutic approaches based on the underlying pathophysiology of the individual's type of OI have been facilitated.

show abstract

Section: Resultsmentioning

confidence: 99%

The evolution of the nosology of osteogenesis imperfecta

Roomaney

Beighton

2020

Clinical Genetics

View full text Add to dashboard Cite

show abstract

“…Some play an important role in the bone anabolic function of the WNT canonical signaling pathway (e.g. LRP5, WNT1, and MESD) and, in addition to OI, can be associated with generalized osteoporosis (WNT1) or similar conditions (LRP5 in osteoporosis pseudoglioma syndrome) (1,5).…”

Section: Modes Of Inheritance and Genetic Featuresmentioning

confidence: 99%

Management of Endocrine Disease: Osteogenesis imperfecta: an update on clinical features and therapies

Marom

Rabenhorst

Morello

2020

European Journal of Endocrinology

127

105

View full text Add to dashboard Cite

Osteogenesis imperfecta (OI) is an inherited skeletal dysplasia characterized by bone fragility and skeletal deformities. While the majority of cases are associated with pathogenic variants in COL1A1 and COL1A2, the genes encoding type I collagen, up to 25% of cases are associated with other genes that function within the collagen biosynthesis pathway or are involved in osteoblast differentiation and bone mineralization. Clinically, OI is heterogeneous in features and variable in severity. In addition to the skeletal findings, it can affect multiple systems including dental and craniofacial abnormalities, muscle weakness, hearing loss, respiratory and cardiovascular complications. A multi-disciplinary approach to care is recommended to address not only the fractures, reduced mobility, growth and bone pain but also other extra-skeletal manifestations. While bisphosphonates remain the mainstay of treatment in OI, new strategies are being explored, such as sclerostin inhibitory antibodies and TGF beta inhibition, to address not only the low bone mineral density but also the inherent bone fragility. Studies in animal models have expanded the understanding of pathomechanisms of OI and, along with ongoing clinical trials, will allow to develop better therapeutic approaches for these patients.

show abstract

“…Thus far, 24+ genes have been identified to cause OI ( Table 1 ). These include IFITM5 [ 5 , 6 ] [MIM: 614757], SERPINF1 [ 7 ] [MIM: 172860], CRTAP [ 8 ] [MIM: 605497], LEPRE1 [ 9 ] [MIM: 610339], P3H1 [ 10 ] [MIM: 610339], PPIB [ 11 ] [MIM: 123841], SERPINH1 [ 12 ] [MIM: 600943], FKBP10 [ 13 ] [MIM: 607063], SP7 [ 14 ] [MIM: 606633], BMP1 [ 15 ] [MIM: 112264], TMEM38B [ 16 ] [MIM: 611236], WNT1 [ 17 , 18 ] [MIM: 164820], CREB3L1 [ 19 ] [MIM: 616215], SPARC [ 20 ] [MIM: 182120], FAM46A [ 21 ] [MIM: 611357], MBTPS2 [ 22 ] [MIM: 300294], MESD [ 23 ] [MIM: 607783], SEC24D [ 24 ] [MIM: 607186], CCDC134 [ 25 ] [MIM: 618788], P4HB [ 26 ] [MIM: 176790], PLOD2 [ 27 ] [MIM: 601865], PLS3 [ 28 ] [MIM: 300131] and KDELR2 [MIM: 609024] [ 29 ]. These genes play a critical role in the processing and post-translational modification of type I collagen, the control of osteoblast differentiation or function or the formation of F-actin bundles.…”

Section: Genetic Causes Of Bone Fragilitymentioning

confidence: 99%

Mechanisms of Bone Fragility: From Osteogenesis Imperfecta to Secondary Osteoporosis

El‐Gazzar

Högler

2021

IJMS

View full text Add to dashboard Cite

Bone material strength is determined by several factors, such as bone mass, matrix composition, mineralization, architecture and shape. From a clinical perspective, bone fragility is classified as primary (i.e., genetic and rare) or secondary (i.e., acquired and common) osteoporosis. Understanding the mechanism of rare genetic bone fragility disorders not only advances medical knowledge on rare diseases, it may open doors for drug development for more common disorders (i.e., postmenopausal osteoporosis). In this review, we highlight the main disease mechanisms underlying the development of human bone fragility associated with low bone mass known to date. The pathways we focus on are type I collagen processing, WNT-signaling, TGF-ß signaling, the RANKL-RANK system and the osteocyte mechanosensing pathway. We demonstrate how the discovery of most of these pathways has led to targeted, pathway-specific treatments.

show abstract

Autosomal-Recessive Mutations in MESD Cause Osteogenesis Imperfecta

Cited by 39 publications

References 27 publications

The evolution of the nosology of osteogenesis imperfecta

The evolution of the nosology of osteogenesis imperfecta

Management of Endocrine Disease: Osteogenesis imperfecta: an update on clinical features and therapies

Mechanisms of Bone Fragility: From Osteogenesis Imperfecta to Secondary Osteoporosis

Contact Info

Product

Resources

About