Novel<i>COL2A1</i>Variant (c.619G&gt;A, p.Gly207Arg) Manifesting as a Phenotype Similar to Progressive Pseudorheumatoid Dysplasia and Spondyloepiphyseal Dysplasia, Stanescu Type

Jurgens, Julie A; Sobreira, Nara; Modaff, Peggy; Reiser, Catherine A.; Seo, Soo Hyun; Seong, Moon Woo; Park, Sung Sup; Kim, Ok Hwa; Cho, Tae-Joon; Pauli, Richard M.

doi:10.1002/humu.22839

Cited by 18 publications

(23 citation statements)

References 17 publications

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“…It was first reported by Stanescu et al in 1984, and is characterized by painful and progressive narrowing of joint space, platyspondyly, pronounced femoral coxa valga, and normal stature. Jurgens et al reported two probands with SED‐S and suggested that the p.Gly207Arg variant causes a distinct type II collagenopathy with features of progressive pseudorheumatoid dysplasia and SED‐S …”

Section: Resultsmentioning

confidence: 99%

Integrated analysis of COL2A1 variant data and classification of type II collagenopathies

Zhang

et al. 2019

Clinical Genetics

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The COL2A1 gene encodes the alpha‐1 chain of type II procollagen. Type II collagen, comprised of three identical alpha‐1 chains, is the major component of cartilage. COL2A1 gene variants are the etiologies of genetic diseases, termed type II collagenopathies, with a wide spectrum of clinical presentations. To date, at least 460 distinct COL2A1 mutations, identified in 663 independent probands, and 21 definite disorders have been reported. Nevertheless, a well‐defined genotype‐phenotype correlation has not been established, and few hot spots of mutation have been reported. In this study, we analyzed data of COL2A1 variants and clinical information of patients obtained from the Leiden Open Variation Database 3.0, as well as the currently available relevant literature. We determined the characteristics of the COL2A1 variants and distributions of the clinical manifestations in patients, and identified four likely genotype‐phenotype correlations. Moreover, we classified 21 COL2A1‐related disorders into five categories, which may assist clinicians in understanding the essence of these complex phenotypes and prompt genetic screening in clinical practice.

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Section: Resultsmentioning

confidence: 99%

Integrated analysis of COL2A1 variant data and classification of type II collagenopathies

Zhang

et al. 2019

Clinical Genetics

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“…The ensuing papers in this special issue of Human Mutation define many of the individual matchmaker services already connected [Buske, et al., a; Chatzimichali et al., ; Sobreira et al., ), or intending to connect to the federated network [Lancaster et al., 2015; Kirkpatrick et al., ; Lambertson et al., ; Mungall et al., ], as well as other core components [Buske et al., b] and concepts [Akle et al., ; Krawitz et al, ] that support genomic matchmaking. A few case examples of discoveries already made through use of matchmaking approaches are highlighted to add further support for this robust approach to rare disease gene discovery [Au et al., ; Jurgens et al., ; Loucks et al., ]. It is our hope that the success of the MME will serve as a model and foundation for innovative data sharing that leverages the increasing role of computational infrastructure to support the scaling of genomics as we collectively advance medicine and improve human health.…”

Section: Discussionmentioning

confidence: 99%

The Matchmaker Exchange: A Platform for Rare Disease Gene Discovery

et al. 2015

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There are few better examples of the need for data sharing than in the rare disease community, where patients, physicians, and researchers must search for “the needle in a haystack” to uncover rare, novel causes of disease within the genome. Impeding the pace of discovery has been the existence of many small siloed datasets within individual research or clinical laboratory databases and/or disease-specific organizations, hoping for serendipitous occasions when two distant investigators happen to learn they have a rare phenotype in common and can “match” these cases to build evidence for causality. However, serendipity has never proven to be a reliable or scalable approach in science. As such, the Matchmaker Exchange (MME) was launched to provide a robust and systematic approach to rare disease gene discovery through the creation of a federated network connecting databases of genotypes and rare phenotypes using a common application programming interface (API). The core building blocks of the MME have been defined and assembled. Three MME services have now been connected through the API and are available for community use. Additional databases that support internal matching are anticipated to join the MME network as it continues to grow.

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“…Embryonic lethality during organogenesis before E15, embryonic growth arrest at E11.5-E12 (Schnieke et al, 1983;Harbers et al, 1984) II (G) Spondyloepiphyseal dysplasias (Lee et al, 1989;Tiller et al, 1990;Chan et al, 1993;Jurgens et al, 2015;Barat-Houari et al, 2016) (G) Spondyloepimetaphyseal dysplasias (Tiller et al, 1995;Sulko et al, 2005) (G) Achondrogenesis 2 (Vissing et al, 1989;Mortier et al, 1995Mortier et al, , 2000Körkkö et al, 2000;Chan et al, 1995;Barat-Houari et al, 2016) (G) Legg-Calvé-Perthes disease (Miyamoto et al, 2007) (G) Kniest dysplasia (Wilkin et al, 1994;Winterpacht et al, 1996) (G) Avascular necrosis of femoral head (Liu et al, 2005;Kannu et al, 2011) Platyspondylic lethal skeletal dysplasia, Torrance type (Nishimura et al, 2004;Zankl et al, 2005) Spondyloperipheral dysplasia (Zankl et al, 2005;Nishimura et al, 2004) (G) Stickler syndrome 1 (Richards et al, 2000(Richards et al, , 2010McAlinden et al, 2008;Körkkö et al, 1993;Barat-Houari et al, 2016) (N) Osteoarthritis with mild chondrodysplasia (Ala-Kokko et al, 1990) (N) Czech dysplasia (Williams et al, 1993;Tzschach et al, 2008;Matsui et al, 2009;Barat-Houari et al, 2016) Perinatal lethality, abnormal skeleton, abnormal cranium, abnormal respiratory system (Li et al, 1995a). IIA isoform-specific knockout: prenatal lethality, holoprosencephal loss of head tissue...…”

Section: Introductionmentioning

confidence: 99%

The triple helix of collagens – an ancient protein structure that enabled animal multicellularity and tissue evolution

Fidler

Boudko

Rokas

et al. 2018

Journal of Cell Science

133

113

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The cellular microenvironment, characterized by an extracellular matrix (ECM), played an essential role in the transition from unicellularity to multicellularity in animals (metazoans), and in the subsequent evolution of diverse animal tissues and organs. A major ECM component are members of the collagen superfamily -comprising 28 types in vertebrates - that exist in diverse supramolecular assemblies ranging from networks to fibrils. Each assembly is characterized by a hallmark feature, a protein structure called a triple helix. A current gap in knowledge is understanding the mechanisms of how the triple helix encodes and utilizes information in building scaffolds on the outside of cells. Type IV collagen, recently revealed as the evolutionarily most ancient member of the collagen superfamily, serves as an archetype for a fresh view of fundamental structural features of a triple helix that underlie the diversity of biological activities of collagens. In this Opinion, we argue that the triple helix is a protein structure of fundamental importance in building the extracellular matrix, which enabled animal multicellularity and tissue evolution.

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NovelCOL2A1Variant (c.619G>A, p.Gly207Arg) Manifesting as a Phenotype Similar to Progressive Pseudorheumatoid Dysplasia and Spondyloepiphyseal Dysplasia, Stanescu Type

Cited by 18 publications

References 17 publications

Integrated analysis of COL2A1 variant data and classification of type II collagenopathies

Integrated analysis of COL2A1 variant data and classification of type II collagenopathies

The Matchmaker Exchange: A Platform for Rare Disease Gene Discovery

The triple helix of collagens – an ancient protein structure that enabled animal multicellularity and tissue evolution

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