Clinical and molecular features of 66 patients with musculocontractural Ehlers−Danlos syndrome caused by pathogenic variants in<i>CHST14</i>(mcEDS-<i>CHST14</i>)

Minatogawa, Mari; Unzaki, Ai; Morisaki, Hiroko; Syx, Delfien; Sonoda, T; Janecke, Andreas; Slavotinek, Anne; Voermans, Nicol C.; Lacassie, Yves; Mendoza-Londoño, Roberto; Wierenga, Klaas J.; Jayakar, Parul; Gahl, William A.; Tifft, Cynthia J.; Figuera, Luis E.; Hilhorst‐Hofstee, Yvonne; Maugeri, Alessandra; Ishikawa, Ken; Kobayashi, Tomoko; Aoki, Yoko; Ohura, Toshihiro; Kawame, Hiroshi; Kono, Michihiro; Mochida, Kosuke; Tokorodani, Chiho; Kikkawa, Kiyoshi; Morisaki, Takayuki; Kobayashi, Tetsuyuki; Nakane, Takaya; Kubo, Akiharu; Ranells, Judith D.; Migita, Ohsuke; Sobey, Glenda; Kaur, Anupriya; Ishikawa, Masayo; Yamaguchi, Tomomi; Matsumoto, Naomichi; Malfait, Fransiska; Miyake, Noriko; Kosho, Tomoki

doi:10.1136/jmedgenet-2020-107623

Cited by 20 publications

(29 citation statements)

References 37 publications

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“…D4ST encoded by carbohydrate sulfotransferase 14 (CHST14) catalyzes the transfer of a sulfate group from 3 -phosphoadenosine 5 -phosphosulfate to the C-4 hydroxy group of GalNAc residues in DS chains (Figure 2) [26,27]. EDS musculocontractural type 1 is caused by a variety of pathogenic variants in CHST14 [22][23][24]81,[87][88][89][90][91][92][93][94][95][96] (Table 2). The characteristic manifestations of the EDS musculocontractural type 1 were craniofacial features including large fontanelle with delayed closure, downslanting palpebral fissures, and hypertelorism; skeletal features including characteristic finger morphologies, joint hypermobility, multiple congenital contractures, progressive talipes deformities, and recurrent joint dislocation; cutaneous features including hyperextensibility, fine/acrogeria-like/wrinkling palmar creases, and bruisability; refractive errors of vision, large subcutaneous hematomas, constipation, cryptorchidism, hypotonia, and motor developmental delay [96].…”

Section: Chst14mentioning

confidence: 99%

The Specific Role of Dermatan Sulfate as an Instructive Glycosaminoglycan in Tissue Development

Mizumoto

Yamada

2022

IJMS

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The crucial roles of dermatan sulfate (DS) have been demonstrated in tissue development of the cutis, blood vessels, and bone through construction of the extracellular matrix and cell signaling. Although DS classically exerts physiological functions via interaction with collagens, growth factors, and heparin cofactor-II, new functions have been revealed through analyses of human genetic disorders as well as of knockout mice with loss of DS-synthesizing enzymes. Mutations in human genes encoding the epimerase and sulfotransferase responsible for the biosynthesis of DS chains cause connective tissue disorders including spondylodysplastic type Ehlers–Danlos syndrome, characterized by skin hyperextensibility, joint hypermobility, and tissue fragility. DS-deficient mice show perinatal lethality, skin fragility, vascular abnormalities, thoracic kyphosis, myopathy-related phenotypes, acceleration of nerve regeneration, and impairments in self-renewal and proliferation of neural stem cells. These findings suggest that DS is essential for tissue development in addition to the assembly of collagen fibrils in the skin, and that DS-deficient knockout mice can be utilized as models of human genetic disorders that involve impairment of DS biosynthesis. This review highlights a novel role of DS in tissue development studies from the past decade.

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Section: Chst14mentioning

confidence: 99%

The Specific Role of Dermatan Sulfate as an Instructive Glycosaminoglycan in Tissue Development

Mizumoto

Yamada

2022

IJMS

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“…Prenatal ultrasound abnormalities sometimes seen in e.g., lysosomal storage diseases (hydrops fetalis) or peroxisome biogenesis disorders (brain anomalies and cystic renal disease), are extremely uncommon in EDS [ 6 ]. The lone exception are the congenital anomalies of the kidney and urinary tract (nephroptosis and ureteropelvic junction obstruction) sometimes observed in musculocontractural EDS (mcEDS) [ 7 ].…”

Section: The Clinical Presentation Of Eds An Overviewmentioning

confidence: 99%

“…Central nervous system abnormalities have been reported only in mcEDS- CHST14 and spEDS- B3GALT6 and include ventricular enlargement, Dandy–Walker anomalies, hypoplasia of the septum pellucidum, hydrocephalus and a tethered spinal cord [ 7 , 12 ]. Intellectual disability is typically not present but has sporadically been reported in families with AR types of EDS.…”

Section: The Clinical Presentation Of Eds An Overviewmentioning

confidence: 99%

“…The facial dysmorphisms in dEDS also combine into a recognizable appearance and include prominent and protuberant eyes with puffy, edematous eyelids and excessive periorbital skin, large fontanels and/or wide cranial sutures, micrognathia and gingival hyperplasia ( Figure 1 M) [ 10 ]. Finally, individuals with mcEDS present with large fontanels, downslanting palpebral fissures, hypertelorism, a short nose with hypoplastic columella, ear deformities, high-arched palate, long philtrum, thin upper lip vermilion, small mouth and microretrognathia ( Figure 1 J) [ 7 , 29 ].…”

Section: The Clinical Presentation Of Eds An Overviewmentioning

confidence: 99%

“…Hearing loss is a key finding in heritable connective tissue disorders, such as osteogenesis imperfecta and Stickler syndrome but is also present in the majority of individuals with kEDS- FKBP14 or mcEDS and a third of the individuals with BCS [ 7 , 12 , 27 ]. Finally, cryptorchidism is present in the large majority of mcEDS- CHST14 individuals and should raise suspicion of mcEDS in a neonate with signs of connective tissue fragility and contractures [ 7 ].…”

Section: The Clinical Presentation Of Eds An Overviewmentioning

confidence: 99%

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The Ehlers–Danlos Syndromes against the Backdrop of Inborn Errors of Metabolism

Damme

Colman

Syx

et al. 2022

Genes

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The Ehlers–Danlos syndromes are a group of multisystemic heritable connective tissue disorders with clinical presentations that range from multiple congenital malformations, over adolescent-onset debilitating or even life-threatening complications of connective tissue fragility, to mild conditions that remain undiagnosed in adulthood. To date, thirteen different EDS types have been recognized, stemming from genetic defects in 20 different genes. While initial biochemical and molecular analyses mainly discovered defects in genes coding for the fibrillar collagens type I, III and V or their modifying enzymes, recent discoveries have linked EDS to defects in non-collagenous matrix glycoproteins, in proteoglycan biosynthesis and in the complement pathway. This genetic heterogeneity explains the important clinical heterogeneity among and within the different EDS types. Generalized joint hypermobility and skin hyperextensibility with cutaneous fragility, atrophic scarring and easy bruising are defining manifestations of EDS; however, other signs and symptoms of connective tissue fragility, such as complications of vascular and internal organ fragility, orocraniofacial abnormalities, neuromuscular involvement and ophthalmological complications are variably present in the different types of EDS. These features may help to differentiate between the different EDS types but also evoke a wide differential diagnosis, including different inborn errors of metabolism. In this narrative review, we will discuss the clinical presentation of EDS within the context of inborn errors of metabolism, give a brief overview of their underlying genetic defects and pathophysiological mechanisms and provide a guide for the diagnostic approach.

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Clinical and pathophysiological delineation of musculocontractural Ehlers—Danlos syndrome caused by dermatan sulfate epimerase deficiency (mcEDS‐ DSE ): A detailed and comprehensive glycobiological and pathological investigation in a novel patient

et al. 2022

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Musculocontractural Ehlers-Danlos syndrome caused by dermatan sulfate epimerase deficiency (mcEDS-DSE) is a rare connective tissue disorder. This is the first report describing the detailed and comprehensive clinical and pathophysiological features of mcEDS-DSE. The patient, with a novel homozygous nonsense variant (NM_013352.4:c.2601C>A:p.(Tyr867*)), exhibited mild skin hyperextensibility without fragility and small joint hypermobility, but developed recurrent large subcutaneous hematomas. Dermatan sulfate (DS) moieties on chondroitin sulfate/DS proteoglycans were significantly decreased, but remained present, in skin fibroblasts. Electron microscopy examination of skin specimens, including cupromeronic blue-staining to visualize glycosaminoglycan (GAG) chains, revealed coexistence of normally assembled collagen fibrils with attached curved GAG chains and dispersed collagen fibrils with linear GAG chains from attached collagen fibrils across interfibrillar spaces to adjacent fibrils. Residual activity of DS-epi1, encoded by DSE, and/or compensation by DS-epi2, a minor homolog of DS-epi1, may contribute to the mild skin involvement through this "mosaic" pattern of collagen fibril assembly.

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Clinical and molecular features of 66 patients with musculocontractural Ehlers−Danlos syndrome caused by pathogenic variants inCHST14(mcEDS-CHST14)

Cited by 20 publications

References 37 publications

The Specific Role of Dermatan Sulfate as an Instructive Glycosaminoglycan in Tissue Development

The Specific Role of Dermatan Sulfate as an Instructive Glycosaminoglycan in Tissue Development

The Ehlers–Danlos Syndromes against the Backdrop of Inborn Errors of Metabolism

Clinical and pathophysiological delineation of musculocontractural Ehlers—Danlos syndrome caused by dermatan sulfate epimerase deficiency (mcEDS‐ DSE ): A detailed and comprehensive glycobiological and pathological investigation in a novel patient

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