A <i>HS6ST2</i> gene variant associated with X‐linked intellectual disability and severe myopia in two male twins

Paganini, Leda; Hadi, Loubna Abdel; Chetta, Massimiliano; Rovina, Davide; Fontana, Laura; Colapietro, Patrizia; Bonaparte, Eleonora; Pezzani, Lidia; Marchisio, Paola; Tabano, Silvia; Costanza, Jole; Sirchia, Silvia Maria; Riboni, Laura; Milani, Donatella; Miozzo, Monica

doi:10.1111/cge.13485

Cited by 18 publications

(13 citation statements)

References 23 publications

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“…The last XLID update published, estimated that 141 genes are associated with XLID. Since then, more genes have been associated to XLID such as CXorf56 , HS6ST2 , NAA15 , POLA1 and SLC9A7 (Figure ). However, the link of some of these genes to XLID is still questionable .…”

Section: Introductionmentioning

confidence: 99%

Non‐syndromic X linked intellectual disability: Current knowledge in light of the recent advances in molecular and functional studies

Tejada

Ibarluzea

2020

Clinical Genetics

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Since the discovery of the FMR1 gene and the clinical and molecular characterization of Fragile X Syndrome in 1991, more than 141 genes have been identified in the Xchromosome in these 28 years thanks to applying continuously evolving molecular techniques to X-linked intellectual disability (XLID) families. In the past decade, array comparative genomic hybridization and next generation sequencing technologies have accelerated gene discovery exponentially. Classically, XLID has been subdivided in syndromic intellectual disability (S-XLID)-where intellectual disability (ID) is always associated with other recognizable physical and/or neurological features-and non-specific or non-syndromic intellectual disability (NS-XLID) where the only common feature is ID. Nevertheless, new advances on the study of these entities have showed that this classification is not always clear-cut because distinct variants in several of these XLID genes can result in S-XLID as well as in NS-XLID. This review focuses on the current knowledge on the XLID genes involved in non-syndromic forms, with the emphasis on their pathogenic mechanism, thus allowing the possibility to elucidate why some of them can give both syndromic and non-syndromic phenotypes.

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Section: Introductionmentioning

confidence: 99%

Non‐syndromic X linked intellectual disability: Current knowledge in light of the recent advances in molecular and functional studies

Tejada

Ibarluzea

2020

Clinical Genetics

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“…Inf). Genes in Group IV included those coding for two core proteins ( GPC2 90-92 and GPC5 93-95 ), three NDSTs ( NDST2 96-98 , NDST3 99-101 , and NDST4 102,103 ), two HS6STs ( HS6ST2 104,105 , HS6ST3 106,107 ), all HS3STs ( HS3ST1 108-110 , HS3ST2 111,112 , HS3ST3A1 113-115 , HS3ST3B1 115 , HS3ST4 116 , HS3ST5 117 , and HS3ST6 118,119 ), and one HS levels regulating genes (EXTL1 120 ). Based in current available data and literature records, it appeared that, at least in the absence of instigating stimuli, these genes are non-causative of disease and are not essential for normal development and homeostasis (Supp.…”

Section: Resultsmentioning

confidence: 99%

Variability in proteoglycan biosynthetic genes reveals new facets of heparan sulfates diversity. A systematic review and analysis

Ouidja

Biard

Chantepie

et al. 2022

Preprint

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Proteoglycans are complex macromolecules formed of glycosaminoglycan chains covalently linked to core proteins through a linker tetrasaccharide common to heparan sulfate proteoglycans (HSPG) and chondroitin sulfate proteoglycans (CSPG). Biosynthesis of a single proteoglycan requires the expression of dozens of genes, which together create the large structural and functional diversity reflected by the numerous diseases or syndromes associated to their genetic variability. Among proteoglycans, HSPG are the most structurally and functionally complex. To decrease this complexity, we retrieved and linked information on pathogenic variants, polymorphism, expression, and literature databases for 50 genes involved in the biosynthesis of HSPG core proteins, heparan sulfate (HS) chains, and their linker tetrasaccharide. This resulted in a new gene organization and biosynthetic pathway representation in which the phenotypic continuum of disorders as linkeropathies and other pathologies could be predictable. Moreover, ubiquitous NDST1, GLCE, HS2ST1, and HS6ST1 appeared to generate ubiquitous heparan sulfate (HS) sequences essential for normal development and homeostasis, whereas the tissue restricted NDST2-4, HS6ST2-3, and HS3ST1-6 appeared to generate specialized HS sequences mainly involved in responsiveness to stimuli. Supported by data on genetic polymorphism and clinical variants, we afford a new vision of HSPG involvement in homeostasis, disease, vulnerability to disease, and behavioral disorders.

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“…Therefore, together with these reports, our findings indicate the possibility that fully sulfated HS in cell types that express Cre under L7 promotor control plays a previously unsuspected role in the regulation of female reproductive behavior. Further support for essential HS functions in normal brain physiology comes from the observations that Ndst1 is a candidate gene for autosomal recessive intellectual disability in four unrelated families [ 64 , 65 ], that the Drosophila Ndst orthologue Sulfateless plays a role in normal social interactions and repetitive behavior in the fly [ 66 ], that Glypican 4 associates with hyperactivity and social interaction deficits in mice [ 67 ], and that a HS 6-O sulfotransferase gene variant associates with intellectual disability in humans [ 68 ].…”

Section: Discussionmentioning

confidence: 99%

Cerebellar Morphology and Behavioral Profiles in Mice Lacking Heparan Sulfate Ndst Gene Function

Lewejohann

Pallerla

Schreiber

et al. 2020

JDB

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Disruption of the Heparan sulfate (HS)-biosynthetic gene N-acetylglucosamine N-Deacetylase/N-sulfotransferase 1 (Ndst1) during nervous system development causes malformations that are composites of those caused by mutations of multiple HS binding growth factors and morphogens. However, the role of Ndst function in adult brain physiology is less explored. Therefore, we generated mice bearing a Purkinje-cell-specific deletion in Ndst1 gene function by using Cre/loxP technology under the control of the Purkinje cell protein 2 (Pcp2/L7) promotor, which results in HS undersulfation. We observed that mutant mice did not show overt changes in the density or organization of Purkinje cells in the adult cerebellum, and behavioral tests also demonstrated normal cerebellar function. This suggested that postnatal Purkinje cell development and homeostasis are independent of Ndst1 function, or that impaired HS sulfation upon deletion of Ndst1 function may be compensated for by other Purkinje cell-expressed Ndst isoforms. To test the latter possibility, we additionally deleted the second Purkinje-cell expressed Ndst family member, Ndst2. This selectively abolished reproductive capacity of compound mutant female, but not male, mice, suggesting that ovulation, gestation, or female reproductive behavior specifically depends on Ndst-dependent HS sulfation in cells types that express Cre under Pcp2/L7 promotor control.

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A HS6ST2 gene variant associated with X‐linked intellectual disability and severe myopia in two male twins

Cited by 18 publications

References 23 publications

Non‐syndromic X linked intellectual disability: Current knowledge in light of the recent advances in molecular and functional studies

Non‐syndromic X linked intellectual disability: Current knowledge in light of the recent advances in molecular and functional studies

Variability in proteoglycan biosynthetic genes reveals new facets of heparan sulfates diversity. A systematic review and analysis

Cerebellar Morphology and Behavioral Profiles in Mice Lacking Heparan Sulfate Ndst Gene Function

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