Autosomal-Dominant Retinitis Pigmentosa Caused by a Mutation in SNRNP200, a Gene Required for Unwinding of U4/U6 snRNAs

Zhao, Chunxia; Bellur, Deepti L.; Lu, Shasha; Zhao, Feng; Grassi, Michael A.; Bowne, Sara J.; Sullivan, Lori S.; Daiger, Stephen P.; Chen, Li Jia; Pang, Chi Pui; Zhao, Kang; Staley, Jonathan P.; Larsson, Catharina

doi:10.1016/j.ajhg.2009.09.020

Cited by 133 publications

(157 citation statements)

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“…In contrast, another non-synonymous variant p.A1995T, which occurred in both patients and controls, was predicted to be benign, suggesting it is unlikely to be pathogenic. Notably, the three DCMs p.Q885E, p.S1087L, and p.R1090L, which were previously identified in three respective adRP pedigrees from northern China, 21,22,33 were not found in our study. In the first sec-63 domain region, which harbors two of these three mutations (p.S1087L and p.R1090L), only three common SNPs (p.L1184L, p.S1218S, and p.S1230s) and three intronic changes (c.3365 þ 145 G4A, c.3366-25 A4G, and c.3639 þ 53_c.3639 þ 93del) were detected in our study subjects.…”

Section: Discussionmentioning

confidence: 41%

“…The RP33 locus, initially mapped to chromosomal region 2cen-q12.1, was identified in a large Chinese family with adRP. 20 Subsequent studies had identified two mutations, p.S1087L 21 and p.R1090L, 22 in the small nuclear ribonucleoprotein 200 kDa (U5) (SNRNP200, MIM 601664) gene to be segregated with RP in two respective large Chinese adRP families. SNRNP200 is a member of the RNA intron-splicing factor protein family and is widely expressed in human tissues.…”

Section: Introductionmentioning

confidence: 99%

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Contribution of SNRNP200 sequence variations to retinitis pigmentosa

Zhang

Lai

Chiang

et al. 2013

Eye

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Purpose Mutations in the SNRNP200 gene have been reported to cause autosomal dominant retinitis pigmentosa (adRP). In this study, we evaluate the mutation profile of SNRNP200 in a cohort of southern Chinese RP patients. Methods Twenty adRP patients from 11 families and 165 index patients with non-syndromic RP with mixed inheritance patterns were screened for mutations in the mutation hotspots of SNRNP200. These included exons 12-16, 22-32, and 38-45, which covered the two helicase ATP-binding domains in DEAD-box and two sec-63 domains. The targeted regions were amplified by polymerase chain reaction and analyzed by direct DNA sequencing, followed by in silico analyses. Results Totally 26 variants were identified, 18 of which were novel.

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Section: Discussionmentioning

confidence: 41%

Section: Introductionmentioning

confidence: 99%

Contribution of SNRNP200 sequence variations to retinitis pigmentosa

Zhang

Lai

Chiang

et al. 2013

Eye

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“…2C). Consistent with the HB ratchet helix being involved in RNA unwinding, some brr2 mutations linked to the RP33 form of autosomal dominant retinitis pigmentosa in humans [60][61][62] lead to exchanges of RNA-contacting residues in this element (S1087L, R1090L). The S1087L RP33 exchange in human Brr2 reduces RNA affinity as well as ATPase and helicase activities 51 and RP33-like N1104L and R1107L exchanges in yeast Brr2 are associated with reduced ATPdependent U4/U6 unwinding in tri-snRNP preparations.…”

Section: Multiple Layers Of Helicase-associated Domains In Brr2mentioning

confidence: 94%

“…The S1087L RP33 exchange in human Brr2 reduces RNA affinity as well as ATPase and helicase activities 51 and RP33-like N1104L and R1107L exchanges in yeast Brr2 are associated with reduced ATPdependent U4/U6 unwinding in tri-snRNP preparations. 60 Mutation of a Brr2 element equivalent to the Hel308 separator loop resulted in reduction or loss of cell viability, 41,52 in line with a similar duplex disruption mechanism as in Hel308. However, in a yeast U4/U6 U5 tri-snRNP structure, 12 Brr2 is loaded on the U4/U6 di-snRNA with the putative separator loop distant from the U4/U6 duplex portion to be unwound and instead with an edge of the RecA2 domain abutting the end of this duplex region (Fig.…”

Section: Multiple Layers Of Helicase-associated Domains In Brr2mentioning

confidence: 96%

Functions and regulation of the Brr2 RNA helicase during splicing

2016

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Pre-mRNA splicing entails the stepwise assembly of an inactive spliceosome, its catalytic activation, splicing catalysis and spliceosome disassembly. Transitions in this reaction cycle are accompanied by compositional and conformational rearrangements of the underlying RNA-protein interaction networks, which are driven and controlled by 8 conserved superfamily 2 RNA helicases. The Ski2-like helicase, Brr2, provides the key remodeling activity during spliceosome activation and is additionally implicated in the catalytic and disassembly phases of splicing, indicating that Brr2 needs to be tightly regulated during splicing. Recent structural and functional analyses have begun to unravel how Brr2 regulation is established via multiple layers of intra-and inter-molecular mechanisms. Brr2 has an unusual structure, including a long N-terminal region and a catalytically inactive C-terminal helicase cassette, which can auto-inhibit and auto-activate the enzyme, respectively. Both elements are essential, also serve as protein-protein interaction devices and the N-terminal region is required for stable Brr2 association with the tri-snRNP, tri-snRNP stability and retention of U5 and U6 snRNAs during spliceosome activation in vivo. Furthermore, a C-terminal region of the Prp8 protein, comprising consecutive RNase H-like and Jab1/MPN-like domains, can both up-and downregulate Brr2 activity. Biochemical studies revealed an intricate cross-talk among the various cis-and transregulatory mechanisms. Comparison of isolated Brr2 to electron cryo-microscopic structures of yeast and human U4/U6 U5 tri-snRNPs and spliceosomes indicates how some of the regulatory elements exert their functions during splicing. The various modulatory mechanisms acting on Brr2 might be exploited to enhance splicing fidelity and to regulate alternative splicing. KEYWORDSPre-mRNA splicing; regulation of pre-mRNA splicing; remodeling of RNAprotein complexes; RNA helicase structure, function and regulation; spliceosome catalytic activation

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“…The disease onset and progression may vary significantly among patients, even within the same family. The patients frequently experience night blindness in the early phase of the disease, The molecular basis of human retinal and vitreoretinal diseases Collin et al, 2008; den Hollander et al, 1999; Dryja et al, 1995; Gal et al., 2000; Huang et al, 1995; Martinez-Mir et al, 1998;Maw et al, 1997;Maw et al, 2000;McLaughlin et al, 1993; Morimura et al, 1998;Nakazawa et al, 1998; Rivolta et al, 2000;Thompson et al, 2001;Tuson et al, 2004;Zangerl et al, 2006;Zhang et al, 2007b) or dominant (Abid et al, 2006; Bowne et al, 2002; Chakarova et al, 2002; Chakarova et al, 2007;Farrar et al, 1991;Freund et al, 1997;Friedman et al, 2009; Kajiwara et al, 1991; Kajiwara et al, 1994; Keen et al, 2002; Kennan et al, 2002;McKie et al, 2001; Rebello et al, 2004; Sato et al, 2005;Vithana et al, 2001;Wada et al, 2001;Zhang et al, 2007a;Zhao et al, 2009), as well as X-linked (Meindl et al, 1996; Roepman et al, 1996a; Roepman et al, 1996b; Schwahn et al, 1998).Interestingly, mutations in several genes can be either dominant or recessive (Bernal et al, 2008; Bessant et al, 1999; Coppieters et al, 2007;Davidson et al, 2009; Dryja et al, 1990; Morimura et al, 1999; Pierce et al, 1999;Sullivan et al, 1999). The splicing category will now be discussed in more detail.…”

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confidence: 99%

The molecular basis of human retinal and vitreoretinal diseases

Berger¹,

Kloeckener-Gruissem²,

Neidhardt³

2010

Progress in Retinal and Eye Research

490

443

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The molecular basis of human retinal and vitreoretinal diseases pathologies of other tissues (syndromic forms) or only affects the retina, retinal pigment epithelium and the vireous body (non-syndromic forms). In addition, the mode of inheritance was used as one characteristic feature of the different disease phenotypes in order to categorize them. Our aim was to provide a comprehensive overview about the molecular basis of retinal and vitreoretinal diseases and to discuss selected aspects in more detail. Non-syndromic retinal and vitreoretinal diseases Diseases of rod photoreceptor cells (stationary and progressive)Rod photoreceptors represent the vast majority of light sensitive cells in the human retina. There are approximately 20 times more rods than cones. These cells are spezialized for low light intensities and are responsible for visual perception under dim light conditions. The center of the human retina, which contains the macula and fovea centralis, is devoid of rod photoreceptor cells but the flanking areas have the highest rod content, which decreases almost lineary towards the retinal periphery.The two major classes of stationary and progressive retinal diseases in humans arerepresented by different forms of stationary night blindness and retinitis pigmentosa, respectively. Congenital stationary night blindness / stationary rod diseasesAs the name implies, congenital stationary night blindness (CSNB) is a nonprogressive visual impairment present at birth. However, it is also one of the first symptoms in progressive diseases, including retinitis pigmentosa (RP). Therefore, a differential diagnosis by genetic testing can provide helpful and important information to the affected individuals and families, in order to exclude or confirm the clinical diagnosis and to provide counselling. Bech-Hansen et al., 1998; Bech-Hansen et al., 2000;Dryja et al., 1993; Dryja et al., 1996; Dryja et al., 2005; Fuchs et al., 1995;Gal et al., 1994;Li et al., 2009; Pusch et al., 2000;Strom et al., 1998;Wycisk et al., 2006;Yamamoto et al., 1997;Zeitz et al., 2005;Zeitz et al., 2006 inheritance. The disease was found to be due to mutations in the alpha subunit of transducin (Dryja et al., 1996). The Schubert Bornschein disease can be subdivided in (i) CSNB1 or complete CSNB and (ii) CSNB2 or incomplete CSNB. In CSNB1, the rod b-wave is significantly reduced or absent, while that of the cones is largely Retinitis pigmentosa and progressive rod cone diseasesThe term retinitis pigmentosa (RP) describes a group of clinically similar phenotypes associated with genetically heterogeneous causes. The disease onset and progression may vary significantly among patients, even within the same family. The patients frequently experience night blindness in the early phase of the disease, The molecular basis of human retinal and vitreoretinal diseases Collin et al., 2008; den Hollander et al., 1999; Dryja et al., 1995; Gal et al., 2000; Huang et al., 1995; Martinez-Mir et al., 1998;Maw et al., 1997;Maw et al., 2000;McLaughlin et a...

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Autosomal-Dominant Retinitis Pigmentosa Caused by a Mutation in SNRNP200, a Gene Required for Unwinding of U4/U6 snRNAs

Cited by 133 publications

References 52 publications

Contribution of SNRNP200 sequence variations to retinitis pigmentosa

Contribution of SNRNP200 sequence variations to retinitis pigmentosa

Functions and regulation of the Brr2 RNA helicase during splicing

The molecular basis of human retinal and vitreoretinal diseases

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