Structural and functional plasticity of subcellular tethering, targeting and processing of RPGRIP1 by RPGR isoforms

Mutations affecting the retinitis pigmentosa GTPase regulator-interacting protein 1 (RPGRIP1) interactome cause syndromic retinal dystrophies. RPGRIP1 interacts with the retinitis pigmentosa GTPase regulator (RPGR) through a domain homologous to RCC1 (RHD), a nucleotide exchange factor of Ran GTPase...

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Autores principales: Patil, Hemangi, Guruju, Mallikarjuna R., Cho, Kyoung-in, Yi, Haiqing, Orry, Andrew, Kim, Hyesung, Ferreira, Paulo A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The Company of Biologists 2011
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3507198/
https://www.ncbi.nlm.nih.gov/pubmed/23213406
http://dx.doi.org/10.1242/bio.2011489
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author Patil, Hemangi
Guruju, Mallikarjuna R.
Cho, Kyoung-in
Yi, Haiqing
Orry, Andrew
Kim, Hyesung
Ferreira, Paulo A.
author_facet Patil, Hemangi
Guruju, Mallikarjuna R.
Cho, Kyoung-in
Yi, Haiqing
Orry, Andrew
Kim, Hyesung
Ferreira, Paulo A.
author_sort Patil, Hemangi
collection PubMed
description Mutations affecting the retinitis pigmentosa GTPase regulator-interacting protein 1 (RPGRIP1) interactome cause syndromic retinal dystrophies. RPGRIP1 interacts with the retinitis pigmentosa GTPase regulator (RPGR) through a domain homologous to RCC1 (RHD), a nucleotide exchange factor of Ran GTPase. However, functional relationships between RPGR and RPGRIP1 and their subcellular roles are lacking. We show by molecular modeling and analyses of RPGR disease-mutations that the RPGR-interacting domain (RID) of RPGRIP1 embraces multivalently the shared RHD of RPGR(1–19) and RPGR(ORF15) isoforms and the mutations are non-overlapping with the interface found between RCC1 and Ran GTPase. RPGR disease-mutations grouped into six classes based on their structural locations and differential impairment with RPGRIP1 interaction. RPGRIP1α(1) expression alone causes its profuse self-aggregation, an effect suppressed by co-expression of either RPGR isoform before and after RPGRIP1α(1) self-aggregation ensue. RPGR(1–19) localizes to the endoplasmic reticulum, whereas RPGR(ORF15) presents cytosolic distribution and they determine uniquely the subcellular co-localization of RPGRIP1α(1). Disease mutations in RPGR(1)(–19), RPGR(ORF15), or RID of RPGRIP1α(1), singly or in combination, exert distinct effects on the subcellular targeting, co-localization or tethering of RPGRIP1α(1) with RPGR(1–19) or RPGR(ORF15) in kidney, photoreceptor and hepatocyte cell lines. Additionally, RPGR(ORF15), but not RPGR(1–19), protects the RID of RPGRIP1α(1) from limited proteolysis. These studies define RPGR- and cell-type-dependent targeting pathways with structural and functional plasticity modulating the expression of mutations in RPGR and RPGRIP1. Further, RPGR isoforms distinctively determine the subcellular targeting of RPGRIP1α(1,) with deficits in RPGR(ORF15)-dependent intracellular localization of RPGRIP1α(1) contributing to pathomechanisms shared by etiologically distinct syndromic retinal dystrophies.
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spelling pubmed-35071982012-12-04 Structural and functional plasticity of subcellular tethering, targeting and processing of RPGRIP1 by RPGR isoforms Patil, Hemangi Guruju, Mallikarjuna R. Cho, Kyoung-in Yi, Haiqing Orry, Andrew Kim, Hyesung Ferreira, Paulo A. Biol Open Research Article Mutations affecting the retinitis pigmentosa GTPase regulator-interacting protein 1 (RPGRIP1) interactome cause syndromic retinal dystrophies. RPGRIP1 interacts with the retinitis pigmentosa GTPase regulator (RPGR) through a domain homologous to RCC1 (RHD), a nucleotide exchange factor of Ran GTPase. However, functional relationships between RPGR and RPGRIP1 and their subcellular roles are lacking. We show by molecular modeling and analyses of RPGR disease-mutations that the RPGR-interacting domain (RID) of RPGRIP1 embraces multivalently the shared RHD of RPGR(1–19) and RPGR(ORF15) isoforms and the mutations are non-overlapping with the interface found between RCC1 and Ran GTPase. RPGR disease-mutations grouped into six classes based on their structural locations and differential impairment with RPGRIP1 interaction. RPGRIP1α(1) expression alone causes its profuse self-aggregation, an effect suppressed by co-expression of either RPGR isoform before and after RPGRIP1α(1) self-aggregation ensue. RPGR(1–19) localizes to the endoplasmic reticulum, whereas RPGR(ORF15) presents cytosolic distribution and they determine uniquely the subcellular co-localization of RPGRIP1α(1). Disease mutations in RPGR(1)(–19), RPGR(ORF15), or RID of RPGRIP1α(1), singly or in combination, exert distinct effects on the subcellular targeting, co-localization or tethering of RPGRIP1α(1) with RPGR(1–19) or RPGR(ORF15) in kidney, photoreceptor and hepatocyte cell lines. Additionally, RPGR(ORF15), but not RPGR(1–19), protects the RID of RPGRIP1α(1) from limited proteolysis. These studies define RPGR- and cell-type-dependent targeting pathways with structural and functional plasticity modulating the expression of mutations in RPGR and RPGRIP1. Further, RPGR isoforms distinctively determine the subcellular targeting of RPGRIP1α(1,) with deficits in RPGR(ORF15)-dependent intracellular localization of RPGRIP1α(1) contributing to pathomechanisms shared by etiologically distinct syndromic retinal dystrophies. The Company of Biologists 2011-12-30 /pmc/articles/PMC3507198/ /pubmed/23213406 http://dx.doi.org/10.1242/bio.2011489 Text en © 2012. Published by The Company of Biologists Ltd http://creativecommons.org/licenses/by-nc-sa/3.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial Share Alike License (http://creativecommons.org/licenses/by-nc-sa/3.0/).
spellingShingle Research Article
Patil, Hemangi
Guruju, Mallikarjuna R.
Cho, Kyoung-in
Yi, Haiqing
Orry, Andrew
Kim, Hyesung
Ferreira, Paulo A.
Structural and functional plasticity of subcellular tethering, targeting and processing of RPGRIP1 by RPGR isoforms
title Structural and functional plasticity of subcellular tethering, targeting and processing of RPGRIP1 by RPGR isoforms
title_full Structural and functional plasticity of subcellular tethering, targeting and processing of RPGRIP1 by RPGR isoforms
title_fullStr Structural and functional plasticity of subcellular tethering, targeting and processing of RPGRIP1 by RPGR isoforms
title_full_unstemmed Structural and functional plasticity of subcellular tethering, targeting and processing of RPGRIP1 by RPGR isoforms
title_short Structural and functional plasticity of subcellular tethering, targeting and processing of RPGRIP1 by RPGR isoforms
title_sort structural and functional plasticity of subcellular tethering, targeting and processing of rpgrip1 by rpgr isoforms
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3507198/
https://www.ncbi.nlm.nih.gov/pubmed/23213406
http://dx.doi.org/10.1242/bio.2011489
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