Pathogenic mutations in TULP1 responsible for retinitis pigmentosa identified in consanguineous familial cases

PURPOSE: To identify pathogenic mutations responsible for autosomal recessive retinitis pigmentosa (arRP) in consanguineous familial cases. METHODS: Seven large familial cases with multiple individuals diagnosed with retinitis pigmentosa were included in the study. Affected individuals in these fami...

Descripción completa

Detalles Bibliográficos
Autores principales: Ullah, Inayat, Kabir, Firoz, Iqbal, Muhammad, Gottsch, Clare Brooks S., Naeem, Muhammad Asif, Assir, Muhammad Zaman, Khan, Shaheen N., Akram, Javed, Riazuddin, Sheikh, Ayyagari, Radha, Hejtmancik, J. Fielding, Riazuddin, S. Amer
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Molecular Vision 2016
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4947966/
https://www.ncbi.nlm.nih.gov/pubmed/27440997
_version_ 1782443260551102464
author Ullah, Inayat
Kabir, Firoz
Iqbal, Muhammad
Gottsch, Clare Brooks S.
Naeem, Muhammad Asif
Assir, Muhammad Zaman
Khan, Shaheen N.
Akram, Javed
Riazuddin, Sheikh
Ayyagari, Radha
Hejtmancik, J. Fielding
Riazuddin, S. Amer
author_facet Ullah, Inayat
Kabir, Firoz
Iqbal, Muhammad
Gottsch, Clare Brooks S.
Naeem, Muhammad Asif
Assir, Muhammad Zaman
Khan, Shaheen N.
Akram, Javed
Riazuddin, Sheikh
Ayyagari, Radha
Hejtmancik, J. Fielding
Riazuddin, S. Amer
author_sort Ullah, Inayat
collection PubMed
description PURPOSE: To identify pathogenic mutations responsible for autosomal recessive retinitis pigmentosa (arRP) in consanguineous familial cases. METHODS: Seven large familial cases with multiple individuals diagnosed with retinitis pigmentosa were included in the study. Affected individuals in these families underwent ophthalmic examinations to document the symptoms and confirm the initial diagnosis. Blood samples were collected from all participating members, and genomic DNA was extracted. An exclusion analysis with microsatellite markers spanning the TULP1 locus on chromosome 6p was performed, and two-point logarithm of odds (LOD) scores were calculated. All coding exons along with the exon–intron boundaries of TULP1 were sequenced bidirectionally. We constructed a single nucleotide polymorphism (SNP) haplotype for the four familial cases harboring the K489R allele and estimated the likelihood of a founder effect. RESULTS: The ophthalmic examinations of the affected individuals in these familial cases were suggestive of RP. Exclusion analyses confirmed linkage to chromosome 6p harboring TULP1 with positive two-point LOD scores. Subsequent Sanger sequencing identified the single base pair substitution in exon14, c.1466A>G (p.K489R), in four families. Additionally, we identified a two-base deletion in exon 4, c.286_287delGA (p.E96Gfs77*); a homozygous splice site variant in intron 14, c.1495+4A>C; and a novel missense variation in exon 15, c.1561C>T (p.P521S). All mutations segregated with the disease phenotype in the respective families and were absent in ethnically matched control chromosomes. Haplotype analysis suggested (p<10(−6)) that affected individuals inherited the causal mutation from a common ancestor. CONCLUSIONS: Pathogenic mutations in TULP1 are responsible for the RP phenotype in seven familial cases with a common ancestral mutation responsible for the disease phenotype in four of the seven families.
format Online
Article
Text
id pubmed-4947966
institution National Center for Biotechnology Information
language English
publishDate 2016
publisher Molecular Vision
record_format MEDLINE/PubMed
spelling pubmed-49479662016-07-20 Pathogenic mutations in TULP1 responsible for retinitis pigmentosa identified in consanguineous familial cases Ullah, Inayat Kabir, Firoz Iqbal, Muhammad Gottsch, Clare Brooks S. Naeem, Muhammad Asif Assir, Muhammad Zaman Khan, Shaheen N. Akram, Javed Riazuddin, Sheikh Ayyagari, Radha Hejtmancik, J. Fielding Riazuddin, S. Amer Mol Vis Research Article PURPOSE: To identify pathogenic mutations responsible for autosomal recessive retinitis pigmentosa (arRP) in consanguineous familial cases. METHODS: Seven large familial cases with multiple individuals diagnosed with retinitis pigmentosa were included in the study. Affected individuals in these families underwent ophthalmic examinations to document the symptoms and confirm the initial diagnosis. Blood samples were collected from all participating members, and genomic DNA was extracted. An exclusion analysis with microsatellite markers spanning the TULP1 locus on chromosome 6p was performed, and two-point logarithm of odds (LOD) scores were calculated. All coding exons along with the exon–intron boundaries of TULP1 were sequenced bidirectionally. We constructed a single nucleotide polymorphism (SNP) haplotype for the four familial cases harboring the K489R allele and estimated the likelihood of a founder effect. RESULTS: The ophthalmic examinations of the affected individuals in these familial cases were suggestive of RP. Exclusion analyses confirmed linkage to chromosome 6p harboring TULP1 with positive two-point LOD scores. Subsequent Sanger sequencing identified the single base pair substitution in exon14, c.1466A>G (p.K489R), in four families. Additionally, we identified a two-base deletion in exon 4, c.286_287delGA (p.E96Gfs77*); a homozygous splice site variant in intron 14, c.1495+4A>C; and a novel missense variation in exon 15, c.1561C>T (p.P521S). All mutations segregated with the disease phenotype in the respective families and were absent in ethnically matched control chromosomes. Haplotype analysis suggested (p<10(−6)) that affected individuals inherited the causal mutation from a common ancestor. CONCLUSIONS: Pathogenic mutations in TULP1 are responsible for the RP phenotype in seven familial cases with a common ancestral mutation responsible for the disease phenotype in four of the seven families. Molecular Vision 2016-07-16 /pmc/articles/PMC4947966/ /pubmed/27440997 Text en Copyright © 2016 Molecular Vision. http://creativecommons.org/licenses/by-nc-nd/3.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited, used for non-commercial purposes, and is not altered or transformed.
spellingShingle Research Article
Ullah, Inayat
Kabir, Firoz
Iqbal, Muhammad
Gottsch, Clare Brooks S.
Naeem, Muhammad Asif
Assir, Muhammad Zaman
Khan, Shaheen N.
Akram, Javed
Riazuddin, Sheikh
Ayyagari, Radha
Hejtmancik, J. Fielding
Riazuddin, S. Amer
Pathogenic mutations in TULP1 responsible for retinitis pigmentosa identified in consanguineous familial cases
title Pathogenic mutations in TULP1 responsible for retinitis pigmentosa identified in consanguineous familial cases
title_full Pathogenic mutations in TULP1 responsible for retinitis pigmentosa identified in consanguineous familial cases
title_fullStr Pathogenic mutations in TULP1 responsible for retinitis pigmentosa identified in consanguineous familial cases
title_full_unstemmed Pathogenic mutations in TULP1 responsible for retinitis pigmentosa identified in consanguineous familial cases
title_short Pathogenic mutations in TULP1 responsible for retinitis pigmentosa identified in consanguineous familial cases
title_sort pathogenic mutations in tulp1 responsible for retinitis pigmentosa identified in consanguineous familial cases
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4947966/
https://www.ncbi.nlm.nih.gov/pubmed/27440997
work_keys_str_mv AT ullahinayat pathogenicmutationsintulp1responsibleforretinitispigmentosaidentifiedinconsanguineousfamilialcases
AT kabirfiroz pathogenicmutationsintulp1responsibleforretinitispigmentosaidentifiedinconsanguineousfamilialcases
AT iqbalmuhammad pathogenicmutationsintulp1responsibleforretinitispigmentosaidentifiedinconsanguineousfamilialcases
AT gottschclarebrookss pathogenicmutationsintulp1responsibleforretinitispigmentosaidentifiedinconsanguineousfamilialcases
AT naeemmuhammadasif pathogenicmutationsintulp1responsibleforretinitispigmentosaidentifiedinconsanguineousfamilialcases
AT assirmuhammadzaman pathogenicmutationsintulp1responsibleforretinitispigmentosaidentifiedinconsanguineousfamilialcases
AT khanshaheenn pathogenicmutationsintulp1responsibleforretinitispigmentosaidentifiedinconsanguineousfamilialcases
AT akramjaved pathogenicmutationsintulp1responsibleforretinitispigmentosaidentifiedinconsanguineousfamilialcases
AT riazuddinsheikh pathogenicmutationsintulp1responsibleforretinitispigmentosaidentifiedinconsanguineousfamilialcases
AT ayyagariradha pathogenicmutationsintulp1responsibleforretinitispigmentosaidentifiedinconsanguineousfamilialcases
AT hejtmancikjfielding pathogenicmutationsintulp1responsibleforretinitispigmentosaidentifiedinconsanguineousfamilialcases
AT riazuddinsamer pathogenicmutationsintulp1responsibleforretinitispigmentosaidentifiedinconsanguineousfamilialcases

Ejemplares similares