FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2005161874> ?p ?o ?g. }

• W2005161874 endingPage "4355" @default.
• W2005161874 startingPage "4350" @default.
• W2005161874 abstract "The peroxisome biogenesis disorders (PBDs), including Zellweger syndrome (ZS) and neonatal adrenoleukodystrophy (NALD), are autosomal recessive diseases caused by defects in peroxisome assembly, for which at least 10 complementation groups have been reported. We have isolated a human PEX1 cDNA (HsPEX1) by functional complementation of peroxisome deficiency of a mutant Chinese hamster ovary (CHO) cell line, ZP107, transformed with peroxisome targeting signal type 1-tagged enhanced green fluorescent protein. This cDNA encodes a hydrophilic protein (Pex1p) comprising 1,283 amino acids, with high homology to the AAA-type ATPase family. A stable transformant of ZP107 with HsPEX1 was morphologically and biochemically restored for peroxisome biogenesis. HsPEX1 expression restored peroxisomal protein import in fibroblasts from three patients with ZS and NALD of complementation group I (CG-I), which is the highest-incidence PBD. A CG-I ZS patient (PBDE-04) possessed compound heterozygous, inactivating mutations: a missense point mutation resulting in Leu-664 --> Pro and a deletion of the sequence from Gly-634 to His-690 presumably caused by missplicing (splice site mutation). Both PBDE-04 PEX1 cDNAs were defective in peroxisome-restoring activity when expressed in the patient fibroblasts as well as in ZP107 cells. These results demonstrate that PEX1 is the causative gene for CG-I peroxisomal disorders." @default.
• W2005161874 created "2016-06-24" @default.
• W2005161874 creator A5019838562 @default.
• W2005161874 creator A5020873351 @default.
• W2005161874 creator A5025587218 @default.
• W2005161874 creator A5025717497 @default.
• W2005161874 creator A5028105316 @default.
• W2005161874 creator A5040212346 @default.
• W2005161874 creator A5053489078 @default.
• W2005161874 creator A5084299482 @default.
• W2005161874 creator A5088922470 @default.
• W2005161874 date "1998-04-14" @default.
• W2005161874 modified "2023-10-18" @default.
• W2005161874 title "Human <i>PEX1</i> cloned by functional complementation on a CHO cell mutant is responsible for peroxisome-deficient Zellweger syndrome of complementation group I" @default.
• W2005161874 cites W1574033922 @default.
• W2005161874 cites W1579185341 @default.
• W2005161874 cites W1666218407 @default.
• W2005161874 cites W1966799030 @default.
• W2005161874 cites W1984636211 @default.
• W2005161874 cites W1987049546 @default.
• W2005161874 cites W1992671721 @default.
• W2005161874 cites W1995333381 @default.
• W2005161874 cites W2001978708 @default.
• W2005161874 cites W2006120283 @default.
• W2005161874 cites W2012634302 @default.
• W2005161874 cites W2016668878 @default.
• W2005161874 cites W2019327981 @default.
• W2005161874 cites W2025104020 @default.
• W2005161874 cites W2025220071 @default.
• W2005161874 cites W2027647762 @default.
• W2005161874 cites W2033241541 @default.
• W2005161874 cites W2047667305 @default.
• W2005161874 cites W2050010612 @default.
• W2005161874 cites W2060624652 @default.
• W2005161874 cites W2065260095 @default.
• W2005161874 cites W2067747241 @default.
• W2005161874 cites W2071948477 @default.
• W2005161874 cites W2073972553 @default.
• W2005161874 cites W2076077839 @default.
• W2005161874 cites W2083543206 @default.
• W2005161874 cites W2083645809 @default.
• W2005161874 cites W2084938165 @default.
• W2005161874 cites W2091630923 @default.
• W2005161874 cites W2092037755 @default.
• W2005161874 cites W2092362067 @default.
• W2005161874 cites W2094238059 @default.
• W2005161874 cites W2100174362 @default.
• W2005161874 cites W2106046158 @default.
• W2005161874 cites W2108827974 @default.
• W2005161874 cites W2112107786 @default.
• W2005161874 cites W2130093817 @default.
• W2005161874 cites W2130944611 @default.
• W2005161874 cites W2132762612 @default.
• W2005161874 cites W2134678739 @default.
• W2005161874 cites W2140309519 @default.
• W2005161874 cites W2158019552 @default.
• W2005161874 cites W223368339 @default.
• W2005161874 cites W2413107236 @default.
• W2005161874 cites W2465014722 @default.
• W2005161874 cites W2468917902 @default.
• W2005161874 cites W4233808990 @default.
• W2005161874 doi "https://doi.org/10.1073/pnas.95.8.4350" @default.
• W2005161874 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/22492" @default.
• W2005161874 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/9539740" @default.
• W2005161874 hasPublicationYear "1998" @default.
• W2005161874 type Work @default.
• W2005161874 sameAs 2005161874 @default.
• W2005161874 citedByCount "92" @default.
• W2005161874 countsByYear W20051618742012 @default.
• W2005161874 countsByYear W20051618742014 @default.
• W2005161874 countsByYear W20051618742016 @default.
• W2005161874 countsByYear W20051618742018 @default.
• W2005161874 countsByYear W20051618742019 @default.
• W2005161874 countsByYear W20051618742020 @default.
• W2005161874 countsByYear W20051618742021 @default.
• W2005161874 countsByYear W20051618742023 @default.
• W2005161874 crossrefType "journal-article" @default.
• W2005161874 hasAuthorship W2005161874A5019838562 @default.
• W2005161874 hasAuthorship W2005161874A5020873351 @default.
• W2005161874 hasAuthorship W2005161874A5025587218 @default.
• W2005161874 hasAuthorship W2005161874A5025717497 @default.
• W2005161874 hasAuthorship W2005161874A5028105316 @default.
• W2005161874 hasAuthorship W2005161874A5040212346 @default.
• W2005161874 hasAuthorship W2005161874A5053489078 @default.
• W2005161874 hasAuthorship W2005161874A5084299482 @default.
• W2005161874 hasAuthorship W2005161874A5088922470 @default.
• W2005161874 hasBestOaLocation W20051618741 @default.
• W2005161874 hasConcept C104317684 @default.
• W2005161874 hasConcept C127078168 @default.
• W2005161874 hasConcept C143065580 @default.
• W2005161874 hasConcept C153911025 @default.
• W2005161874 hasConcept C170493617 @default.
• W2005161874 hasConcept C175656101 @default.
• W2005161874 hasConcept C188082640 @default.
• W2005161874 hasConcept C2777485865 @default.
• W2005161874 hasConcept C2781317408 @default.
• W2005161874 hasConcept C54355233 @default.
• W2005161874 hasConcept C86803240 @default.

• next