WRNIP1

Information WRNIP1

Description

Werner's syndrome is a rare autosomal recessive disorder characterized by accelerated aging that is caused by defects in the Werner syndrome ATP-dependent helicase gene (WRN). The protein encoded by this gene interacts with the exonuclease-containing N-terminal portion of the Werner protein. This protein has a ubiquitin-binding zinc-finger domain in the N-terminus, an ATPase domain, and two leucine zipper motifs in the C-terminus. It has sequence similarity to replication factor C family proteins and is conserved from E. coli to human. This protein likely accumulates at sites of DNA damage by interacting with polyubiquinated proteins and also binds to DNA polymerase delta and increases the initiation frequency of DNA polymerase delta-mediated DNA synthesis. This protein also interacts with nucleoporins at nuclear pore complexes. Two transcript variants encoding different isoforms have been isolated for this gene. [provided by RefSeq, Jul 2012]

Full Name

WRN helicase interacting protein 1

Source NCBI

ReMap Statistics

Datasets
1
Biotypes
1
Peaks
67
Non-redundant peaks
67

TF Classification

Super Class
Unknown
Class
Unknown
Familly
Unknown
Sub Familly
Unknown

Source TFClass

External IDs

JASPAR
Ensembl
ENSG00000124535
UniProt
Q96S55
Genevisible
Q96S55
RefSeq
NM_020135
Aliases
FLJ22526; WHIP; bA420G6.2
All peaks WRNIP1
Download BED file
Non redundant peaks WRNIP1
Download BED file
SEQUENCES WRNIP1
Download FASTA file
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Datasets Table for WRNIP1

Target name Target modification Ecotype/Strain Biotype Biotype modification Source Species Experiment Peaks
WRNIP1 GM12878 ENCODE Homo sapiens ENCSR000EAA 67
Target name Target modification Ecotype/Strain Biotype Biotype modification Source Species Experiment Peaks

ReMap is a database of transcriptional regulators peaks derived from curated ChIP-seq, ChIP-exo, DAP-seq experiments in Human and Thaliana.

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The ReMap catalogues (2020, 2018, 2015) are under CC BY-NC 4.0 international license, while ReMapEnrich, remap-pipeline under GNU GPLv3 licence.

Inserm TAGC
AMU AMU-MESO

This work was granted access to the HPC resources of Aix-Marseille Université financed by the project Equip@Meso (ANR-10-EQPX-29-01) of the program "Investissements d’Avenir" supervised by the Agence Nationale de la Recherche.