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Chloride channels are a diverse group of proteins that regulate fundamental cellular processes including stabilization of cell membrane potential, transepithelial transport, maintenance of intracellular pH, and regulation of cell volume. Additionally we are shipping CLIC1 Kits (12) and CLIC1 Proteins (12) and many more products for this protein.
Showing 10 out of 115 products:
Human Polyclonal CLIC1 Primary Antibody for WB - ABIN1881210
Valenzuela, Martin, Por, Robbins, Warton, Bootcov, Schofield, Campbell, Breit: Molecular cloning and expression of a chloride ion channel of cell nuclei. in The Journal of biological chemistry 1997
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Human Monoclonal CLIC1 Primary Antibody for IF, IHC (p) - ABIN560404
Megger, Bracht, Kohl, Ahrens, Naboulsi, Weber, Hoffmann, Stephan, Kuhlmann, Eisenacher, Schlaak, Baba, Meyer, Sitek: Proteomic differences between hepatocellular carcinoma and nontumorous liver tissue investigated by a combined gel-based and label-free quantitative proteomics study. in Molecular & cellular proteomics : MCP 2013
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Human Monoclonal CLIC1 Primary Antibody for IHC (p), ELISA - ABIN560405
Chaze, Meunier, Chambon, Jurie, Picard: Proteome dynamics during contractile and metabolic differentiation of bovine foetal muscle. in Animal : an international journal of animal bioscience 2012
Cow (Bovine) Polyclonal CLIC1 Primary Antibody for IHC, WB - ABIN2776130
Novarino, Fabrizi, Tonini, Denti, Malchiodi-Albedi, Lauro, Sacchetti, Paradisi, Ferroni, Curmi, Breit, Mazzanti: Involvement of the intracellular ion channel CLIC1 in microglia-mediated beta-amyloid-induced neurotoxicity. in The Journal of neuroscience : the official journal of the Society for Neuroscience 2004
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After CLIC1 knockdown, the expression levels of ITGalpha3, ITGalphav, ITGbeta1 and Bcl-2 (show BCL2 Antibodies) mRNA and protein were decreased significantly in gastric cancer cells, as well as AKT (show AKT1 Antibodies)-phosphorylation, ERK (show EPHB2 Antibodies)-phosphorylation and p38 (show CRK Antibodies)-phosphorylation, were reduced in vivo.
The current study provides the first statistically convincing evidence that downregulation of miR (show MLXIP Antibodies)-372 may occur in gallbladder cancer tissues, which may be associated with aggressive and progressive tumor behavior by affecting CLIC1 expression.
The CLIC1-mediated drug resistance is achieved through positive regulation of MRP1 (show MDM4 Antibodies) in choriocarcinoma.CLIC1 is highly expressed in chemoresistant choriocarcinoma.
Proteomic analysis indicates that CLIC1 promotes tumorgenesis in epithelial ovarian cancer.
CLIC1 is a possible tumor marker for ovarian cancer. Dendritic cells pulsed with MtHsp70 (show HSPA9 Antibodies)-CLIC1 can enhance antitumor immunity against ovarian cancer, providing a novel immune therapeutic strategy.
Either dysfunction or downregulation of CLIC1 can partially decrease the antineoplastic effects of metformin.
The expression of CLIC1 might be closely related to the carcinogenesis, clinical biological behaviors, and prognosis of pancreatic ductal adenocarcinomas.
Extracellular vesicle-mediated transfer of CLIC1 protein is a novel mechanism for the regulation of glioblastoma growth.
Results indicate that CLIC1 is an important contributor to tumor invasion, metastasis, and angiogenesis.
CLIC1 acts as a putative oncogene (show RAB1A Antibodies) in pancreatic cancer.
Results indicate CLICs (CLIC1, CLIC4 (show CLIC4 Antibodies) and CLIC5 (show CLIC5 Antibodies))-dependent chloride efflux as an essential and proximal upstream event for NLRP3 (show NLRP3 Antibodies) activation.
We conclude that the role of CLIC1 in macrophage superoxide production is to support redistribution of NADPH oxidase (show NOX1 Antibodies) to the plasma membrane, and not through major effects on ERM (show ETV5 Antibodies) cytoskeleton or by acting as a plasma membrane chloride channel (show CLCA1 Antibodies).
Data, including data from studies in primary cells from knockout mice, suggest Clic1 and Clic4 (show CLIC4 Antibodies) participate in signaling interleukin 1beta secretion and in activation of Nlrp3 (show NLRP3 Antibodies) inflammasomes; in LPS (show TLR4 Antibodies) macrophage activation, Clic1 and Clic4 (show CLIC4 Antibodies) are translocated to nucleus/cell membranes. (Clic1 = chloride intracellular channel 1; Clic4 (show CLIC4 Antibodies) = chloride intracellular channel 4 (show CLIC4 Antibodies), mitochondrial; Nlrp3 (show NLRP3 Antibodies) = NLR family pyrin domain containing 3 (show NLRP3 Antibodies))
This study demonstrates for the first time that CLIC1 is overexpressed during AS development both in vitro and in vivo and can regulate the accumulation of inflammatory cytokines and production of oxidative stress.
Clic1 have a role in migration and invasion in hepatocarcinoma maybe via modulating the expression of Annexin A7 (show ANXA7 Antibodies) and Gelsolin (show GSN Antibodies).
These data all point to an important role for CLIC1 in regulating macrophage function through its ion channel activity.
The down-regulation of CLIC1 enhanced proliferative activity.
CLIC1 may play an important role in tumor metastasis.
CLIC1 is essential for the proliferation and invasion of hepatocellular carcinoma cells.
Chloride channels are a diverse group of proteins that regulate fundamental cellular processes including stabilization of cell membrane potential, transepithelial transport, maintenance of intracellular pH, and regulation of cell volume. Chloride intracellular channel 1 is a member of the p64 family\; the protein localizes principally to the cell nucleus and exhibits both nuclear and plasma membrane chloride ion channel activity.
chloride intracellular channel 1
, RNCC protein
, chloride channel ABP
, chloride intracellular channel protein 1
, nuclear chloride ion channel 27
, nuclear chloride ion channel protein
, regulatory nuclear chloride ion channel protein