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04-893 Sigma-AldrichAnti-JNK3/SAPK1b Antibody, clone C05T, rabbit monoclonal

Detect JNK3/SAPK1b using this Anti-JNK3/SAPK1b Antibody, clone C05T validated for use in WB.

Anti-JNK3/SAPK1b Antibody, clone C05T, rabbit monoclonal MSDS (material safety data sheet) or SDS, CoA and CoQ, dossiers, brochures and other available documents.

SDS
CoA
References

Research Category: Signaling Research Sub-Category: Kinases & Phosphatases Gene Symbol: EC 2.7.11.24, FLJ12099, FLJ33785, JNK3, JNK3A , MGC50974, OTTHUMP00000161180, OTTHUMP00000161182, OTTHUMP00000161183 , PRKM10, p493F12 , p54bSAPK UniProt Number: P49187

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Key Spec Table

Species Reactivity	Key Applications	Host	Format	Antibody Type
H, R	WB	Rb	Culture Supernatant	Monoclonal Antibody

Description
Catalogue Number	04-893
Replaces	05-893
Description	Anti-JNK3/SAPK1b Antibody, clone C05T, rabbit monoclonal
Alternate Names	JNK3 alpha protein kinase MAP kinase MAP kinase p49 3F12 Stress-activated protein kinase JNK3 c-Jun N-terminal kinase 3 c-Jun kinase 3 mitogen-activated protein kinase 10 stress activated protein kinase JNK3 stress activated protein kinase beta
Background Information	The stress-activated protein kinase 1 family is also referred to as the jun N-terminal kinase family, in light of the substrate preference of these serine/threonine kinases. The SAPK family shares 42-45% identity in the kinase domains with the MAPK family, and the SAPKs are activated by phosphorylation of a threonine and tyrosine by MKK4 and SKK4, just as the MAP kinases are phosphorylated on a threonine and tyrosine by MEK1 and MEK2. By contrast to the mitogen-activated kinases, the stress-activated kinases are only weakly activated by mitogenic stimuli, but potently activated by stress stimuli, such as inflammatory cytokines, ischemia, chemotherapeutic agents and irradiation. The JNK/SAPK1 kinases, like the other MAPK-like kinases, are thought to phosphorylate multiple substrates and regulate many processes, including proliferation (in some cell types) and apoptosis. The SAPK2/3 family is most widely referred to as the p38 family. These kinases are also activated by stresses, most notably inflammatory cytokines, irradiation, and certain toxins such as anisomycin and arsenite. The activating kinases of SAPK2/3 are SKK2/MEK3 for SAPK2a and 2b, and MKK6 for SAPK3. The targets of the SAPK2/3 family include the MAPKAP kinases 2 and 3/3pK. In addition, SKK4 is related to this family, exhibiting 60% identity, and is activated by MKK6.

References

Product Information
Format	Culture Supernatant
Control	RIPA cell lysates from A431 cells.
Presentation	Cultured supernantant in 0.05% sodium azide.
Quality Level	MQ100

Applications
Application	Detect JNK3/SAPK1b using this Anti-JNK3/SAPK1b Antibody, clone C05T validated for use in WB.
Key Applications	Western Blotting
Application Notes	Western Blot Analysis: A 1:500-1:2,000 dilution of this lot detected JNK3 in RIPA lysates from A431 cells.

Biological Information
Immunogen	GST fusion protein corresponding to full-length rat JNK3/ SAPK1b
Clone	C05T
Host	Rabbit
Specificity	Recognizes JNK3/SAPK1b. Does not cross react with JNK1 or JNK2.
Isotype	IgG
Species Reactivity	Human Rat
Antibody Type	Monoclonal Antibody
Entrez Gene Number	NM_002753.2
Entrez Gene Summary	The protein encoded by this gene is a member of the MAP kinase family. MAP kinases act as an integration point for multiple biochemical signals, and are involved in a wide variety of cellular processes such as proliferation, differentiation, transcription regulation and development. This protein is a neuronal-specific form of c-Jun N-terminal kinases (JNKs). Through its phosphorylation and nuclear localization, this kinase plays regulatory roles in the signaling pathways during neuronal apoptosis. Beta-arrestin 2, a receptor-regulated MAP kinase scaffold protein, is found to interact with, and stimulate the phosphorylation of this kinase by MAP kinase kinase 4 (MKK4). Cyclin-dependent kianse 5 can phosphorylate, and inhibit the activity of this kinase, which may be important in preventing neuronal apoptosis. Four alternatively spliced transcript variants encoding distinct isoforms have been reported. [provided by RefSeq]
Gene Symbol	EC 2.7.11.24 FLJ12099 FLJ33785 JNK3 JNK3A MGC50974 OTTHUMP00000161180 OTTHUMP00000161182 OTTHUMP00000161183 PRKM10 p493F12 p54bSAPK
UniProt Number	P49187
UniProt Summary	FUNCTION: Responds to activation by environmental stress and pro-inflammatory cytokines by phosphorylating a number of transcription factors, primarily components of AP-1 such as c-Jun and ATF2 and thus regulates AP-1 transcriptional activity. Required for stress-induced neuronal apoptosis and the pathogenesis of glutamate excitotoxicity By similarity. Catalytic activity ATP + a protein = ADP + a phosphoprotein. Cofactor Magnesium By similarity. Enzyme regulation Activated by threonine and tyrosine phosphorylation by two dual specificity kinases, MAP2K4 and MAP2K7. MAP2K7 phosphorylates MAPK10 on Thr-221 causing a conformational change and a large increase in Vmax for the enzyme. MAP2K4 then phosphorylates Tyr-223 resulting in a further increase in Vmax. Inhibited by dual specificity phosphatases, such as DUSP1. Inhibited by HDAC9 By similarity. SUBUNIT: Binds to at least four scaffolding proteins, MAPK8IP1/JIP-1, MAPK8IP2/JIP-2, MAPK8IP3/JIP-3/JSAP1 and SPAG9/MAPK8IP4/JIP-4. These proteins also bind other components of the JNK signaling pathway. Interacts with HDAC9 and MAPKBP1 By similarity. DOMAIN: The TXY motif contains the threonine and tyrosine residues whose phosphorylation activates the MAP kinases. PTM:Dually phosphorylated on Thr-221 and Tyr-223, which activates the enzyme By similarity. SIMILARITY: Belongs to the protein kinase superfamily. CMGC Ser/Thr protein kinase family. MAP kinase subfamily. Contains 1 protein kinase domain.
Molecular Weight	46-54kDa

Physicochemical Information

Dimensions

Materials Information

Toxicological Information

Safety Information according to GHS

Safety Information

Product Usage Statements
Quality Assurance	Routinely evaluated by western blot on RIPA lysates from A431 cells.
Usage Statement	Unless otherwise stated in our catalog or other company documentation accompanying the product(s), our products are intended for research use only and are not to be used for any other purpose, which includes but is not limited to, unauthorized commercial uses, in vitro diagnostic uses, ex vivo or in vivo therapeutic uses or any type of consumption or application to humans or animals.

Storage and Shipping Information
Storage Conditions	Stable for 1 year at -20°C from date of receipt.

Packaging Information
Material Size	100 µL

Transport Information

Supplemental Information

Specifications

Global Trade Item Number
Catalogue Number	GTIN
04-893	04053252515194

Documentation

Anti-JNK3/SAPK1b Antibody, clone C05T, rabbit monoclonal MSDS

Title
Safety Data Sheet (SDS)

Anti-JNK3/SAPK1b Antibody, clone C05T, rabbit monoclonal Certificates of Analysis

Title	Lot Number
Anti-JNK3/SAPK1b, clone C05T - 2424726	2424726
Anti-JNK3/SAPK1b, clone C05T - 2299154	2299154
Anti-JNK3/SAPK1b, clone C05T - 2491121	2491121
Anti-JNK3/SAPK1b, clone C05T - 3157580	3157580
Anti-JNK3/SAPK1b, clone C05T - 3485510	3485510
Anti-JNK3/SAPK1b, clone C05T - DAM1561708	DAM1561708
Anti-JNK3/SAPK1b, clone C05T -2608740	2608740
Anti-JNK3/SAPK1b, clone C05T -2768160	2768160
Anti-JNK3/SAPK1b, clone C05T Monoclonal Antibody	2899948

References

Reference overview	Pub Med ID
Small peptide inhibitor of JNK3 protects dopaminergic neurons from MPTP induced injury via inhibiting the ASK1-JNK3 signaling pathway. Pan, J; Li, H; Zhang, B; Xiong, R; Zhang, Y; Kang, WY; Chen, W; Zhao, ZB; Chen, SD PloS one 10 e0119204 2015 Show Abstract The ASK1-JNK3 signaling pathway plays a pivotal role in the pathogenesis of Parkinson's disease (PD). The specific binding of β-arrestin2 to JNK3 is essential for activation of the ASK1-JNK3 cascade, representing a potential therapeutic target for preventing dopaminergic neuronal death in PD. The aim of this study was to identify a novel strategy for the prevention of dopaminergic neuronal death in PD.Based on the specific binding of β-arrestin2 to JNK3, a 21-amino-acid fusion peptide, termed JNK3-N-Tat, was synthesized. We evaluated the ability of this peptide to inhibit the binding of β-arrestin2 to its target domain in JNK3 in vitro and in vivo.The JNK3-N-Tat peptide inhibited activation of the ASK1-JNK3 cascade by disrupting the interaction between β-arrestin2 and JNK3. JNK3-N-Tat exerted beneficial effects through pathways downstream of JNK3 and improved mitochondrial function, resulting in attenuated MPP+/MPTP-induced damage. JNK3-N-Tat protected mesencephalic dopaminergic neurons against MPTP-induced toxicity.JNK3-N-Tat, a JNK3-inhibitory peptide, protects dopaminergic neurons against MPP+/MPTP-induced injury by inhibiting the ASK1-JNK3 signaling pathway.	25856433
SUMOylation of the kainate receptor subunit GluK2 contributes to the activation of the MLK3-JNK3 pathway following kainate stimulation. Qiu-Ju Zhu,Yan Xu,Cai-Ping Du,Xiao-Yu Hou FEBS letters 586 2011 Show Abstract Protein SUMOylation has been implicated in the pathogenesis of ischemic stroke. However, the underlying mechanisms remain unclear. Here, we found that global brain ischemia evokes a sustained elevation of GluK2 SUMOylation in the rat hippocampal CA1 region. Over-expression of wild-type GluK2, but not SUMOylation-deficient mutant, significantly increased the activity of MLK3 and JNK3 after kainate stimulation. SUMOylation deficiency attenuated the kainate-stimulated interaction between MLK3 and GluK2. In addition, inhibition of kainate-evoked GluK2 endocytosis decreased the activation of MLK3-JNK3 signaling and the binding of MLK3-GluK2 in cultured cortical neurons. These results suggest that the internalization of GluK2 following SUMO modification promotes its binding with MLK3, thereby activating the MLK3-JNK3 pathway, which may be responsible for ischemic neuronal cell death.	22483987

Reference overview

Pub Med ID

Small peptide inhibitor of JNK3 protects dopaminergic neurons from MPTP induced injury via inhibiting the ASK1-JNK3 signaling pathway.
Pan, J; Li, H; Zhang, B; Xiong, R; Zhang, Y; Kang, WY; Chen, W; Zhao, ZB; Chen, SD
PloS one 10 e0119204 2015

Show Abstract

25856433

SUMOylation of the kainate receptor subunit GluK2 contributes to the activation of the MLK3-JNK3 pathway following kainate stimulation.
Qiu-Ju Zhu,Yan Xu,Cai-Ping Du,Xiao-Yu Hou
FEBS letters 586 2011

Show Abstract

22483987

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