MAP Kinase Signaling
Phospho-SAPK/JNK (Thr183/Tyr185) Blocking Peptide
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| CSTコード |
包装 |
希望納入価格 (円) |
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| #1215S | 100 μg | 16,000 | |
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SAPK, JNK抗体製品一覧
| 使用目的 | |
| Phospho-SAPK/JNK (Thr183/Tyr185) Antibody (#9251) の反応をブロックし、抗体の反応特異性を確認するために使用 |
IHC-P (paraffin)

Immunohistochemical analysis of paraffin-embedded human lung carcinoma, using Phospho-SAPK/JNK (Thr183/Tyr185) Antibody #9251 in the presence of control peptide (left) or Phospho-SAPK/JNK (Thr183/Tyr185) Blocking Peptide (right).
The stress-activated protein kinase/Jun-amino-terminal kinase SAPK/JNK is potently and preferentially activated by a variety of environmental stresses including UV and gamma radiation, ceramides, inflammatory cytokines, and in some instances, by growth factors and GPCR agonists (1-6). As with the other MAPKs, the core signaling unit is composed of a MAPKKK, typically MEKK1-MEKK4, or by one of the mixed lineage kinases (MLKs), which phosphorylate and activate MKK4/7. Upon activation, MKKs phosphorylate and activate the SAPK/JNK kinase (2). Stress signals are delivered to this cascade by small GTPases of the Rho family (Rac, Rho, cdc42) (3). Both Rac1 and cdc42 mediate the stimulation of MEKKs and MLKs (3). Alternatively, MKK4/7 can be activated in a GTPase-independent mechanism via stimulation of a germinal center kinase (GCK) family member (4). There are three SAPK/JNK genes each of which undergoes alternative splicing resulting in numerous isoforms (3). SAPK/JNK, when active as a dimer, can translocate to the nucleus and regulate transcription through its effects on c-Jun, ATF-2, and other transcription factors (3,5).
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Davis, R.J. (1999) Biochem Soc Symp 64, 1-12.
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Kyriakis, J.M. and Avruch, J. (2001) Physiol Rev 81, 807-69.
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Leppä, S. and Bohmann, D. (1999) Oncogene 18, 6158-62.
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Whitmarsh, A.J. and Davis, R.J. (1998) Trends Biochem Sci 23, 481-5.