Revision 8

#77533Store at -20C

1 Kit

(9 x 20 microliters)

Cell Signaling Technology

Orders: 877-616-CELL (2355) [email protected]

Support: 877-678-TECH (8324)

Web: [email protected] cellsignal.com

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For Research Use Only. Not for Use in Diagnostic Procedures.
Product Includes Product # Quantity Mol. Wt Isotype/Source
TREM2 (D8I4C) Rabbit mAb 91068 20 µl 28 kDa Rabbit IgG
DAP12 (D7G1X) Rabbit mAb 12492 20 µl 10, 12 kDa Rabbit IgG
Syk (D3Z1E) XP® Rabbit mAb 13198 20 µl 72 kDa Rabbit IgG
Phospho-Syk (Tyr525/526) (C87C1) Rabbit mAb 2710 20 µl 72 kDa Rabbit IgG
Phospho-Zap-70 (Tyr319)/Syk (Tyr352) (65E4) Rabbit mAb 2717 20 µl 70, 72 kDa Rabbit IgG
PLCγ1 (D9H10) XP® Rabbit mAb 5690 20 µl 150 kDa Rabbit IgG
Phospho-PLCγ1 (Tyr783) (D6M9S) Rabbit mAb 14008 20 µl 155 kDa Rabbit IgG
PLCγ2 (E5U4T) Rabbit mAb 55512 20 µl 150 kDa Rabbit IgG
Phospho-PLCγ2 (Tyr759) (E9E9Y) Rabbit mAb 50535 20 µl 150 kDa Rabbit IgG
Anti-rabbit IgG, HRP-linked Antibody 7074 100 µl Goat 

Please visit cellsignal.com for individual component applications, species cross-reactivity, dilutions, protocols, and additional product information.

Storage

All antibodies are supplied in 10 mM sodium HEPES (pH 7.5), 150 mM NaCl, 100 µg/ml BSA, 50% glycerol and less than 0.02% sodium azide. Store at –20°C. Do not aliquot the antibody.

Background

Microglia cells are resident macrophages of the brain that survey the brain environment and dynamically respond to maintain brain homeostasis. Microglial responses include phagocytosis of cellular debris, restricting sites injury or pathology, and/or releasing inflammatory signals to initiate an immune response. Such responses are important during normal development and during diseased states (1).Recently, the role of microglia in neurodegenerative disease pathology, particularly Alzheimer’s disease (AD), has been of intense investigation. Much of this work is driven by human genetic data that links microglia-enriched genes with AD progression (2). The triggering receptor expressed on myeloid cells 2 (TREM2) protein is an innate immune receptor that is expressed on the cell surface of microglia (3). TREM2 plays a role in innate immunity, and a rare functional variant (R47H) of the TREM2 gene is associated with the late-onset risk of AD (3,4). How TREM2 contributes to disease function is currently an active area of research (4,5), but might drive a number of microglial cellular functions ranging from microgliosis, phagocytosis, and cytokine release via a variety of signaling cascades triggered by TREM2.The TREM2 receptor is a single-pass type I membrane glycoprotein that consists of an extracellular immunoglobulin-like domain, a transmembrane domain, and a cytoplasmic tail. Ligands for TREM2 include phospholipids, apolipoproteins, and lipoproteins. Upon activation, TREM2 interacts with the tyrosine kinase-binding protein DNAX-activating protein 12 (DAP12, TYROBP) to form a receptor-signaling complex (6). Ligand binding by DAP12-associated receptors, including TREM2, results in phosphorylation of tyrosine residues within the DAP12 immunoreceptor tyrosine-based activation motif (ITAM) by Src family kinases; ITAM phosphorylation leads to activation of spleen tyrosine kinase (Syk) and downstream signaling cascades (7). Tyr525 and Tyr526 are located in the activation loop of the Syk kinase domain and phosphorylation at these residues (equivalent to Tyr519/520 of mouse Syk) is essential for Syk function (8). Syk phosphorylation is also a readout for β-amyloid triggered TREM2 activity (9). Phosphoinositide-specific phospholipase C γ 1/2 (PLCγ1/2) is reported to be down stream of Syk (10). Tyr352 of Syk is involved in the association of PLCγ1 (11); Syk-mediated phosphorylation PLCγ1 at Tyr783 activates PLCγ1 enzymatic activity (12). Interestingly, mutations in the microglia-enriched PLCγ2 gene are associated with AD (13,14,15).

  1. Kierdorf, K. and Prinz, M. (2017) J Clin Invest 127, 3201-9.
  2. McQuade, A. and Blurton-Jones, M. (2019) J Mol Biol.
  3. Colonna, M. (2003) Nat Rev Immunol 3, 445-53.
  4. Yeh, F.L. et al. (2017) Trends Mol Med 23, 512-33.
  5. Ulland, T.K. and Colonna, M. (2018) Nat Rev Neurol 14, 667-75.
  6. Peng, Q. et al. (2010) Sci Signal 3, ra38.
  7. Lanier, L.L. et al. (1998) Nature 391, 703-7.
  8. Zhang, J. et al. (2000) J Biol Chem 275, 35442-7.
  9. Zhao, Y. et al. (2018) Neuron 97, 1023-1031.e7.
  10. Kusuyama, J. et al. (2018) J Cell Physiol 233, 2549-59.
  11. Law, C.L. et al. (1996) Mol Cell Biol 16, 1305-15.
  12. Wang, Z. et al. (1998) Mol Cell Biol 18, 590-7.
  13. Magno, L. et al. (2019) Alzheimers Res Ther 11, 16.
  14. Sims, R. et al. (2017) Nat Genet 49, 1373-84.
  15. Dalmasso, M.C. et al. (2019) Transl Psychiatry 9, 55.

Background References

    Trademarks and Patents

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