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Signaling molecules as therapeutic targets in allergic diseases

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Presentation on theme: "Signaling molecules as therapeutic targets in allergic diseases"— Presentation transcript:

1 Signaling molecules as therapeutic targets in allergic diseases
Magdalena M. Gorska, MD, Rafeul Alam, MD, PhD  Journal of Allergy and Clinical Immunology  Volume 112, Issue 2, Pages (August 2003) DOI: /mai Copyright © 2003 Mosby, Inc. Terms and Conditions

2 Fig. 1 Homeostatic regulation of signaling mechanism. Two different regulatory mechanisms are shown. The left panel is an example of negative feedback mechanism, whereas the right panel illustrates a counter-regulatory mechanism. Journal of Allergy and Clinical Immunology  , DOI: ( /mai ) Copyright © 2003 Mosby, Inc. Terms and Conditions

3 Fig. 2 Specificity of signaling molecules. Specificity is usually determined by the position of the signaling molecule in the hierarchy of the signaling cascade. Receptor-proximal molecules are usually specific for the receptor family, whereas the effector function-associated molecules are relatively specific for the function. The intermediate signaling molecules are usually nonspecific. A right combination (quality and quantity) of nonspecific signals elicits a specific cellular function. Journal of Allergy and Clinical Immunology  , DOI: ( /mai ) Copyright © 2003 Mosby, Inc. Terms and Conditions

4 Fig. 3 Examples of master signaling regulators. The left panel shows a master regulatory molecule that is receptor-associated and transduces signals through multiple downstream pathways. The right panel shows an example of a master regulatory molecule, which is not receptor-associated and functions downstream of many receptors. Signals from multiple surface receptors converge on this signaling molecule, which then transduces signals through multiple pathways. Journal of Allergy and Clinical Immunology  , DOI: ( /mai ) Copyright © 2003 Mosby, Inc. Terms and Conditions

5 Fig. 4 A schematic model of signal transduction from the receptor. Binding of the ligand to the receptor activates receptor-associated signaling molecules, eg, G proteins or tyrosine or serine/threonine protein kinases. The foregoing signaling molecules might activate cytosolic tyrosine kinases, eg, Syk, which leads to the recruitment of adapter protein. Some receptor-associated tyrosine kinases (eg, JAKs) directly activate transcriptional factors of the STAT family. Many phosphatases (eg, SHP-1) downregulate signaling processes by inactivating kinases at this stage. Adapter proteins, in turn, recruit downstream molecules such as lipid metabolism enzymes or small G proteins. The activation of these molecules results in the stimulation of cytosolic serine-threonine kinase cascade (eg, MAPKs) or calcium signaling. These pathways lead to the activation of various transcriptional factors. Journal of Allergy and Clinical Immunology  , DOI: ( /mai ) Copyright © 2003 Mosby, Inc. Terms and Conditions

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