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. 2020 Dec 18;32(1):9–31. doi: 10.1681/ASN.2020050697

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Figure 2. — SPHKs are activated by a variety of factors, including cytokines, hormones, growth factors, small GTPases, tyrosine kinase receptors, FcεRI, and others. Following their activation, SPHKs promote (green arrows) or inhibit (red arrow) pathways that regulate cell health and death. Most factors activate SPHK1 (yellow arrows), whereas only a few are known to activate SPHK2 (gray arrows) (reviewed in ^247–249). Bcl-xL,⁴⁰ B cell lymphoma extra large; bFGF,²³⁶ fibroblast growth factor; Ca²⁺, calcium; EGF^56,237; Est, estrogen²³⁷; FcεRI⁴¹, high-affinity IgE receptor; His, histamine²³⁸; IGF-1, insulin-like growth factor; IL-1β²³⁹, interleukin 1 beta; NGF,²⁴⁰ nerve growth factor; PA, phosphatidic acid; PDGF²⁴¹, platelet-derived growth factor; phorbol esters TMA²³⁸ and PMA²⁴²; TGF-β²⁴³, transforming growth factor beta; TKR,²³⁷ tyrosine kinase receptor; TNF²⁴⁴, tumor necrosis factor alpha; TRAF2,⁴² TNF-α receptor–associated factor 2; VEGF²⁴⁵, vascular endothelial growth factor; VitD3²⁴⁶, vitamin D3.