Regulation and function of TPL-2, an IκB kinase-regulated MAP kinase kinase kinase

T Gantke, S Sriskantharajah, SC Ley - Cell research, 2011 - nature.com
T Gantke, S Sriskantharajah, SC Ley
Cell research, 2011nature.com
The IκB kinase (IKK) complex plays a well-documented role in innate and adaptive
immunity. This function has been widely attributed to its role as the central activator of the NF-
κB family of transcription factors. However, another important consequence of IKK activation
is the regulation of TPL-2, a MEK kinase that is required for activation of ERK-1/2 MAP
kinases in myeloid cells following Toll-like receptor and TNF receptor stimulation. In
unstimulated cells, TPL-2 is stoichiometrically complexed with the NF-κB inhibitory protein …
Abstract
The IκB kinase (IKK) complex plays a well-documented role in innate and adaptive immunity. This function has been widely attributed to its role as the central activator of the NF-κB family of transcription factors. However, another important consequence of IKK activation is the regulation of TPL-2, a MEK kinase that is required for activation of ERK-1/2 MAP kinases in myeloid cells following Toll-like receptor and TNF receptor stimulation. In unstimulated cells, TPL-2 is stoichiometrically complexed with the NF-κB inhibitory protein NF-κB1 p105, which blocks TPL-2 access to its substrate MEK, and the ubiquitin-binding protein ABIN-2 (A20-binding inhibitor of NF-κB 2), both of which are required to maintain TPL-2 protein stability. Following agonist stimulation, the IKK complex phosphorylates p105, triggering its K48-linked ubiquitination and degradation by the proteasome. This releases TPL-2 from p105-mediated inhibition, facilitating activation of MEK, in addition to modulating NF-κB activation by liberating associated Rel subunits for translocation into the nucleus. IKK-induced proteolysis of p105, therefore, can directly regulate both NF-κB and ERK MAP kinase activation via NF-κB1 p105. TPL-2 is critical for production of the proinflammatory cytokine TNF during inflammatory responses. Consequently, there has been considerable interest in the pharmaceutical industry to develop selective TPL-2 inhibitors as drugs for the treatment of TNF-dependent inflammatory diseases, such as rheumatoid arthritis and inflammatory bowel disease. This review summarizes our current understanding of the regulation of TPL-2 signaling function, and also the complex positive and negative roles of TPL-2 in immune and inflammatory responses.
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