@article {Lee:December 2005:0929-8673:2979, author = "Lee, Matthew R.", author = "Dominguez, Celia", title = "MAP Kinase p38Inhibitors: Clinical Results and an Intimate Look at Their Interactions with p38alpha Protein", journal = "Current Medicinal Chemistry", volume = "12", year = "December 2005", abstract = "Mitogen-activated protein kinase p38 is a serine/threonine kinase originally isolated from lipopolysaccharide (LPS) stimulated monocytes. There are four isoforms p38 agr

, p38

, p38

, and p38

. The most thoroughly studied isoform is p38 agr

, whose activation has been observed in many hematopoietic and nonhematopoietic cell types upon appropriate stimuli. Subsequently, p38 agr

kinase has been shown to be involved in the biosynthesis of TNF agr

and IL-1

at the translational and transcriptional level. MAP kinase p38agr; represents a point of convergence for multiple signaling processes that are activated in inflammation and thus a key potential target for the modulation of cytokine production. The discovery and publication of p38 agr

and the pyridinyl-imidazole inhibitor initiated a huge effort by many companies to develop p38 agr

inhibitors as potential treatment for inflammatory diseases. Herein we provide a brief overview of recent reported clinical results for AMG 548, BIRB 796, VX 702, SCIO 469, and SCIO 323. However, our focus will be on the binding modes of these inhibitors and other p38 inhibitors in the recent literature.", pages = "2979-2994(16)", url = "http://www.ingentaconnect.com/content/ben/cmc/2005/00000012/00000025/art00007" doi = "doi:10.2174/092986705774462914" }