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W67061917 abstract "Mitogen-activated protein kinase (MAPK) cascades control cell fate decisions, such as proliferation, differentiation, and apoptosis by integrating and processing intra- and extracellular cues. However, similar MAPK kinetic profiles can be associated with opposing cellular decisions depending on cell type, signal strength, and dynamics. This implies that signaling by each individual MAPK cascade has to be considered in the context of the entire MAPK network. Here, we develop a dynamic model of feedback and crosstalk for the three major MAPK cascades; extracellular signal-regulated kinase (ERK), p38 mitogen-activated protein kinase (p38), c-Jun N-terminal kinase (JNK), and also include input from protein kinase B (AKT) signaling. Focusing on the bistable activation characteristics of the JNK pathway, this model explains how pathway crosstalk harmonizes different MAPK responses resulting in pivotal cell fate decisions. We show that JNK can switch from a transient to sustained activity due to multiple positive feedback loops. Once activated, positive feedback locks JNK in a highly active state and promotes cell death. The switch is modulated by the ERK, p38, and AKT pathways. ERK activation enhances the dual specificity phosphatase (DUSP) mediated dephosphorylation of JNK and shifts the threshold of the apoptotic switch to higher inputs. Activation of p38 restores the threshold by inhibiting ERK activity via the PP1 or PP2A phosphatases. Finally, AKT activation inhibits the JNK positive feedback, thus abrogating the apoptotic switch and allowing only proliferative signaling. Our model facilitates understanding of how cancerous deregulations disturb MAPK signal processing and provides explanations for certain drug resistances. We highlight a critical role of DUSP1 and DUSP2 expression patterns in facilitating the switching of JNK activity and show how oncogene induced ERK hyperactivity prevents the normal apoptotic switch explaining the failure of certain drugs to induce apoptosis." @default.
W67061917 created "2016-06-24" @default.
W67061917 creator A5003776093 @default.
W67061917 creator A5036674933 @default.
W67061917 creator A5051465312 @default.
W67061917 creator A5077163269 @default.
W67061917 date "2012-01-01" @default.
W67061917 modified "2023-10-12" @default.
W67061917 title "Crosstalk and Signaling Switches in Mitogen-Activated Protein Kinase Cascades" @default.
W67061917 cites W1535234514 @default.
W67061917 cites W1576664335 @default.
W67061917 cites W1602618290 @default.
W67061917 cites W1965790167 @default.
W67061917 cites W1965853004 @default.
W67061917 cites W1968877074 @default.
W67061917 cites W1969268163 @default.
W67061917 cites W1969419810 @default.
W67061917 cites W1970661255 @default.
W67061917 cites W1974140472 @default.
W67061917 cites W1978486653 @default.
W67061917 cites W1984920104 @default.
W67061917 cites W1985911638 @default.
W67061917 cites W1986753065 @default.
W67061917 cites W1989041138 @default.
W67061917 cites W1990320961 @default.
W67061917 cites W1995035611 @default.
W67061917 cites W1995819749 @default.
W67061917 cites W1997706935 @default.
W67061917 cites W1999903313 @default.
W67061917 cites W2000514139 @default.
W67061917 cites W2000817203 @default.
W67061917 cites W2003060606 @default.
W67061917 cites W2006545622 @default.
W67061917 cites W2007114641 @default.
W67061917 cites W2009520959 @default.
W67061917 cites W2018697124 @default.
W67061917 cites W2019307738 @default.
W67061917 cites W2019686202 @default.
W67061917 cites W2020976545 @default.
W67061917 cites W2024468216 @default.
W67061917 cites W2024944632 @default.
W67061917 cites W2026894807 @default.
W67061917 cites W2028083348 @default.
W67061917 cites W2028415754 @default.
W67061917 cites W2034188706 @default.
W67061917 cites W2035967893 @default.
W67061917 cites W2037250704 @default.
W67061917 cites W2038715496 @default.
W67061917 cites W2038959355 @default.
W67061917 cites W2042921323 @default.
W67061917 cites W2047365291 @default.
W67061917 cites W2048781554 @default.
W67061917 cites W2050568471 @default.
W67061917 cites W2052071148 @default.
W67061917 cites W2053024011 @default.
W67061917 cites W2054139370 @default.
W67061917 cites W2056929243 @default.
W67061917 cites W2062289724 @default.
W67061917 cites W2066893159 @default.
W67061917 cites W2068652881 @default.
W67061917 cites W2070477528 @default.
W67061917 cites W2070658593 @default.
W67061917 cites W2071141381 @default.
W67061917 cites W2071523020 @default.
W67061917 cites W2071900417 @default.
W67061917 cites W2072027286 @default.
W67061917 cites W2072515105 @default.
W67061917 cites W2073106992 @default.
W67061917 cites W2074267409 @default.
W67061917 cites W2080352303 @default.
W67061917 cites W2081633731 @default.
W67061917 cites W2084472730 @default.
W67061917 cites W2086936470 @default.
W67061917 cites W2092363432 @default.
W67061917 cites W2095169768 @default.
W67061917 cites W2095852754 @default.
W67061917 cites W2100212868 @default.
W67061917 cites W2107034836 @default.
W67061917 cites W2107149701 @default.
W67061917 cites W2107589168 @default.
W67061917 cites W2109444989 @default.
W67061917 cites W2114845119 @default.
W67061917 cites W2116357670 @default.
W67061917 cites W2117209575 @default.
W67061917 cites W2117692326 @default.
W67061917 cites W2123333705 @default.
W67061917 cites W2123619341 @default.
W67061917 cites W2123646075 @default.
W67061917 cites W2124911220 @default.
W67061917 cites W2126841263 @default.
W67061917 cites W2130027917 @default.
W67061917 cites W2132014973 @default.
W67061917 cites W2135086805 @default.
W67061917 cites W2136693393 @default.
W67061917 cites W2138468336 @default.
W67061917 cites W2143734893 @default.
W67061917 cites W2147985467 @default.
W67061917 cites W2151407889 @default.
W67061917 cites W2152585118 @default.
W67061917 cites W2153100796 @default.