The Molecular Scaffold Kinase Suppressor of Ras 1 (KSR1) Regulates Adipogenesis

Self Cite

In primary mouse embryo fibroblasts (MEFs), oncogenic Ras induces growth arrest via؊/؊ MEFs are completely resistant to Ras V12 -induced transformation. These data show that escape from senescence is not necessarily a precursor for oncogenic transformation. Furthermore, these data indicate that KSR1 is a member of a unique class of proteins whose deletion blocks both senescence and transformation.

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

The Molecular Scaffold Kinase Suppressor of Ras 1 Is a Modifier of Ras^V12-Induced and Replicative Senescence

Kortum

Johnson

Costanzo

et al. 2006

Self Cite

“…KSR2 Ϫ/Ϫ mice become spontaneously obese and possess cellular defects in both glucose uptake and fatty acid oxidation (13). KSR1 Ϫ/Ϫ mice have enlarged adipocytes and in vitro defects in adipogenesis and lipid accumulation (37). Because KSR proteins regulate both metabolism and tumorigenesis, we designed a study to determine how KSR1 impacts metabolism driven by oncogenic Ras.…”

mentioning

confidence: 99%

Kinase Suppressor of Ras 1 (KSR1) Regulates PGC1α and Estrogen-Related Receptor α To Promote Oncogenic Ras-Dependent Anchorage-Independent Growth

Fisher

Das

Kortum

et al. 2011

Self Cite

Kinase suppressor of ras 1 (KSR1) is a molecular scaffold of the Raf/MEK/extracellular signal-regulated kinase (ERK) cascade that enhances oncogenic Ras signaling. Here we show KSR1-dependent, but ERKindependent, regulation of metabolic capacity is mediated through the expression of peroxisome proliferatoractivated receptor gamma coactivator 1␣ (PGC1␣) and estrogen-related receptor ␣ (ERR␣). This KSR1-regulated pathway is essential for the transformation of cells by oncogenic Ras. In mouse embryo fibroblasts (MEFs) expressing H-Ras V12 , ectopic PGC1␣ was sufficient to rescue ERR␣ expression, metabolic capacity, and anchorage-independent growth in the absence of KSR1. The ability of PGC1␣ to promote anchorageindependent growth required interaction with ERR␣, and treatment with an inhibitor of ERR␣ impeded anchorage-independent growth. In contrast to PGC1␣, the expression of constitutively active ERR␣ (CA-ERR␣) was sufficient to enhance metabolic capacity but not anchorage-independent growth in the absence of KSR1. These data reveal KSR1-dependent control of PGC1␣-and ERR␣-dependent pathways that are necessary and sufficient for signaling by oncogenic H-Ras V12 to regulate metabolism and anchorage-independent growth, providing novel targets for therapeutic intervention.

“…In C. elegans, KSR2 is required for Ras-mediated signaling during germ line meiotic progression and functions redundantly with KSR1 during development of the excretory system, hermaphrodite vulva, and male spicules (46). Subsequent studies in mammalian systems showed that KSR1 and KSR2 interact with Raf, MEK, and ERK to coordinate the intensity and duration of ERK signaling (3,9,10,29,31,54,62,63). Manipulation of KSR1 in mouse embryo fibroblasts (MEFs) revealed the intricate regulation of ERK signaling to enhance the oncogenic potential of Ras, adipogenic differentiation, and replicative senescence (29-31).…”

mentioning

confidence: 99%

Kinase Suppressor of Ras 2 (KSR2) Regulates Tumor Cell Transformation via AMPK

Fernandez

Henry

Lewis

2012

Self Cite

Kinase suppressor of Ras 1 (KSR1) and KSR2 are scaffolds that promote extracellular signal-regulated kinase (ERK) signaling but have dramatically different physiological functions. KSR2 ؊/؊ mice show marked deficits in energy expenditure that cause obesity. In contrast, KSR1 disruption has inconsequential effects on development but dramatically suppresses tumor formation by activated Ras. We examined the role of KSR2 in the generation and maintenance of the transformed phenotype in KSR1 (28,55,57). In C. elegans, KSR2 is required for Ras-mediated signaling during germ line meiotic progression and functions redundantly with KSR1 during development of the excretory system, hermaphrodite vulva, and male spicules (46). Subsequent studies in mammalian systems showed that KSR1 and KSR2 interact with Raf, MEK, and ERK to coordinate the intensity and duration of ERK signaling (3,9,10,29,31,54,62,63). Manipulation of KSR1 in mouse embryo fibroblasts (MEFs) revealed the intricate regulation of ERK signaling to enhance the oncogenic potential of Ras, adipogenic differentiation, and replicative senescence (29-31). Studies with mammalian KSR2 showed that it uniquely coordinates calcium-mediated Rasto-ERK signaling (10). KSR scaffolds have also been implicated in regulating cellular metabolism, as both KSR1 Ϫ/Ϫ and KSR2 Ϫ/Ϫ mice exhibit metabolic defects. KSR1 Ϫ/Ϫ mice have hypertrophic adipocytes (29). Disruption of KSR2 in mice led to reduced expression of genes responsible for oxidative phosphorylation (OXPHOS) and deregulated 5= AMP-activated protein kinase (AMPK)-mediated processes, which led to spontaneous obesity and insulin resistance. KSR2 interacts with all AMPK subunits and promotes AMPK phosphorylation in vitro and in vivo (6). KSR1 mediates the Ras-dependent upregulation of peroxisome proliferator-activated receptor ␥ coactivator 1␣ (PGC1␣) and estrogenrelated receptor ␣ (ERR␣), transcription factors that regulate mitochondrial biogenesis in MEFs, and is essential to promote anchorage-independent growth (12).AMPK is a trimeric enzyme regulating the cell energy homeostasis that is activated during nutrient deprivation due to increased intracellular AMP/ATP ratios, as the allosteric activator AMP promotes AMPK activity during energy stress (16, 51). AMP and ADP promote the binding of ␣ and ␥ subunits to protect dephosphorylation of Thr172 in the ␣ subunit (45, 61). As ATP levels increase, AMPK activity is suppressed (45, 51). Activation of AMPK promotes the activation of catabolic pathways that generate ATP and the inhibition of anabolic pathways that consume ATP. AMPK activation promotes glucose and fatty acid uptake, glycolysis, and fatty acid oxidation and enhances mitochondrial biogenesis while inhibiting fatty acid synthesis, gluconeogenesis, glycogen storage, and cholesterol biosynthesis (53).KSR1 is the most extensively characterized of the KSR scaffolds involved in the regulation of cell proliferation and tumorigenesis. T cells isolated from KSR1 Ϫ/Ϫ mice exhibited lower proliferative rates (44). Elevating...