Increased Insulin Sensitivity and Hypoinsulinemia in APS Knockout Mice

Minami, Asako; Iseki, Masanori; Kishi, Kazuhiro; Wang, Miao; Ogura, Makoto; Furukawa, Noboru; Hayashi, Sanae; Yamada, Mizuki; Obata, Toshiyuki; Takeshita, Yukari; Nakaya, Yutaka; Bando, Yoshimi; Izumi, Kiyotaka; Moodie, Shonna A.; Kajiura, Fumiko; Matsumoto, Machiko; Takatsu, Kiyoshi; Takaki, Satoshi; Ebina, Yasuhiko

doi:10.2337/diabetes.52.11.2657

Cited by 86 publications

(60 citation statements)

References 54 publications

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“…However, the siRNAmediated ablation of Cbl, CAP and CrkII do not have any significant effect on insulin-stimulated glucose uptake or GLUT4 translocation , Zhou et al 2004. Furthermore, while the generation of Cbl knockout mice does not result in a significant difference in insulin sensitivity (Molero et al 2004), APS knockout mice show enhanced insulin sensitivity and hypoinsulinaemia (Minami et al 2003). Finally, studies performed in muscle cells indicate that TC10 signalling may not be required for cortical actin rearrangements as has been shown in adipocytes ( JeBailey et al 2004).…”

Section: Early Signalling Events At the Plasma Membranementioning

confidence: 94%

The molecular basis of insulin-stimulated glucose uptake: signalling, trafficking and potential drug targets

Leney¹,

Tavaré²

2009

Journal of Endocrinology

132

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The search for the underlying mechanism through which insulin regulates glucose uptake into peripheral tissues has unveiled a highly intricate network of molecules that function in concert to elicit the redistribution or 'translocation' of the glucose transporter isoform GLUT4 from intracellular membranes to the cell surface. Following recent technological advances within this field, this review aims to bring together the key molecular players that are thought to be involved in GLUT4 translocation and will attempt to address the spatial relationship between the signalling and trafficking components of this event. We will also explore the degree to which components of the insulin signalling and GLUT4 trafficking machinery may serve as potential targets for the development of orally available insulin mimics for the treatment of diabetes mellitus.

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Section: Early Signalling Events At the Plasma Membranementioning

confidence: 94%

The molecular basis of insulin-stimulated glucose uptake: signalling, trafficking and potential drug targets

Leney¹,

Tavaré²

2009

Journal of Endocrinology

132

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“…The TC10␣ isoform is highly expressed in muscle and fat and was activated by insulin in most studies (50,53,54). Mediators of insulin signaling to TC10␣ remain uncertain; in particular, disruption of the proposed signaling proteins APS and c-Cbl did not impair, but actually enhanced, insulin action (49,(55)(56)(57)(58)(59). Other proteins may mediate upstream signaling (60).…”

Section: Discussionmentioning

confidence: 99%

Enhanced Fasting Glucose Turnover in Mice with Disrupted Action of TUG Protein in Skeletal Muscle

Löffler¹,

Birkenfeld²,

Philbrick³

et al. 2013

Journal of Biological Chemistry

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Background: Insulin stimulates endoproteolytic cleavage of TUG proteins to promote glucose uptake in cultured adipocytes, but the role of this pathway in muscle is uncharacterized. Results: Transgenic mice with constitutive and unregulated TUG cleavage in muscle had increased whole-body and musclespecific glucose uptake during fasting. Conclusion: Insulin acts through TUG to control glucose uptake in muscle. Significance: Understanding insulin action will elucidate diabetes pathogenesis.

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“…12 Mice deficient for members of this family have demonstrated the positive (SH2-B) and negative (Lnk and APS) role of these adaptors in growth factor, cytokine, and antigen-receptor signaling. [13][14][15][16][17][18] In particular, Lnk nullizygous mice show mainly a profound perturbation in hematopoiesis. These animals exhibit splenomegaly together with fibrosis, expansion of hematopoietic stem cells (HSCs), and myeloid and B lymphoid progenitors.…”

Section: Introductionmentioning

confidence: 99%

Lnk adaptor protein down-regulates specific Kit-induced signaling pathways in primary mast cells

Simon

Dondi

Chaix

et al. 2008

Blood

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IntroductionMast cells are multifunctional hematopoietic cells, important for both innate and specific immunity. 1 Immature mast cells leave the bone marrow to migrate to target tissues, mostly mucosal and connective tissues, where they undergo terminal differentiation and perform their biologic functions. 2 Stem cell factor (SCF) and its receptor Kit are essential for mast cell development in vivo, as shown by the phenotype of mice with null mutations in the Kit (White Spotting or W) or SCF (Steel or Sl) loci. Indeed, these mice lack tissue mast cells and also exhibit defects in hematopoiesis, pigmentation, and reproduction. 3 In bone marrow mast cells (BMMCs), activation of Kit, a type III receptor tyrosine kinase (RTK), stimulates cellular responses such as proliferation, survival, differentiation, chemotaxis, cell adhesion, and degranulation. 4 Upon SCF binding, the Kit receptor dimerizes, autophosphorylates, and subsequently transphosphorylates specific tyrosines (Y). The resulting phosphotyrosine (pY) residues serve as docking sites for Src homology 2 (SH2) domain-containing proteins, which control intracellular signaling pathways such as all 3 mitogen-activated protein kinases (MAPKs; ERK, p38, and c-jun N-terminal kinase [JNK]), phosphatidylinositol 3-kinase (PI-3K), and Janus kinases (JAK)/signal transducers and activators of transcription (STAT) pathways. 4,5 Recruitment of particular targets is mediated by the ability of SH2 domains to recognize specific pY-containing motifs on the activated receptor. Analyses of individual docking sites on Kit have provided valuable information about the activation of pathways emanating from this receptor. 6 Juxtamembrane Y567 and Y569 are critical recruitment sites for different regulatory signaling molecules. These include activators such as Src family kinases (Fyn and Lyn), Shp-2 phosphatase and Shc adaptor protein, or negative modulators such as Shp-1 phosphatase, Csk-homology kinase (Chk), suppressors of cytokine signaling (SOCS) proteins, and APS adaptor protein. 5,7,8 Mutational and "knock-in" studies on Kit Y567/Y569 have revealed their important role in cell development, proliferation, survival, and migration. 6,9-11 However, the biologic significance of these interactions is still poorly understood.Lnk is a member of the adaptor protein family that includes APS and SH2-B. All 3 members share common protein-protein interaction domains and motifs: a dimerization domain at the aminoterminus, a pleckstrin homology (PH) domain, an SH2 domain, and a conserved tyrosine near the carboxy-terminus. 12 Mice deficient for members of this family have demonstrated the positive (SH2-B) and negative (Lnk and APS) role of these adaptors in growth factor, cytokine, and antigen-receptor signaling. [13][14][15][16][17][18] In particular, Lnk nullizygous mice show mainly a profound perturbation in hematopoiesis. These animals exhibit splenomegaly together with fibrosis, expansion of hematopoietic stem cells (HSCs), and myeloid and B lymphoid progenitors. [17][18][19] Recent ana...

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Increased Insulin Sensitivity and Hypoinsulinemia in APS Knockout Mice

Cited by 86 publications

References 54 publications

The molecular basis of insulin-stimulated glucose uptake: signalling, trafficking and potential drug targets

The molecular basis of insulin-stimulated glucose uptake: signalling, trafficking and potential drug targets

Enhanced Fasting Glucose Turnover in Mice with Disrupted Action of TUG Protein in Skeletal Muscle

Lnk adaptor protein down-regulates specific Kit-induced signaling pathways in primary mast cells

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