Fibroblast growth factor 2 endocytosis in endothelial cells proceed via syndecan-4-dependent activation of Rac1 and a Cdc42-dependent macropinocytic pathway

Tkachenko, Eugene; Lutgens, Esther; Stan, Radu V.; Simons, Michael

doi:10.1242/jcs.01190

Cited by 123 publications

(105 citation statements)

References 44 publications

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“…The timing of EGFR co-localization with EEA1-containing endosomes was delayed, which could be due to the altered ubiquitylation and subsequent endocytosis of the receptors associated with HSPG in TERM. Syndecans are known to mediate endocytosis of heparin-binding ligands and proteins (e.g., FGF2 or eosinophil cationic protein) by macropinocytosis (42,43). This pathway is slow and involves formation of uncoated vesicles that eventually fuse with sorting endosomes.…”

Section: Discussionmentioning

confidence: 99%

Metastasis Suppressor Tetraspanin CD82/KAI1 Regulates Ubiquitylation of Epidermal Growth Factor Receptor

Odintsova

Niel

Conjeaud

et al. 2013

Journal of Biological Chemistry

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Background: Tetraspanin CD82/KAI1 is associated with EGF receptor and regulates its signaling. Results: CD82 controls ubiquitylation of EGF receptor after stimulation with heparin-binding ligands and alters receptor trafficking. Conclusion: CD82 regulates communication between heparan sulfate proteoglycans and ligand-bound EGFR, thus affecting the activity of c-Cbl. Significance: Lateral cross-talk initiated by CD82-dependent interactions is critical for modulation of EGFR function.

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Section: Discussionmentioning

confidence: 99%

Metastasis Suppressor Tetraspanin CD82/KAI1 Regulates Ubiquitylation of Epidermal Growth Factor Receptor

Odintsova

Niel

Conjeaud

et al. 2013

Journal of Biological Chemistry

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“…Syndecan 4 is also expressed by endothelial cells wherein it regulates multiple aspects of angiogenesis including ligand endocytosis (e.g., FGF-2 and VEGF) and stimulates endothelial migration and tubularization (Tkachenko et al, 2004(Tkachenko et al, , 2006Nunes et al, 2008). This raises the possibility that motoneuron-derived angiogenin may stimulate endothelial cells to induce neovascularization.…”

Section: Discussionmentioning

confidence: 99%

“…Although these receptors lack catalytic activity, syndecan 4 is unique in being capable of binding phosphatidylinositol (4,5)-P2, therefore independently initiating signaling via Rac1, protein kinase C␣, PI3K, Cdc42, mTORC2, and Akt (Ilan et al, 1998;Simons and Horowitz, 2001;Tkachenko et al, 2004;Partovian et al, 2008). Previous reports have also demonstrated that the uptake of angiogenic molecules such as bFGF, which requires astroglia to mediate neuroprotection in vitro, is mediated via syndecan 4, the in vivo expression of which appears to be restricted to glial lineages (Knusel et al, 1990;Engele and Bohn, 1991;Hou et al, 1997;Hsueh and Sheng, 1999;Tkachenko et al, 2004). We therefore investigated whether angiogenin endocytosis was mediated by syndecan 4.…”

Section: The Receptor For Angiogenin Uptake Into Astrocytes Is Syndecmentioning

confidence: 99%

Motoneurons Secrete Angiogenin to Induce RNA Cleavage in Astroglia

Skorupa

King²,

Aparicio³

et al. 2012

J. Neurosci.

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Amyotrophic lateral sclerosis (ALS) is an incurable neurodegenerative disorder affecting motoneurons. Mutations in angiogenin, encoding a member of the pancreatic RNase A superfamily, segregate with ALS. We previously demonstrated that angiogenin administration shows promise as a neuroprotective therapeutic in studies using transgenic ALS mice and primary motoneuron cultures. Its mechanism of action and target cells in the spinal cord, however, are largely unknown. Using mixed motoneuron cultures, motoneuron-like NSC34 cells, and primary astroglia cultures as model systems, we here demonstrate that angiogenin is a neuronally secreted factor that is endocytosed by astroglia and mediates neuroprotection in paracrine. We show that wild-type angiogenin acts unidirectionally to induce RNA cleavage in astroglia, while the ALS-associated K40I mutant is also secreted and endocytosed, but fails to induce RNA cleavage. Angiogenin uptake into astroglia requires heparan sulfate proteoglycans, and engages clathrin-mediated endocytosis. We show that this uptake mechanism exists for mouse and human angiogenin, and delivers a functional RNase output. Moreover, we identify syndecan 4 as the angiogenin receptor mediating the selective uptake of angiogenin into astroglia. Our data provide new insights into the paracrine activities of angiogenin in the nervous system, and further highlight the critical role of non-neuronal cells in the pathogenesis of ALS.

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“…Syndecan-4 is recruited to focal adhesions (7), has both phosphatidylinositol 4,5-bisphosphate and PSD-95/ Discs-large/ZO-1 homology domain binding regions and has been implicated in the activation of protein kinase C (8). Syndecan-4 is a powerful regulator of FGF-2 signaling and can modulate growth factor response in multiple cell types (9)(10)(11). In addition, syndecan-4 is capable of signaling in response to FGF independently of FGF receptor interactions (12).…”

mentioning

confidence: 99%

Syndecan-4 proteoliposomes enhance fibroblast growth factor-2 (FGF-2)–induced proliferation, migration, and neovascularization of ischemic muscle

Jang

Albadawi

Watkins

et al. 2012

Proc. Natl. Acad. Sci. U.S.A.

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Ischemia of the myocardium and lower limbs is a common consequence of arterial disease and a major source of morbidity and mortality in modernized countries. Inducing neovascularization for the treatment of ischemia is an appealing therapeutic strategy for patients for whom traditional treatment modalities cannot be performed or are ineffective. In the past, the stimulation of blood vessel growth was pursued using direct delivery of growth factors, angiogenic gene therapy, or cellular therapy. Although therapeutic angiogenesis holds great promise for treating patients with ischemia, current methods have not found success in clinical trials. Fibroblast growth factor-2 (FGF-2) was one of the first growth factors to be tested for use in therapeutic angiogenesis. Here, we present a method for improving the biological activity of FGF-2 by codelivering the growth factor with a liposomally embedded coreceptor, syndecan-4. This technique was shown to increase FGF-2 cellular signaling, uptake, and nuclear localization in comparison with FGF-2 alone. Delivery of syndecan-4 proteoliposomes also increased endothelial proliferation, migration, and angiogenic tube formation in response to FGF-2. Using an animal model of limb ischemia, syndecan-4 proteoliposomes markedly improved the neovascularization following femoral artery ligation and recovery of perfusion of the ischemic limb. Taken together, these results support liposomal delivery of syndecan-4 as an effective means to improving the potential of using growth factors to achieve therapeutic neovascularization of ischemic tissue.

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Fibroblast growth factor 2 endocytosis in endothelial cells proceed via syndecan-4-dependent activation of Rac1 and a Cdc42-dependent macropinocytic pathway

Cited by 123 publications

References 44 publications

Metastasis Suppressor Tetraspanin CD82/KAI1 Regulates Ubiquitylation of Epidermal Growth Factor Receptor

Metastasis Suppressor Tetraspanin CD82/KAI1 Regulates Ubiquitylation of Epidermal Growth Factor Receptor

Motoneurons Secrete Angiogenin to Induce RNA Cleavage in Astroglia

Syndecan-4 proteoliposomes enhance fibroblast growth factor-2 (FGF-2)–induced proliferation, migration, and neovascularization of ischemic muscle

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