Growth stimulation of A431 cells by epidermal growth factor: identification of high-affinity receptors for epidermal growth factor by an anti-receptor monoclonal antibody.

Kawamoto, Tomoyuki; Sato, Jun; Le, Anh D.; Polikoff, J.; Sato, Gordon; Mendelsohn, John

doi:10.1073/pnas.80.5.1337

Cited by 682 publications

(382 citation statements)

References 30 publications

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“…171 The binding of the antibody initiates EGFR internalization and degradation, which leads to signal termination. 110,[172][173][174] The treatment has shown consistent benefit to clinical outcome when added to chemotherapy. 173 However, this class of treatment only inhibits ligand-dependent activation of EGFR and not autophosphorylation of the tyrosine kinase domain via constitutive activation.…”

Section: Monoclonal Antibodiesmentioning

confidence: 99%

Molecular pathology of lung cancer: key to personalized medicine

et al. 2012

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The majority of lung adenocarcinoma patients with epidermal growth factor receptor-(EGFR) mutated or EML4-ALK rearrangement-positive tumors are sensitive to tyrosine kinase inhibitors. Both primary and acquired resistance in a significant number of those patients to these therapies remains a major clinical problem. The specific molecular mechanisms associated with tyrosine kinase inhibitor resistance are not fully understood. Clinicopathological observations suggest that molecular alterations involving so-called 'driver mutations' could be used as markers that aid in the selection of patients most likely to benefit from targeted therapies. In this review, we summarize recent developments involving the specific molecular mechanisms and markers that have been associated with primary and acquired resistance to EGFR-targeted therapy in lung adenocarcinomas. Understanding these mechanisms may provide new treatment avenues and improve current treatment algorithms.

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Section: Monoclonal Antibodiesmentioning

confidence: 99%

Molecular pathology of lung cancer: key to personalized medicine

et al. 2012

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“…In order to con®rm a direct interaction between epiregulin and EGFR, ErbB-2, ErbB-3 and ErbB-4, the cross-linking analysis was performed using an anti-EGFR mAb that binds to the extracellular domain of EGFR but does not activate tyrosine kinase of EGFR (Kawamoto et al, 1983). No protein chemically crosslinked with [ 125 I]epiregulin could be immunoprecipitated by pretreatment with anti-EGFR mAb in SK-BR-3 cells (Figure 3a).…”

Section: Binding Of [ 125 I]epiregulin To Erbb Receptorsmentioning

confidence: 99%

Epiregulin binds to epidermal growth factor receptor and ErbB-4 and induces tryosine phosphorylation of epidermal growth factor receptor, ErbB-2, ErbB-3 and ErbB-4

et al. 1997

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Epiregulin is a member of the epidermal growth factor (EGF) family, and has certain characteristics that are di erent from that of EGF, including mitogenic responses and binding to EGF receptor (EGFR). Epiregulin may also have another cell surface receptor and/or induces di erent receptor heterodimerizations for intracellular signaling. We investigated the binding ability of epiregulin to four ErbB family receptors using four human breast carcinoma cell lines that expressed di erent subsets of receptors. Chemical cross-linking experiments showed that [ 125 I]epiregulin directly bound to each of EGFR and ErbB-4 but not to ErbB-2 and ErbB-3. Furthermore, although epiregulin stimulated tyrosine phosphorylation of all four ErbB receptors, the main intracellular signal was mediated by ErbB-4 and/or EGFR. The pattern of activation of ErbB family receptors was di erent from that of other EGF-related ligands. Our ®ndings indicate that ErbB-4 and EGFR are receptors for epiregulin, and suggest that EGFrelated ligands transduce signals for di erent biological responses by the hierarchical mechanism.

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“…In the present study, we investigate the mechanism of EGFR-mediated apoptosis in colorectal carcinoma cells by delineating the involvement of Bax. We report experiments utilizing mAb 225 against the EGFR which blocks binding of ligand and prevents ligand-induced activation of receptor tyrosine kinase (Kawamoto et al, 1983). We demonstrate that mAb 225-induced apoptosis in colorectal cancer cells was preceded by enhanced expression of newly synthesized Bax protein, a redistribution of Bax from the cytosol to the nucleus and subsequently to the nuclear membranes.…”

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confidence: 94%

Nuclear targeting of Bax during apoptosis in human colorectal cancer cells

et al. 1998

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Homeostasis in colonic epithelial cells is regulated by the balance between proliferative activity and cell loss by apoptosis. Because epithelial cells at the apex of colonic crypts undergo apoptosis and proliferative activity is usually restricted to the base of the crypts, it has been proposed that the limited availability of growth factorsignals at the upper portions of the crypts may trigger apoptosis. In the present studies, we investigate the mechanism of apoptosis mediated by growth factor deprivation in colorectal carcinoma cells by delineating the possible involvement of Bax and its subcellular localization. We report that inhibition of epidermal growth factor receptor (EGFR) tyrosine kinase activity and downregulation of EGFR by anti-EGFR mAb 225 induces apoptosis in human colorectal carcinoma DiFi and FET cells. Induction of apoptosis was preceded by enhanced expression of newly synthesized Bax protein, and required protein synthesis. In the mAb 225-treated cells, Bax was redistributed from the cytosol to the nucleus and subsequently, to the nuclear membranes. The observed induction of Bax expression by mAb 225 was not associated with p53 induction. However, mAb 225 treatment also triggered relocalization of p53 from the cytosol to a nuclear membrane-bound form. Induction of Bax and its redistribution to the nucleus of DiFi cells during apoptosis was also demonstrated in response to butyrate, a physiological relevant molecule in colonic epithelial cells as it is the principal short-chain fatty acid produced by bacterial fermentation of dietary ®ber in colonic epithelium. Using immuno¯uorescence and confocal microscopy, we observed that Bax is predominantly localized in the cytosol, but during apoptosis it is localized both inside and along the nuclear membrane. Taken together, these ®ndings suggest that apoptosis induced by growth factor-deprivation or butyrate may involve the subcellular redistribution of Bax in human colorectal carcinoma cells.

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Growth stimulation of A431 cells by epidermal growth factor: identification of high-affinity receptors for epidermal growth factor by an anti-receptor monoclonal antibody.

Cited by 682 publications

References 30 publications

Molecular pathology of lung cancer: key to personalized medicine

Molecular pathology of lung cancer: key to personalized medicine

Epiregulin binds to epidermal growth factor receptor and ErbB-4 and induces tryosine phosphorylation of epidermal growth factor receptor, ErbB-2, ErbB-3 and ErbB-4

Nuclear targeting of Bax during apoptosis in human colorectal cancer cells

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