Destabilization of the Epidermal Growth Factor Receptor (EGFR) by a Peptide That Inhibits EGFR Binding to Heat Shock Protein 90 and Receptor Dimerization

Ahsan, Aarif; Ray, Dipankar; Ramanand, Susmita G.; Hegde, Ashok N.; Whitehead, Christopher; Rehemtulla, Alnawaz; Morishima, Yosuke; Pratt, William B.; Osawa, Yoichi; Lawrence, Theodore S.; Nyati, Mukesh K.

doi:10.1074/jbc.m113.492280

Cited by 33 publications

(33 citation statements)

References 34 publications

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“…In addition to forming a homodimer with itself, EGFR can dimerize with other receptor tyrosine kinases including Erb2, Erb3, and c-Met leading to downstream signal transduction (Mueller et al, 2010, Ahsan et al, 2014). Additionally, EGFR binds to the chaperone protein hsp90 promoting stability of the inactivated receptor (Ahsan et al, 2013). Recent studies suggest novel drugs that degrade EGFR are more effective than drugs that inhibit EGFR in preclinical models (Haglund et al, 2003, Zhuang et al, 2003, Feng et al, 2007, Kirisits et al, 2007, Ahsan et al, 2009, Ahsan et al, 2010).…”

Section: Interaction Of Egfr With Radiation and Chemotherapymentioning

confidence: 99%

“…The development of novel agents which target EGFR by different mechanisms such as receptor degradation and inhibition of dimerization may also be necessary to overcome resistance. Additionally, combinations of EGFR targeted therapies with other novel agents, such as drugs targeting hsp90, may improve the efficacy of these therapies (Ahsan et al 2013). …”

Section: Scheduling Of Egfr Inhibitors With Radiation and Patient mentioning

confidence: 99%

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EGFR targeted therapies and radiation: Optimizing efficacy by appropriate drug scheduling and patient selection

Cuneo

Nyati

Ray

et al. 2015

Pharmacology & Therapeutics

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The epidermal growth factor receptor (EGFR) plays an important role in tumor progression and treatment resistance for many types of malignancies including head and neck, colorectal, and nonsmall cell lung cancer. Several EGFR targeted therapies are efficacious as single agents or in combination with chemotherapy. Given the toxicity associated with chemoradiation and poor outcomes seen in several types of cancers, combinations of EGFR targeted agents with or without chemotherapy have been tested in patients receiving radiation. To date, the only FDA approved use of an anti-EGFR therapy in combination with radiation therapy is for locally advanced head and neck cancer. Given the important role EGFR plays in lung and colorectal cancer and the benefit of EGFR inhibition combined with chemotherapy in these disease sites, it is perplexing why EGFR targeted therapies in combination with radiation or chemoradiation have not been more successful. In this review we summarize the clinical findings of EGFR targeted therapies combined with radiation and chemoradiation regimens. We then discuss the interaction between EGFR and radiation including radiation induced EGFR signaling, the effect of EGFR on DNA damage repair, and potential mechanisms of radiosensitization. Finally, we examine the potential pitfalls with scheduling EGFR targeted therapies with chemoradiation and the use of predictive biomarkers to improve patient selection.

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Section: Interaction Of Egfr With Radiation and Chemotherapymentioning

confidence: 99%

Section: Scheduling Of Egfr Inhibitors With Radiation and Patient mentioning

confidence: 99%

EGFR targeted therapies and radiation: Optimizing efficacy by appropriate drug scheduling and patient selection

Cuneo

Nyati

Ray

et al. 2015

Pharmacology & Therapeutics

Self Cite

View full text Add to dashboard Cite

show abstract

“…Investigations of HSP90 are the most advanced, as this important chaperone molecule that regulates the folding and stability of a number of receptor tyrosine kinase proteins such as HER-2 or EGFR (Ahsan et al, 2013;Sidera et al, 2008). Since HER-2 plays an essential role in mammary tumorigenesis, HSP90 inhibitors that can induce HER-2 degradation and selectively eliminate cancer cells that express HER-2 on the cell surface membrane are greatly anticipated as novel mammary tumor therapies (Schulz et al, 2014).…”

Section: Discussionmentioning

confidence: 99%

Localization of heat shock protein 110 in canine mammary gland tumors

Okada

Furuya

Takenaka

et al. 2015

Veterinary Immunology and Immunopathology

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“…Although few in number, there are indications that peptide therapy may have interesting potential in cancer therapy. For example, similar to small molecule inhibitors of tyrosine kinases targeting EGFR involved in proliferation and migration of cancer cells, a synthetic six amino acid peptide of the alphaC-beta4 loop region of EGFR has been shown to inhibit the dimerization and signaling activity of EGFR in the presence of its ligand 17 . This short peptide, targeting EGFR’s ATP-binding cleft and its dimerization face, additionally promotes EGFR interaction with the heat shock protein Hsp90, thereby catalyzing EGFR degradation as well 17 .…”

Section: Peptides As Potential Anticancer Drugsmentioning

confidence: 99%

“…For example, similar to small molecule inhibitors of tyrosine kinases targeting EGFR involved in proliferation and migration of cancer cells, a synthetic six amino acid peptide of the alphaC-beta4 loop region of EGFR has been shown to inhibit the dimerization and signaling activity of EGFR in the presence of its ligand 17 . This short peptide, targeting EGFR’s ATP-binding cleft and its dimerization face, additionally promotes EGFR interaction with the heat shock protein Hsp90, thereby catalyzing EGFR degradation as well 17 . Indeed, several peptides such as Cilengitide, Trebananib, NGR-hTNF, Tyroserleutide, etc., are currently undergoing phase III clinical trials in patients with glioblastoma, ovarian, mesothelioma, or liver cancers 16 .…”

Section: Peptides As Potential Anticancer Drugsmentioning

confidence: 99%

Bacterial proteins and peptides in cancer therapy

2014

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Cancer is one of the most deadly diseases worldwide. In the last three decades many efforts have been made focused on understanding how cancer grows and responds to drugs. The dominant drug-development paradigm has been the “one drug, one target.” Based on that, the two main targeted therapies developed to combat cancer include the use of tyrosine kinase inhibitors and monoclonal antibodies. Development of drug resistance and side effects represent the major limiting factors for their use in cancer treatment. Nowadays, a new paradigm for cancer drug discovery is emerging wherein multi-targeted approaches gain ground in cancer therapy. Therefore, to overcome resistance to therapy, it is clear that a new generation of drugs is urgently needed. Here, regarding the concept of multi-targeted therapy, we discuss the challenges of using bacterial proteins and peptides as a new generation of effective anti-cancer drugs.

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Destabilization of the Epidermal Growth Factor Receptor (EGFR) by a Peptide That Inhibits EGFR Binding to Heat Shock Protein 90 and Receptor Dimerization

Cited by 33 publications

References 34 publications

EGFR targeted therapies and radiation: Optimizing efficacy by appropriate drug scheduling and patient selection

EGFR targeted therapies and radiation: Optimizing efficacy by appropriate drug scheduling and patient selection

Localization of heat shock protein 110 in canine mammary gland tumors

Bacterial proteins and peptides in cancer therapy

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