A novel pH-dependent membrane peptide that binds to EphA2 and inhibits cell migration
Misregulation of the signaling axis formed by the receptor tyrosine kinase (RTK) EphA2 and its ligand, ephrinA1, causes aberrant cell-cell contacts that contribute to metastasis. Solid tumors are characterized by an acidic extracellular medium. We intend to take advantage of this tumor feature to de...
| Main Authors: | , , , , , , , , , , , |
|---|---|
| Format: | Article |
| Language: | English |
| Published: |
eLife Sciences Publications Ltd
2018-09-01
|
| Series: | eLife |
| Subjects: | |
| Online Access: | https://elifesciences.org/articles/36645 |
| id |
doaj-c5d8558633184388971353fd6c908488 |
|---|---|
| record_format |
Article |
| spelling |
doaj-c5d8558633184388971353fd6c9084882021-05-05T16:09:19ZengeLife Sciences Publications LtdeLife2050-084X2018-09-01710.7554/eLife.36645A novel pH-dependent membrane peptide that binds to EphA2 and inhibits cell migrationDaiane S Alves0https://orcid.org/0000-0001-9154-4748Justin M Westerfield1https://orcid.org/0000-0002-3937-5833Xiaojun Shi2https://orcid.org/0000-0002-8060-5880Vanessa P Nguyen3https://orcid.org/0000-0002-7650-0138Katherine M Stefanski4https://orcid.org/0000-0003-3007-0598Kristen R Booth5Soyeon Kim6Jennifer Morrell-Falvey7https://orcid.org/0000-0002-9362-7528Bing-Cheng Wang8Steven M Abel9https://orcid.org/0000-0003-0491-8647Adam W Smith10https://orcid.org/0000-0001-5216-9017Francisco N Barrera11https://orcid.org/0000-0002-5200-7891Department of Biochemistry & Cellular and Molecular Biology, University of Tennessee, Knoxville, United StatesDepartment of Biochemistry & Cellular and Molecular Biology, University of Tennessee, Knoxville, United StatesDepartment of Chemistry, University of Akron, Akron, United States; Department of Physiology and Biophysics, Case Western Reserve University, Cleveland, United States; Pharmacology, Case Western Reserve University, Cleveland, United States; Rammelkamp Center for Research, MetroHealth Medical Center, Cleveland, United StatesDepartment of Biochemistry & Cellular and Molecular Biology, University of Tennessee, Knoxville, United StatesGraduate School of Genome Science and Technology, University of Tennessee, Knoxville, United StatesDepartment of Biochemistry & Cellular and Molecular Biology, University of Tennessee, Knoxville, United StatesDepartment of Chemistry, University of Akron, Akron, United StatesDepartment of Biochemistry & Cellular and Molecular Biology, University of Tennessee, Knoxville, United States; Biosciences Division, Oak Ridge National Laboratory, Oak Ridge, United StatesDepartment of Physiology and Biophysics, Case Western Reserve University, Cleveland, United States; Pharmacology, Case Western Reserve University, Cleveland, United States; Rammelkamp Center for Research, MetroHealth Medical Center, Cleveland, United StatesDepartment of Chemical and Biomolecular Engineering, University of Tennessee, Knoxville, United States; National Institute for Mathematical and Biological Synthesis, University of Tennessee, Knoxville, United StatesDepartment of Chemistry, University of Akron, Akron, United StatesDepartment of Biochemistry & Cellular and Molecular Biology, University of Tennessee, Knoxville, United StatesMisregulation of the signaling axis formed by the receptor tyrosine kinase (RTK) EphA2 and its ligand, ephrinA1, causes aberrant cell-cell contacts that contribute to metastasis. Solid tumors are characterized by an acidic extracellular medium. We intend to take advantage of this tumor feature to design new molecules that specifically target tumors. We created a novel pH-dependent transmembrane peptide, TYPE7, by altering the sequence of the transmembrane domain of EphA2. TYPE7 is highly soluble and interacts with the surface of lipid membranes at neutral pH, while acidity triggers transmembrane insertion. TYPE7 binds to endogenous EphA2 and reduces Akt phosphorylation and cell migration as effectively as ephrinA1. Interestingly, we found large differences in juxtamembrane tyrosine phosphorylation and the extent of EphA2 clustering when comparing TYPE7 with activation by ephrinA1. This work shows that it is possible to design new pH-triggered membrane peptides to activate RTK and gain insights on its activation mechanism.https://elifesciences.org/articles/36645EphA2 activationreceptor tyrosine kinasemembrane active peptidepH responsive |
| collection |
DOAJ |
| language |
English |
| format |
Article |
| sources |
DOAJ |
| author |
Daiane S Alves Justin M Westerfield Xiaojun Shi Vanessa P Nguyen Katherine M Stefanski Kristen R Booth Soyeon Kim Jennifer Morrell-Falvey Bing-Cheng Wang Steven M Abel Adam W Smith Francisco N Barrera |
| spellingShingle |
Daiane S Alves Justin M Westerfield Xiaojun Shi Vanessa P Nguyen Katherine M Stefanski Kristen R Booth Soyeon Kim Jennifer Morrell-Falvey Bing-Cheng Wang Steven M Abel Adam W Smith Francisco N Barrera A novel pH-dependent membrane peptide that binds to EphA2 and inhibits cell migration eLife EphA2 activation receptor tyrosine kinase membrane active peptide pH responsive |
| author_facet |
Daiane S Alves Justin M Westerfield Xiaojun Shi Vanessa P Nguyen Katherine M Stefanski Kristen R Booth Soyeon Kim Jennifer Morrell-Falvey Bing-Cheng Wang Steven M Abel Adam W Smith Francisco N Barrera |
| author_sort |
Daiane S Alves |
| title |
A novel pH-dependent membrane peptide that binds to EphA2 and inhibits cell migration |
| title_short |
A novel pH-dependent membrane peptide that binds to EphA2 and inhibits cell migration |
| title_full |
A novel pH-dependent membrane peptide that binds to EphA2 and inhibits cell migration |
| title_fullStr |
A novel pH-dependent membrane peptide that binds to EphA2 and inhibits cell migration |
| title_full_unstemmed |
A novel pH-dependent membrane peptide that binds to EphA2 and inhibits cell migration |
| title_sort |
novel ph-dependent membrane peptide that binds to epha2 and inhibits cell migration |
| publisher |
eLife Sciences Publications Ltd |
| series |
eLife |
| issn |
2050-084X |
| publishDate |
2018-09-01 |
| description |
Misregulation of the signaling axis formed by the receptor tyrosine kinase (RTK) EphA2 and its ligand, ephrinA1, causes aberrant cell-cell contacts that contribute to metastasis. Solid tumors are characterized by an acidic extracellular medium. We intend to take advantage of this tumor feature to design new molecules that specifically target tumors. We created a novel pH-dependent transmembrane peptide, TYPE7, by altering the sequence of the transmembrane domain of EphA2. TYPE7 is highly soluble and interacts with the surface of lipid membranes at neutral pH, while acidity triggers transmembrane insertion. TYPE7 binds to endogenous EphA2 and reduces Akt phosphorylation and cell migration as effectively as ephrinA1. Interestingly, we found large differences in juxtamembrane tyrosine phosphorylation and the extent of EphA2 clustering when comparing TYPE7 with activation by ephrinA1. This work shows that it is possible to design new pH-triggered membrane peptides to activate RTK and gain insights on its activation mechanism. |
| topic |
EphA2 activation receptor tyrosine kinase membrane active peptide pH responsive |
| url |
https://elifesciences.org/articles/36645 |
| work_keys_str_mv |
AT daianesalves anovelphdependentmembranepeptidethatbindstoepha2andinhibitscellmigration AT justinmwesterfield anovelphdependentmembranepeptidethatbindstoepha2andinhibitscellmigration AT xiaojunshi anovelphdependentmembranepeptidethatbindstoepha2andinhibitscellmigration AT vanessapnguyen anovelphdependentmembranepeptidethatbindstoepha2andinhibitscellmigration AT katherinemstefanski anovelphdependentmembranepeptidethatbindstoepha2andinhibitscellmigration AT kristenrbooth anovelphdependentmembranepeptidethatbindstoepha2andinhibitscellmigration AT soyeonkim anovelphdependentmembranepeptidethatbindstoepha2andinhibitscellmigration AT jennifermorrellfalvey anovelphdependentmembranepeptidethatbindstoepha2andinhibitscellmigration AT bingchengwang anovelphdependentmembranepeptidethatbindstoepha2andinhibitscellmigration AT stevenmabel anovelphdependentmembranepeptidethatbindstoepha2andinhibitscellmigration AT adamwsmith anovelphdependentmembranepeptidethatbindstoepha2andinhibitscellmigration AT francisconbarrera anovelphdependentmembranepeptidethatbindstoepha2andinhibitscellmigration AT daianesalves novelphdependentmembranepeptidethatbindstoepha2andinhibitscellmigration AT justinmwesterfield novelphdependentmembranepeptidethatbindstoepha2andinhibitscellmigration AT xiaojunshi novelphdependentmembranepeptidethatbindstoepha2andinhibitscellmigration AT vanessapnguyen novelphdependentmembranepeptidethatbindstoepha2andinhibitscellmigration AT katherinemstefanski novelphdependentmembranepeptidethatbindstoepha2andinhibitscellmigration AT kristenrbooth novelphdependentmembranepeptidethatbindstoepha2andinhibitscellmigration AT soyeonkim novelphdependentmembranepeptidethatbindstoepha2andinhibitscellmigration AT jennifermorrellfalvey novelphdependentmembranepeptidethatbindstoepha2andinhibitscellmigration AT bingchengwang novelphdependentmembranepeptidethatbindstoepha2andinhibitscellmigration AT stevenmabel novelphdependentmembranepeptidethatbindstoepha2andinhibitscellmigration AT adamwsmith novelphdependentmembranepeptidethatbindstoepha2andinhibitscellmigration AT francisconbarrera novelphdependentmembranepeptidethatbindstoepha2andinhibitscellmigration |
| _version_ |
1721459593037479936 |