random 12 mer peptides Search Results


heptapeptide phage display library  (Mimotopes)
90
Mimotopes heptapeptide phage display library
Heptapeptide Phage Display Library, supplied by Mimotopes, used in various techniques. Bioz Stars score: 90/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
https://www.bioz.com/result/heptapeptide phage display library/product/Mimotopes
Average 90 stars, based on 1 article reviews
heptapeptide phage display library - by Bioz Stars, 2026-03
90/100 stars
  Buy from Supplier
12-mer wildtype mutant peptides spanning ppxy motifs icd human erbb4  (GenScript corporation)
90
GenScript corporation 12-mer wildtype mutant peptides spanning ppxy motifs icd human erbb4
Modular organization of human <t>ErbB4</t> and YAP2 proteins. (a) ErbB4 contains the canonical ECD-TM-ICD receptor tyrosine kinase modular cassette, where the central single-helical transmembrane (TM) domain is flanked between an N-terminal extracellular domain (ECD) and a C-terminal intracellular domain (ICD). The three PPXY motifs (designated PY1, PY2 and PY3) within the ICD are located at the extreme C-terminus. Note that the amino acid sequence of 12-mer peptides containing the PPXY motifs and flanking residues are provided. The numerals indicate the nomenclature used in this study to distinguish residues within and flanking the PPXY motifs relative to the first consensus proline, which is arbitrarily assigned zero. (b) YAP2 is comprised of a tandem copy of WW domains, designated WW1 and WW2, located N-terminal to the trans-activation (TA) domain.
12 Mer Wildtype Mutant Peptides Spanning Ppxy Motifs Icd Human Erbb4, supplied by GenScript corporation, used in various techniques. Bioz Stars score: 90/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
https://www.bioz.com/result/12-mer wildtype mutant peptides spanning ppxy motifs icd human erbb4/product/GenScript corporation
Average 90 stars, based on 1 article reviews
12-mer wildtype mutant peptides spanning ppxy motifs icd human erbb4 - by Bioz Stars, 2026-03
90/100 stars
  Buy from Supplier
a mixture of 9 overlapping peptides (9-mer) spanning kras codon 12  (Peptron Inc)
90
Peptron Inc a mixture of 9 overlapping peptides (9-mer) spanning kras codon 12
Modular organization of human <t>ErbB4</t> and YAP2 proteins. (a) ErbB4 contains the canonical ECD-TM-ICD receptor tyrosine kinase modular cassette, where the central single-helical transmembrane (TM) domain is flanked between an N-terminal extracellular domain (ECD) and a C-terminal intracellular domain (ICD). The three PPXY motifs (designated PY1, PY2 and PY3) within the ICD are located at the extreme C-terminus. Note that the amino acid sequence of 12-mer peptides containing the PPXY motifs and flanking residues are provided. The numerals indicate the nomenclature used in this study to distinguish residues within and flanking the PPXY motifs relative to the first consensus proline, which is arbitrarily assigned zero. (b) YAP2 is comprised of a tandem copy of WW domains, designated WW1 and WW2, located N-terminal to the trans-activation (TA) domain.
A Mixture Of 9 Overlapping Peptides (9 Mer) Spanning Kras Codon 12, supplied by Peptron Inc, used in various techniques. Bioz Stars score: 90/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
https://www.bioz.com/result/a mixture of 9 overlapping peptides (9-mer) spanning kras codon 12/product/Peptron Inc
Average 90 stars, based on 1 article reviews
a mixture of 9 overlapping peptides (9-mer) spanning kras codon 12 - by Bioz Stars, 2026-03
90/100 stars
  Buy from Supplier
low affinity 12-mer peptide p53  (Novartis)
90
Novartis low affinity 12-mer peptide p53
Modular organization of human <t>ErbB4</t> and YAP2 proteins. (a) ErbB4 contains the canonical ECD-TM-ICD receptor tyrosine kinase modular cassette, where the central single-helical transmembrane (TM) domain is flanked between an N-terminal extracellular domain (ECD) and a C-terminal intracellular domain (ICD). The three PPXY motifs (designated PY1, PY2 and PY3) within the ICD are located at the extreme C-terminus. Note that the amino acid sequence of 12-mer peptides containing the PPXY motifs and flanking residues are provided. The numerals indicate the nomenclature used in this study to distinguish residues within and flanking the PPXY motifs relative to the first consensus proline, which is arbitrarily assigned zero. (b) YAP2 is comprised of a tandem copy of WW domains, designated WW1 and WW2, located N-terminal to the trans-activation (TA) domain.
Low Affinity 12 Mer Peptide P53, supplied by Novartis, used in various techniques. Bioz Stars score: 90/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
https://www.bioz.com/result/low affinity 12-mer peptide p53/product/Novartis
Average 90 stars, based on 1 article reviews
low affinity 12-mer peptide p53 - by Bioz Stars, 2026-03
90/100 stars
  Buy from Supplier
peptides encoding the wbp1 tail (wild-type, kkletfkktn; mutant, kkletfsstn)  (GenScript corporation)
90
GenScript corporation peptides encoding the wbp1 tail (wild-type, kkletfkktn; mutant, kkletfsstn)
Modular organization of human <t>ErbB4</t> and YAP2 proteins. (a) ErbB4 contains the canonical ECD-TM-ICD receptor tyrosine kinase modular cassette, where the central single-helical transmembrane (TM) domain is flanked between an N-terminal extracellular domain (ECD) and a C-terminal intracellular domain (ICD). The three PPXY motifs (designated PY1, PY2 and PY3) within the ICD are located at the extreme C-terminus. Note that the amino acid sequence of 12-mer peptides containing the PPXY motifs and flanking residues are provided. The numerals indicate the nomenclature used in this study to distinguish residues within and flanking the PPXY motifs relative to the first consensus proline, which is arbitrarily assigned zero. (b) YAP2 is comprised of a tandem copy of WW domains, designated WW1 and WW2, located N-terminal to the trans-activation (TA) domain.
Peptides Encoding The Wbp1 Tail (Wild Type, Kkletfkktn; Mutant, Kkletfsstn), supplied by GenScript corporation, used in various techniques. Bioz Stars score: 90/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
https://www.bioz.com/result/peptides encoding the wbp1 tail (wild-type, kkletfkktn; mutant, kkletfsstn)/product/GenScript corporation
Average 90 stars, based on 1 article reviews
peptides encoding the wbp1 tail (wild-type, kkletfkktn; mutant, kkletfsstn) - by Bioz Stars, 2026-03
90/100 stars
  Buy from Supplier
overlapping 12-mer peptides  (Pepscan Inc)
90
Pepscan Inc overlapping 12-mer peptides
Modular organization of human <t>ErbB4</t> and YAP2 proteins. (a) ErbB4 contains the canonical ECD-TM-ICD receptor tyrosine kinase modular cassette, where the central single-helical transmembrane (TM) domain is flanked between an N-terminal extracellular domain (ECD) and a C-terminal intracellular domain (ICD). The three PPXY motifs (designated PY1, PY2 and PY3) within the ICD are located at the extreme C-terminus. Note that the amino acid sequence of 12-mer peptides containing the PPXY motifs and flanking residues are provided. The numerals indicate the nomenclature used in this study to distinguish residues within and flanking the PPXY motifs relative to the first consensus proline, which is arbitrarily assigned zero. (b) YAP2 is comprised of a tandem copy of WW domains, designated WW1 and WW2, located N-terminal to the trans-activation (TA) domain.
Overlapping 12 Mer Peptides, supplied by Pepscan Inc, used in various techniques. Bioz Stars score: 90/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
https://www.bioz.com/result/overlapping 12-mer peptides/product/Pepscan Inc
Average 90 stars, based on 1 article reviews
overlapping 12-mer peptides - by Bioz Stars, 2026-03
90/100 stars
  Buy from Supplier
17-mer peptides overlapping by 11-12 amino acids encompassing the entire sequence of all influenza viral proteins  (BEI Resources)
90
BEI Resources 17-mer peptides overlapping by 11-12 amino acids encompassing the entire sequence of all influenza viral proteins
Modular organization of human <t>ErbB4</t> and YAP2 proteins. (a) ErbB4 contains the canonical ECD-TM-ICD receptor tyrosine kinase modular cassette, where the central single-helical transmembrane (TM) domain is flanked between an N-terminal extracellular domain (ECD) and a C-terminal intracellular domain (ICD). The three PPXY motifs (designated PY1, PY2 and PY3) within the ICD are located at the extreme C-terminus. Note that the amino acid sequence of 12-mer peptides containing the PPXY motifs and flanking residues are provided. The numerals indicate the nomenclature used in this study to distinguish residues within and flanking the PPXY motifs relative to the first consensus proline, which is arbitrarily assigned zero. (b) YAP2 is comprised of a tandem copy of WW domains, designated WW1 and WW2, located N-terminal to the trans-activation (TA) domain.
17 Mer Peptides Overlapping By 11 12 Amino Acids Encompassing The Entire Sequence Of All Influenza Viral Proteins, supplied by BEI Resources, used in various techniques. Bioz Stars score: 90/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
https://www.bioz.com/result/17-mer peptides overlapping by 11-12 amino acids encompassing the entire sequence of all influenza viral proteins/product/BEI Resources
Average 90 stars, based on 1 article reviews
17-mer peptides overlapping by 11-12 amino acids encompassing the entire sequence of all influenza viral proteins - by Bioz Stars, 2026-03
90/100 stars
  Buy from Supplier
random 20-mer peptide library  (AdAlta Inc)
90
AdAlta Inc random 20-mer peptide library
Modular organization of human <t>ErbB4</t> and YAP2 proteins. (a) ErbB4 contains the canonical ECD-TM-ICD receptor tyrosine kinase modular cassette, where the central single-helical transmembrane (TM) domain is flanked between an N-terminal extracellular domain (ECD) and a C-terminal intracellular domain (ICD). The three PPXY motifs (designated PY1, PY2 and PY3) within the ICD are located at the extreme C-terminus. Note that the amino acid sequence of 12-mer peptides containing the PPXY motifs and flanking residues are provided. The numerals indicate the nomenclature used in this study to distinguish residues within and flanking the PPXY motifs relative to the first consensus proline, which is arbitrarily assigned zero. (b) YAP2 is comprised of a tandem copy of WW domains, designated WW1 and WW2, located N-terminal to the trans-activation (TA) domain.
Random 20 Mer Peptide Library, supplied by AdAlta Inc, used in various techniques. Bioz Stars score: 90/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
https://www.bioz.com/result/random 20-mer peptide library/product/AdAlta Inc
Average 90 stars, based on 1 article reviews
random 20-mer peptide library - by Bioz Stars, 2026-03
90/100 stars
  Buy from Supplier
mutant peptides (w5k, w5f, y9f, l11q and r15q)  (GenScript corporation)
90
GenScript corporation mutant peptides (w5k, w5f, y9f, l11q and r15q)
Modular organization of human <t>ErbB4</t> and YAP2 proteins. (a) ErbB4 contains the canonical ECD-TM-ICD receptor tyrosine kinase modular cassette, where the central single-helical transmembrane (TM) domain is flanked between an N-terminal extracellular domain (ECD) and a C-terminal intracellular domain (ICD). The three PPXY motifs (designated PY1, PY2 and PY3) within the ICD are located at the extreme C-terminus. Note that the amino acid sequence of 12-mer peptides containing the PPXY motifs and flanking residues are provided. The numerals indicate the nomenclature used in this study to distinguish residues within and flanking the PPXY motifs relative to the first consensus proline, which is arbitrarily assigned zero. (b) YAP2 is comprised of a tandem copy of WW domains, designated WW1 and WW2, located N-terminal to the trans-activation (TA) domain.
Mutant Peptides (W5k, W5f, Y9f, L11q And R15q), supplied by GenScript corporation, used in various techniques. Bioz Stars score: 90/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
https://www.bioz.com/result/mutant peptides (w5k, w5f, y9f, l11q and r15q)/product/GenScript corporation
Average 90 stars, based on 1 article reviews
mutant peptides (w5k, w5f, y9f, l11q and r15q) - by Bioz Stars, 2026-03
90/100 stars
  Buy from Supplier
12-mer amino acids  (JPT Peptide Technologies GmbH)
90
JPT Peptide Technologies GmbH 12-mer amino acids
Modular organization of human <t>ErbB4</t> and YAP2 proteins. (a) ErbB4 contains the canonical ECD-TM-ICD receptor tyrosine kinase modular cassette, where the central single-helical transmembrane (TM) domain is flanked between an N-terminal extracellular domain (ECD) and a C-terminal intracellular domain (ICD). The three PPXY motifs (designated PY1, PY2 and PY3) within the ICD are located at the extreme C-terminus. Note that the amino acid sequence of 12-mer peptides containing the PPXY motifs and flanking residues are provided. The numerals indicate the nomenclature used in this study to distinguish residues within and flanking the PPXY motifs relative to the first consensus proline, which is arbitrarily assigned zero. (b) YAP2 is comprised of a tandem copy of WW domains, designated WW1 and WW2, located N-terminal to the trans-activation (TA) domain.
12 Mer Amino Acids, supplied by JPT Peptide Technologies GmbH, used in various techniques. Bioz Stars score: 90/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
https://www.bioz.com/result/12-mer amino acids/product/JPT Peptide Technologies GmbH
Average 90 stars, based on 1 article reviews
12-mer amino acids - by Bioz Stars, 2026-03
90/100 stars
  Buy from Supplier
12-mer peptide dhlaslwwgtel  (GL Biochem)
90
GL Biochem 12-mer peptide dhlaslwwgtel
Modular organization of human <t>ErbB4</t> and YAP2 proteins. (a) ErbB4 contains the canonical ECD-TM-ICD receptor tyrosine kinase modular cassette, where the central single-helical transmembrane (TM) domain is flanked between an N-terminal extracellular domain (ECD) and a C-terminal intracellular domain (ICD). The three PPXY motifs (designated PY1, PY2 and PY3) within the ICD are located at the extreme C-terminus. Note that the amino acid sequence of 12-mer peptides containing the PPXY motifs and flanking residues are provided. The numerals indicate the nomenclature used in this study to distinguish residues within and flanking the PPXY motifs relative to the first consensus proline, which is arbitrarily assigned zero. (b) YAP2 is comprised of a tandem copy of WW domains, designated WW1 and WW2, located N-terminal to the trans-activation (TA) domain.
12 Mer Peptide Dhlaslwwgtel, supplied by GL Biochem, used in various techniques. Bioz Stars score: 90/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
https://www.bioz.com/result/12-mer peptide dhlaslwwgtel/product/GL Biochem
Average 90 stars, based on 1 article reviews
12-mer peptide dhlaslwwgtel - by Bioz Stars, 2026-03
90/100 stars
  Buy from Supplier
16 mer peptides overlapping by 12 residues  (Mimotopes)
90
Mimotopes 16 mer peptides overlapping by 12 residues
Modular organization of human <t>ErbB4</t> and YAP2 proteins. (a) ErbB4 contains the canonical ECD-TM-ICD receptor tyrosine kinase modular cassette, where the central single-helical transmembrane (TM) domain is flanked between an N-terminal extracellular domain (ECD) and a C-terminal intracellular domain (ICD). The three PPXY motifs (designated PY1, PY2 and PY3) within the ICD are located at the extreme C-terminus. Note that the amino acid sequence of 12-mer peptides containing the PPXY motifs and flanking residues are provided. The numerals indicate the nomenclature used in this study to distinguish residues within and flanking the PPXY motifs relative to the first consensus proline, which is arbitrarily assigned zero. (b) YAP2 is comprised of a tandem copy of WW domains, designated WW1 and WW2, located N-terminal to the trans-activation (TA) domain.
16 Mer Peptides Overlapping By 12 Residues, supplied by Mimotopes, used in various techniques. Bioz Stars score: 90/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
https://www.bioz.com/result/16 mer peptides overlapping by 12 residues/product/Mimotopes
Average 90 stars, based on 1 article reviews
16 mer peptides overlapping by 12 residues - by Bioz Stars, 2026-03
90/100 stars
  Buy from Supplier

Image Search Results


Modular organization of human ErbB4 and YAP2 proteins. (a) ErbB4 contains the canonical ECD-TM-ICD receptor tyrosine kinase modular cassette, where the central single-helical transmembrane (TM) domain is flanked between an N-terminal extracellular domain (ECD) and a C-terminal intracellular domain (ICD). The three PPXY motifs (designated PY1, PY2 and PY3) within the ICD are located at the extreme C-terminus. Note that the amino acid sequence of 12-mer peptides containing the PPXY motifs and flanking residues are provided. The numerals indicate the nomenclature used in this study to distinguish residues within and flanking the PPXY motifs relative to the first consensus proline, which is arbitrarily assigned zero. (b) YAP2 is comprised of a tandem copy of WW domains, designated WW1 and WW2, located N-terminal to the trans-activation (TA) domain.

Journal: Biochimie

Article Title: Molecular Basis of the Binding of YAP Transcriptional Regulator to the ErbB4 Receptor Tyrosine Kinase

doi: 10.1016/j.biochi.2014.01.011

Figure Lengend Snippet: Modular organization of human ErbB4 and YAP2 proteins. (a) ErbB4 contains the canonical ECD-TM-ICD receptor tyrosine kinase modular cassette, where the central single-helical transmembrane (TM) domain is flanked between an N-terminal extracellular domain (ECD) and a C-terminal intracellular domain (ICD). The three PPXY motifs (designated PY1, PY2 and PY3) within the ICD are located at the extreme C-terminus. Note that the amino acid sequence of 12-mer peptides containing the PPXY motifs and flanking residues are provided. The numerals indicate the nomenclature used in this study to distinguish residues within and flanking the PPXY motifs relative to the first consensus proline, which is arbitrarily assigned zero. (b) YAP2 is comprised of a tandem copy of WW domains, designated WW1 and WW2, located N-terminal to the trans-activation (TA) domain.

Article Snippet: Peptide synthesis 12-mer wildtype and mutant peptides spanning various PPXY motifs within the ICD of human ErbB4 were commercially obtained from GenScript Corporation.

Techniques: Sequencing, Activation Assay

Representative ITC isotherms for the binding of WW1 domain of YAP2 to ErbB4_PY1 (a), ErbB4_PY2 (b) and ErbB4_PY3 (c) peptides. The upper panels show the raw ITC data expressed as change in thermal power with respect to time over the period of titration. In the lower panels, change in molar heat is expressed as a function of molar ratio of corresponding peptide to WW1 domain. The red solid lines in the lower panels show the fit of data to a one-site binding model using the integrated ORIGIN software as described earlier [22, 20].

Journal: Biochimie

Article Title: Molecular Basis of the Binding of YAP Transcriptional Regulator to the ErbB4 Receptor Tyrosine Kinase

doi: 10.1016/j.biochi.2014.01.011

Figure Lengend Snippet: Representative ITC isotherms for the binding of WW1 domain of YAP2 to ErbB4_PY1 (a), ErbB4_PY2 (b) and ErbB4_PY3 (c) peptides. The upper panels show the raw ITC data expressed as change in thermal power with respect to time over the period of titration. In the lower panels, change in molar heat is expressed as a function of molar ratio of corresponding peptide to WW1 domain. The red solid lines in the lower panels show the fit of data to a one-site binding model using the integrated ORIGIN software as described earlier [22, 20].

Article Snippet: Peptide synthesis 12-mer wildtype and mutant peptides spanning various PPXY motifs within the ICD of human ErbB4 were commercially obtained from GenScript Corporation.

Techniques: Binding Assay, Titration, Software

Thermodynamic parameters for the binding of WW1 and WW2 domains of YAP2 to PPXY peptides derived from the ICD of ErbB4

Journal: Biochimie

Article Title: Molecular Basis of the Binding of YAP Transcriptional Regulator to the ErbB4 Receptor Tyrosine Kinase

doi: 10.1016/j.biochi.2014.01.011

Figure Lengend Snippet: Thermodynamic parameters for the binding of WW1 and WW2 domains of YAP2 to PPXY peptides derived from the ICD of ErbB4

Article Snippet: Peptide synthesis 12-mer wildtype and mutant peptides spanning various PPXY motifs within the ICD of human ErbB4 were commercially obtained from GenScript Corporation.

Techniques: Binding Assay, Derivative Assay, Sequencing

Thermodynamic parameters for the binding of WW1 domain of YAP2 to wildtype (PY3_WT) and single alanine mutants of ErbB4_PY3 peptide

Journal: Biochimie

Article Title: Molecular Basis of the Binding of YAP Transcriptional Regulator to the ErbB4 Receptor Tyrosine Kinase

doi: 10.1016/j.biochi.2014.01.011

Figure Lengend Snippet: Thermodynamic parameters for the binding of WW1 domain of YAP2 to wildtype (PY3_WT) and single alanine mutants of ErbB4_PY3 peptide

Article Snippet: Peptide synthesis 12-mer wildtype and mutant peptides spanning various PPXY motifs within the ICD of human ErbB4 were commercially obtained from GenScript Corporation.

Techniques: Binding Assay, Sequencing

Thermodynamic parameters for the binding of WW2 domain of YAP2 to wildtype (PY3_WT) and single alanine mutants of ErbB4_PY3 peptide

Journal: Biochimie

Article Title: Molecular Basis of the Binding of YAP Transcriptional Regulator to the ErbB4 Receptor Tyrosine Kinase

doi: 10.1016/j.biochi.2014.01.011

Figure Lengend Snippet: Thermodynamic parameters for the binding of WW2 domain of YAP2 to wildtype (PY3_WT) and single alanine mutants of ErbB4_PY3 peptide

Article Snippet: Peptide synthesis 12-mer wildtype and mutant peptides spanning various PPXY motifs within the ICD of human ErbB4 were commercially obtained from GenScript Corporation.

Techniques: Binding Assay, Sequencing

Far-UV CD spectra of ErbB4_PY1 (red), ErbB4_PY2 (green) and ErbB4_PY3 (blue) peptides. Note that the mean ellipticity, [θ], was calculated using Eq [3].

Journal: Biochimie

Article Title: Molecular Basis of the Binding of YAP Transcriptional Regulator to the ErbB4 Receptor Tyrosine Kinase

doi: 10.1016/j.biochi.2014.01.011

Figure Lengend Snippet: Far-UV CD spectra of ErbB4_PY1 (red), ErbB4_PY2 (green) and ErbB4_PY3 (blue) peptides. Note that the mean ellipticity, [θ], was calculated using Eq [3].

Article Snippet: Peptide synthesis 12-mer wildtype and mutant peptides spanning various PPXY motifs within the ICD of human ErbB4 were commercially obtained from GenScript Corporation.

Techniques: Circular Dichroism

Structural models of WW1 (a) and WW2 (b) domains of YAP2 in complex with ErbB4_PY3 peptide containing the PPXY motif. The β-strands in the WW domains are shown in blue with loops depicted in gray and the peptide is colored yellow. Note that two orientations related by a 90°-rotation about the horizontal axis are depicted for the inquisitive eye. The sidechain moieties of all residues, including the PPXY motif (which corresponds to P0, P+1 and Y+3), within the bound peptide are shown in green. For the WW domains, the sidechain moieties colored in red denote all residues pointing toward the peptide on the concave side.

Journal: Biochimie

Article Title: Molecular Basis of the Binding of YAP Transcriptional Regulator to the ErbB4 Receptor Tyrosine Kinase

doi: 10.1016/j.biochi.2014.01.011

Figure Lengend Snippet: Structural models of WW1 (a) and WW2 (b) domains of YAP2 in complex with ErbB4_PY3 peptide containing the PPXY motif. The β-strands in the WW domains are shown in blue with loops depicted in gray and the peptide is colored yellow. Note that two orientations related by a 90°-rotation about the horizontal axis are depicted for the inquisitive eye. The sidechain moieties of all residues, including the PPXY motif (which corresponds to P0, P+1 and Y+3), within the bound peptide are shown in green. For the WW domains, the sidechain moieties colored in red denote all residues pointing toward the peptide on the concave side.

Article Snippet: Peptide synthesis 12-mer wildtype and mutant peptides spanning various PPXY motifs within the ICD of human ErbB4 were commercially obtained from GenScript Corporation.

Techniques:

Conformational dynamics as probed through MD simulations conducted on WW1 and WW2 domains of YAP2 in complex with ErbB4_PY3 peptide containing the PPXY motif. (a) RMSD of backbone atoms (N, Cα and C) within each simulated structure relative to the initial modeled structure of WW1 (top panel) and WW2 (bottom panel) domains in complex with ErbB4_PY3 peptide as a function of simulation time. Note that the overall RMSD for each WW-peptide complex (black) is deconvoluted into the WW domain alone (red) and the peptide alone (green). (b) RMSF of backbone atoms (N, Cα and C) averaged over the entire course of corresponding MD trajectory of WW1 (top panel) and WW2 (bottom panel) domains in complex with ErbB4_PY3 peptide as a function of residue number within each WW domain. The shaded vertical rectangular boxes denote residues located within the β1-β2 and β2-β3 loops. (c) RMSF of backbone atoms (N, Cα and C) averaged over the entire course of corresponding MD trajectory of WW1 (top panel) and WW2 (bottom panel) domains in complex with ErbB4_PY3 peptide as a function of residue number within the peptide (see Figure 1a for nomenclature). The PPXY motif and the flanking residues are overlayed for reference.

Journal: Biochimie

Article Title: Molecular Basis of the Binding of YAP Transcriptional Regulator to the ErbB4 Receptor Tyrosine Kinase

doi: 10.1016/j.biochi.2014.01.011

Figure Lengend Snippet: Conformational dynamics as probed through MD simulations conducted on WW1 and WW2 domains of YAP2 in complex with ErbB4_PY3 peptide containing the PPXY motif. (a) RMSD of backbone atoms (N, Cα and C) within each simulated structure relative to the initial modeled structure of WW1 (top panel) and WW2 (bottom panel) domains in complex with ErbB4_PY3 peptide as a function of simulation time. Note that the overall RMSD for each WW-peptide complex (black) is deconvoluted into the WW domain alone (red) and the peptide alone (green). (b) RMSF of backbone atoms (N, Cα and C) averaged over the entire course of corresponding MD trajectory of WW1 (top panel) and WW2 (bottom panel) domains in complex with ErbB4_PY3 peptide as a function of residue number within each WW domain. The shaded vertical rectangular boxes denote residues located within the β1-β2 and β2-β3 loops. (c) RMSF of backbone atoms (N, Cα and C) averaged over the entire course of corresponding MD trajectory of WW1 (top panel) and WW2 (bottom panel) domains in complex with ErbB4_PY3 peptide as a function of residue number within the peptide (see Figure 1a for nomenclature). The PPXY motif and the flanking residues are overlayed for reference.

Article Snippet: Peptide synthesis 12-mer wildtype and mutant peptides spanning various PPXY motifs within the ICD of human ErbB4 were commercially obtained from GenScript Corporation.

Techniques: Residue

Intermolecular distances, as probed through MD simulations, between consensus residues within the PPXY motif of ErbB4_PY3 peptide and residues lining the binding groove within WW1 and WW2 domains of YAP2. (a) Distance between Cγ pyrrolidine carbon of P0 within the PPXY motif and Nε1 indole nitrogens of W199 and W258 located respectively within WW1 (top panel) and WW2 (bottom panel) domains. (b) Distance between Cγ pyrrolidine carbon of P+1 within the PPXY motif and Cζ phenolic carbons of Y188 and Y247 located respectively within WW1 (top panel) and WW2 (bottom panel) domains. (c) Distance between Oη phenolic oxygen of Y+3 within the PPXY motif and Nδ1 imidazole nitrogens of H192 and H251 located respectively within WW1 (top panel) and WW2 (bottom panel) domains.

Journal: Biochimie

Article Title: Molecular Basis of the Binding of YAP Transcriptional Regulator to the ErbB4 Receptor Tyrosine Kinase

doi: 10.1016/j.biochi.2014.01.011

Figure Lengend Snippet: Intermolecular distances, as probed through MD simulations, between consensus residues within the PPXY motif of ErbB4_PY3 peptide and residues lining the binding groove within WW1 and WW2 domains of YAP2. (a) Distance between Cγ pyrrolidine carbon of P0 within the PPXY motif and Nε1 indole nitrogens of W199 and W258 located respectively within WW1 (top panel) and WW2 (bottom panel) domains. (b) Distance between Cγ pyrrolidine carbon of P+1 within the PPXY motif and Cζ phenolic carbons of Y188 and Y247 located respectively within WW1 (top panel) and WW2 (bottom panel) domains. (c) Distance between Oη phenolic oxygen of Y+3 within the PPXY motif and Nδ1 imidazole nitrogens of H192 and H251 located respectively within WW1 (top panel) and WW2 (bottom panel) domains.

Article Snippet: Peptide synthesis 12-mer wildtype and mutant peptides spanning various PPXY motifs within the ICD of human ErbB4 were commercially obtained from GenScript Corporation.

Techniques: Binding Assay

Intermolecular distances, as probed through MD simulations, between residues flanking the PPXY motif of ErbB4_PY3 peptide and residues lining the binding groove within WW1 and WW2 domains of YAP2. (a) Distance between Cγ1/Cγ2 methyl carbons of V-3 within the PPXY motif and Cδ1/Cδ2 indole carbons of W199 and W258 located respectively within WW1 (top panel) and WW2 (bottom panel) domains. (b) Distance between Cδ1/Cδ2 methyl carbons of L-2 within the PPXY motif and Cδ carbons of Q186 and E245 located respectively within WW1 (top panel) and WW2 (bottom panel) domains. (c) Distance between Nη1/Nη2 guanidine nitrogens of R+6 within the PPXY motif and Oε1/Oε2 carbonyl oxygens of E178 and E237 located respectively within WW1 (top panel) and WW2 (bottom panel) domains.

Journal: Biochimie

Article Title: Molecular Basis of the Binding of YAP Transcriptional Regulator to the ErbB4 Receptor Tyrosine Kinase

doi: 10.1016/j.biochi.2014.01.011

Figure Lengend Snippet: Intermolecular distances, as probed through MD simulations, between residues flanking the PPXY motif of ErbB4_PY3 peptide and residues lining the binding groove within WW1 and WW2 domains of YAP2. (a) Distance between Cγ1/Cγ2 methyl carbons of V-3 within the PPXY motif and Cδ1/Cδ2 indole carbons of W199 and W258 located respectively within WW1 (top panel) and WW2 (bottom panel) domains. (b) Distance between Cδ1/Cδ2 methyl carbons of L-2 within the PPXY motif and Cδ carbons of Q186 and E245 located respectively within WW1 (top panel) and WW2 (bottom panel) domains. (c) Distance between Nη1/Nη2 guanidine nitrogens of R+6 within the PPXY motif and Oε1/Oε2 carbonyl oxygens of E178 and E237 located respectively within WW1 (top panel) and WW2 (bottom panel) domains.

Article Snippet: Peptide synthesis 12-mer wildtype and mutant peptides spanning various PPXY motifs within the ICD of human ErbB4 were commercially obtained from GenScript Corporation.

Techniques: Binding Assay