P33151

Author

Hamed Khakzad

Published

August 10, 2024

General information

Code 
import requests
import urllib3
urllib3.disable_warnings()

def fetch_uniprot_data(uniprot_id):
    url = f"https://rest.uniprot.org/uniprotkb/{uniprot_id}.json"
    response = requests.get(url, verify=False)  # Disable SSL verification
    response.raise_for_status()  # Raise an error for bad status codes
    return response.json()

def display_uniprot_data(data):
    primary_accession = data.get('primaryAccession', 'N/A')
    protein_name = data.get('proteinDescription', {}).get('recommendedName', {}).get('fullName', {}).get('value', 'N/A')
    gene_name = data.get('gene', [{'geneName': {'value': 'N/A'}}])[0]['geneName']['value']
    organism = data.get('organism', {}).get('scientificName', 'N/A')
    
    function_comment = next((comment for comment in data.get('comments', []) if comment['commentType'] == "FUNCTION"), None)
    function = function_comment['texts'][0]['value'] if function_comment else 'N/A'

    # Printing the data
    print(f"UniProt ID: {primary_accession}")
    print(f"Protein Name: {protein_name}")
    print(f"Organism: {organism}")
    print(f"Function: {function}")

# Replace this with the UniProt ID you want to fetch
uniprot_id = "P33151"
data = fetch_uniprot_data(uniprot_id)
display_uniprot_data(data)
UniProt ID: P33151
Protein Name: Cadherin-5
Organism: Homo sapiens
Function: Cadherins are calcium-dependent cell adhesion proteins (By similarity). They preferentially interact with themselves in a homophilic manner in connecting cells; cadherins may thus contribute to the sorting of heterogeneous cell types (PubMed:21269602). This cadherin may play a important role in endothelial cell biology through control of the cohesion and organization of the intercellular junctions (By similarity). It associates with alpha-catenin forming a link to the cytoskeleton (PubMed:10861224). Acts in concert with KRIT1 and PALS1 to establish and maintain correct endothelial cell polarity and vascular lumen (By similarity). These effects are mediated by recruitment and activation of the Par polarity complex and RAP1B (PubMed:20332120). Required for activation of PRKCZ and for the localization of phosphorylated PRKCZ, PARD3, TIAM1 and RAP1B to the cell junction (PubMed:20332120)

More information:   

AlphaFold model

Surface representation - binding sites

The computed point cloud for pLDDT > 0.6. Each atom is sampled on average by 10 points.

To see the predicted binding interfaces, you can choose color theme “uncertainty”.

  • Go to the “Controls Panel”

  • Below “Components”, to the right, click on “…”

  • “Set Coloring” by “Atom Property”, and “Uncertainty/Disorder”

All detected seeds aligned

Seed scores per sites

Code 
import re
import pandas as pd
import os
import plotly.express as px

ID = "P33151"
data_list = []

name_pattern = re.compile(r'name: (\S+)')
score_pattern = re.compile(r'score: (\d+\.\d+)')
desc_dist_score_pattern = re.compile(r'desc_dist_score: (\d+\.\d+)')

directory = f"/Users/hamedkhakzad/Research_EPFL/1_postdoc_project/Surfaceome_web_app/www/Surfaceome_top100_per_site/{ID}_A"

for filename in os.listdir(directory):
    if filename.startswith("output_sorted_") and filename.endswith(".score"):
        filepath = os.path.join(directory, filename)
        with open(filepath, 'r') as file:
            for line in file:
                name_match = name_pattern.search(line)
                score_match = score_pattern.search(line)
                desc_dist_score_match = desc_dist_score_pattern.search(line)
                
                if name_match and score_match and desc_dist_score_match:
                    name = name_match.group(1)
                    score = float(score_match.group(1))
                    desc_dist_score = float(desc_dist_score_match.group(1))
                    
                    simple_filename = filename.replace("output_sorted_", "").replace(".score", "")
                    data_list.append({
                        'name': name[:-1],
                        'score': score,
                        'desc_dist_score': desc_dist_score,
                        'file': simple_filename
                    })

data = pd.DataFrame(data_list)

fig = px.scatter(
    data,
    x='score',
    y='desc_dist_score',
    color='file',
    title='Score vs Desc Dist Score',
    labels={'score': 'Score', 'desc_dist_score': 'Desc Dist Score'},
    hover_data={'name': True}
)

fig.update_layout(
    legend_title_text='File',
    legend=dict(
        yanchor="top",
        y=0.99,
        xanchor="left",
        x=1.05
    )
)

fig.show()

Binding site metrics

Code 
import pandas as pd
pd.options.mode.chained_assignment = None
import plotly.express as px

df_total = pd.read_csv('/Users/hamedkhakzad/Research_EPFL/1_postdoc_project/Surfaceome_web_app/www/database/df_flattened.csv')
df_plot = df_total[df_total['acc_flat'] == ID]
df_plot ['Total seeds'] = df_plot.loc[:,['seedss_a','seedss_b']].sum(axis=1)
df_plot.loc[:, ["acc_flat", "main_classs", "sub_classs", "seedss_a", "seedss_b", "areass", "bsss", "hpss"]]
acc_flat main_classs sub_classs seedss_a seedss_b areass bsss hpss
559 P33151 Miscellaneous StructuralAndAdhesion 5 61 1264.842242 553 -9.59990
560 P33151 Miscellaneous StructuralAndAdhesion 19 48 3678.972161 466 -32.50000
561 P33151 Miscellaneous StructuralAndAdhesion 304 83 1365.831453 760 7.39999
Code 
import math
import matplotlib.pyplot as plt

features = ['seedss_a', 'seedss_b', 'areass', 'hpss']
titles = ['Alpha seeds', 'Beta seeds', 'Area', 'Hydrophobicity']
num_features = len(features)

if len(df_plot) > 8:
    num_rows = 2
    num_cols = 2
else:
    num_rows = 1
    num_cols = 4

fig, axes = plt.subplots(nrows=num_rows, ncols=num_cols, figsize=(9, num_rows * 5))

axes = axes.flatten()
positions = range(1, len(df_plot) + 1)

for i, feature in enumerate(features):
    title = titles[i]
    axes[i].bar(positions, df_plot[feature], color=['blue', 'orange', 'green', 'red', 'purple', 'brown'])
    axes[i].set_title(title, fontsize=13)
    axes[i].set_xticks(positions)
    axes[i].set_xticklabels(df_plot['bsss'], rotation=90)
    axes[i].set_xlabel("Center residues", fontsize=13)
    axes[i].set_ylabel(title, fontsize=13)

for j in range(len(features), len(axes)):
    fig.delaxes(axes[j])

plt.tight_layout()
plt.show()

Binding site sequence composition

Code 
amino_acid_map = {
    'ALA': 'A', 'ARG': 'R', 'ASN': 'N', 'ASP': 'D', 'CYS': 'C',
    'GLN': 'Q', 'GLU': 'E', 'GLY': 'G', 'HIS': 'H', 'ILE': 'I',
    'LEU': 'L', 'LYS': 'K', 'MET': 'M', 'PHE': 'F', 'PRO': 'P',
    'SER': 'S', 'THR': 'T', 'TRP': 'W', 'TYR': 'Y', 'VAL': 'V'
}

from collections import Counter
from ast import literal_eval
from matplotlib.gridspec import GridSpec
import warnings
warnings.filterwarnings("ignore", message="Attempting to set identical low and high xlims")

def convert_to_single_letter(aa_list):
    if type(aa_list) == str:
        aa_list = literal_eval(aa_list)
    return [amino_acid_map[aa] for aa in aa_list]

def create_sequence_visualizations(df, max_letters_per_row=20):
    for idx, row in df.iterrows():
        bsss = row['bsss']
        AAss = row['AAss']
        single_letter_sequence = convert_to_single_letter(AAss)
        
        freq_counter = Counter(single_letter_sequence)
        total_aa = len(single_letter_sequence)
        frequencies = {aa: freq / total_aa for aa, freq in freq_counter.items()}
        
        cmap = plt.get_cmap('viridis')
        norm = plt.Normalize(0, max(frequencies.values()) if frequencies else 1)
        
        n_rows = (len(single_letter_sequence) + max_letters_per_row - 1) // max_letters_per_row
        fig = plt.figure(figsize=(max_letters_per_row * 0.6, n_rows * 1.2 + 0.5))
        
        gs = GridSpec(n_rows + 1, 1, height_ratios=[1] * n_rows + [0.1], hspace=0.3)
        
        for row_idx in range(n_rows):
            start_idx = row_idx * max_letters_per_row
            end_idx = min((row_idx + 1) * max_letters_per_row, len(single_letter_sequence))
            ax = fig.add_subplot(gs[row_idx, 0])
            ax.set_xlim(0, max_letters_per_row)
            ax.set_ylim(0, 1)
            ax.axis('off')
            
            for i, aa in enumerate(single_letter_sequence[start_idx:end_idx]):
                freq = frequencies[aa]
                color = cmap(norm(freq))
                ax.text(i + 0.5, 0.5, aa, ha='center', va='center', fontsize=24, color=color, fontweight='bold')
        
        cbar_ax = fig.add_subplot(gs[-1, 0])
        sm = plt.cm.ScalarMappable(cmap=cmap, norm=norm)
        sm.set_array([])
        cbar = plt.colorbar(sm, cax=cbar_ax, orientation='horizontal')
        cbar.set_label('Frequency', fontsize=12)
        cbar.ax.tick_params(labelsize=12)
        
        plt.suptitle(f"Center residue {bsss}", fontsize=14)
        plt.subplots_adjust(left=0.1, right=0.9, top=0.9, bottom=0.1)
        plt.show()
            
create_sequence_visualizations(df_plot)

Download

To download all the seeds and score files for this entry Click Here!