ReddRadar
Agent skill
bio-epidemiological-genomics-pathogen-typing
Perform multi-locus sequence typing (MLST), core genome MLST, and SNP-based strain typing for bacterial isolate characterization using mlst and chewBBACA. Use when identifying strain types, tracking outbreak clones, or characterizing bacterial isolates.
Install this agent skill to your Project
npx add-skill https://github.com/FreedomIntelligence/OpenClaw-Medical-Skills/tree/main/skills/bio-epidemiological-genomics-pathogen-typing
SKILL.md
Version Compatibility
Reference examples tested with: mlst 2.23+, numpy 1.26+, pandas 2.2+, scanpy 1.10+, scipy 1.12+
Before using code patterns, verify installed versions match. If versions differ:
- Python:
pip show <package>thenhelp(module.function)to check signatures - CLI:
<tool> --versionthen<tool> --helpto confirm flags
If code throws ImportError, AttributeError, or TypeError, introspect the installed package and adapt the example to match the actual API rather than retrying.
Pathogen Typing
"Type my bacterial isolates by MLST" → Assign multi-locus sequence types to bacterial genomes for isolate characterization, outbreak clone identification, and strain tracking.
- CLI:
mlst assembly.fastafor 7-gene MLST typing - CLI:
chewBBACA.py AlleleCallfor core genome MLST (cgMLST)
MLST with mlst Tool
# Install mlst
conda install -c bioconda mlst
# Basic MLST typing
mlst genome.fasta
# Output: genome.fasta ecoli ST131 adk(53) fumC(40) gyrB(47) ...
# Batch typing
mlst *.fasta > typing_results.tsv
# Specify scheme
mlst --scheme senterica genome.fasta
# List available schemes
mlst --list
# Include allele sequences in output
mlst --csv genome.fasta > results.csv
Parse MLST Results
import pandas as pd
import subprocess
def run_mlst(fasta_files, scheme=None):
'''Run MLST on multiple genomes
Returns DataFrame with:
- Sample name
- Scheme (auto-detected or specified)
- Sequence type (ST)
- Allele profiles
ST interpretation:
- Known ST: Matches existing type in database
- Novel allele: New allele combination, may be unreported ST
- Failed: Unable to determine (poor assembly or wrong scheme)
'''
cmd = ['mlst'] + fasta_files
if scheme:
cmd.extend(['--scheme', scheme])
result = subprocess.run(cmd, capture_output=True, text=True)
lines = result.stdout.strip().split('\n')
data = [line.split('\t') for line in lines]
return pd.DataFrame(data, columns=['file', 'scheme', 'ST'] +
[f'locus{i}' for i in range(1, len(data[0])-2)])
Core Genome MLST (cgMLST)
# chewBBACA for cgMLST
pip install chewbbaca
# Download or create schema
chewBBACA.py DownloadSchema -sp "Salmonella enterica" -o schema_dir
# Run cgMLST
chewBBACA.py AlleleCall -i genomes/ -g schema_dir -o results/
# Analyze results
chewBBACA.py ExtractCgMLST -i results/results_alleles.tsv \
-o cgmlst_results.tsv --threshold 0.95
cgMLST Distance Analysis
Goal: Compute pairwise allelic distances between isolates and cluster them to identify potential outbreak groups.
Approach: Count allelic differences between each pair of isolate profiles (ignoring missing data), then apply single-linkage hierarchical clustering with a pathogen-specific distance threshold.
import pandas as pd
import numpy as np
def calculate_cgmlst_distance(profiles):
'''Calculate allelic distances between isolates
Distance interpretation (typical thresholds):
- 0-5 allele differences: Same cluster (likely recent transmission)
- 6-15 differences: Related (possible epidemiological link)
- >15 differences: Different clones
Note: Thresholds are pathogen-specific. Consult literature.
'''
n = len(profiles)
distances = np.zeros((n, n))
for i in range(n):
for j in range(i+1, n):
# Count allelic differences (excluding missing data)
diff = sum(1 for a, b in zip(profiles.iloc[i], profiles.iloc[j])
if a != b and a != 0 and b != 0)
distances[i, j] = distances[j, i] = diff
return pd.DataFrame(distances, index=profiles.index, columns=profiles.index)
def identify_clusters(distance_matrix, threshold=5):
'''Identify cgMLST clusters
Threshold values by organism:
- E. coli: 10 alleles
- Salmonella: 7 alleles
- Listeria: 7 alleles
- S. aureus: 24 alleles
'''
from scipy.cluster.hierarchy import linkage, fcluster
# Convert to condensed distance matrix
condensed = distance_matrix.values[np.triu_indices(len(distance_matrix), k=1)]
# Hierarchical clustering
Z = linkage(condensed, method='single')
clusters = fcluster(Z, t=threshold, criterion='distance')
return dict(zip(distance_matrix.index, clusters))
SNP-Based Typing
def snp_typing_from_vcf(vcf_file, reference_positions):
'''Extract SNP profile for typing
Some organisms use canonical SNP positions for typing
(e.g., Mycobacterium tuberculosis lineages)
'''
from cyvcf2 import VCF
vcf = VCF(vcf_file)
profile = {}
for pos in reference_positions:
chrom, position = pos.split(':')
for variant in vcf(f'{chrom}:{position}-{position}'):
profile[pos] = variant.ALT[0] if variant.ALT else variant.REF
return profile
Enterobase Integration
import requests
def query_enterobase(st, organism='ecoli'):
'''Query Enterobase for ST metadata
Enterobase provides:
- Geographic distribution
- Temporal trends
- Associated serotypes
- Virulence gene profiles
'''
# Note: Requires API token
url = f'https://enterobase.warwick.ac.uk/api/v2.0/{organism}/sts/{st}'
# Would need authentication headers
# response = requests.get(url, headers={'Authorization': f'Bearer {token}'})
print(f'Query Enterobase for ST{st}: {url}')
return None # Placeholder - requires authentication
Related Skills
- epidemiological-genomics/phylodynamics - Time-scaled trees from typed isolates
- epidemiological-genomics/transmission-inference - Outbreak investigation
- metagenomics/kraken-classification - Species identification
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