install
source · Clone the upstream repo
git clone https://github.com/mdbabumiamssm/LLMs-Universal-Life-Science-and-Clinical-Skills-
Claude Code · Install into ~/.claude/skills/
T=$(mktemp -d) && git clone --depth=1 https://github.com/mdbabumiamssm/LLMs-Universal-Life-Science-and-Clinical-Skills- "$T" && mkdir -p ~/.claude/skills && cp -r "$T/Skills/3D_Genomics/hi-c-analysis/hic-differential" ~/.claude/skills/mdbabumiamssm-llms-universal-life-science-and-clinical-skills-hic-differential && rm -rf "$T"
manifest:
Skills/3D_Genomics/hi-c-analysis/hic-differential/SKILL.mdsource content
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name: bio-hi-c-analysis-hic-differential description: Compare Hi-C contact matrices between conditions to identify differential chromatin interactions. Compute log2 fold changes, statistical significance, and visualize differential contact maps. Use when comparing Hi-C contacts between conditions. tool_type: python primary_tool: cooltools measurable_outcome: Execute skill workflow successfully with valid output within 15 minutes. allowed-tools:
- read_file
- run_shell_command
Hi-C Differential Analysis
Compare Hi-C contact matrices between conditions.
Required Imports
import cooler import cooltools import numpy as np import pandas as pd import matplotlib.pyplot as plt from matplotlib.colors import TwoSlopeNorm from scipy import stats import bioframe
Load Two Conditions
# Load balanced cooler files at same resolution clr1 = cooler.Cooler('condition1.mcool::resolutions/10000') clr2 = cooler.Cooler('condition2.mcool::resolutions/10000') print(f'Condition 1: {clr1.info["sum"]:,} contacts') print(f'Condition 2: {clr2.info["sum"]:,} contacts')
Compute Log2 Fold Change
def log2_fold_change(clr1, clr2, region, pseudocount=1): '''Compute log2(condition2/condition1) for a region''' mat1 = clr1.matrix(balance=True).fetch(region) mat2 = clr2.matrix(balance=True).fetch(region) # Add pseudocount and compute log2 ratio log2fc = np.log2((mat2 + pseudocount) / (mat1 + pseudocount)) log2fc[np.isinf(log2fc)] = np.nan return log2fc region = 'chr1:50000000-60000000' log2fc = log2_fold_change(clr1, clr2, region) print(f'Log2FC range: {np.nanmin(log2fc):.2f} to {np.nanmax(log2fc):.2f}')
Plot Differential Contact Map
fig, axes = plt.subplots(1, 3, figsize=(15, 5)) # Condition 1 mat1 = clr1.matrix(balance=True).fetch(region) im1 = axes[0].imshow(np.log2(mat1 + 1), cmap='Reds', vmin=-10, vmax=-3) axes[0].set_title('Condition 1') plt.colorbar(im1, ax=axes[0]) # Condition 2 mat2 = clr2.matrix(balance=True).fetch(region) im2 = axes[1].imshow(np.log2(mat2 + 1), cmap='Reds', vmin=-10, vmax=-3) axes[1].set_title('Condition 2') plt.colorbar(im2, ax=axes[1]) # Log2 fold change (diverging colormap) norm = TwoSlopeNorm(vmin=-2, vcenter=0, vmax=2) im3 = axes[2].imshow(log2fc, cmap='coolwarm', norm=norm) axes[2].set_title('Log2(Cond2/Cond1)') plt.colorbar(im3, ax=axes[2]) plt.tight_layout() plt.savefig('differential_hic.png', dpi=150)
Split View Comparison
def plot_split_view(mat1, mat2, title=''): '''Upper triangle: condition1, Lower triangle: condition2''' combined = np.triu(mat1) + np.tril(mat2, k=-1) fig, ax = plt.subplots(figsize=(8, 8)) im = ax.imshow(np.log2(combined + 1), cmap='Reds', vmin=-10, vmax=-3) ax.axline((0, 0), slope=1, color='black', linewidth=0.5) ax.set_title(f'{title}\nUpper: Cond1, Lower: Cond2') plt.colorbar(im, ax=ax) return fig mat1 = clr1.matrix(balance=True).fetch(region) mat2 = clr2.matrix(balance=True).fetch(region) fig = plot_split_view(mat1, mat2) plt.savefig('split_view.png', dpi=150)
Depth Normalization
def depth_normalize(clr, target_depth=None): '''Normalize matrix to target sequencing depth''' total = clr.info['sum'] if target_depth is None: return 1.0 return target_depth / total # Normalize both samples to same depth target = min(clr1.info['sum'], clr2.info['sum']) scale1 = depth_normalize(clr1, target) scale2 = depth_normalize(clr2, target) mat1_norm = clr1.matrix(balance=True).fetch(region) * scale1 mat2_norm = clr2.matrix(balance=True).fetch(region) * scale2
Statistical Testing (Per-Pixel)
def differential_test(matrices1, matrices2, method='ttest'): ''' Test for differential contacts between replicates. matrices1/2: lists of numpy arrays (replicates) ''' n1, n2 = len(matrices1), len(matrices2) shape = matrices1[0].shape pvalues = np.ones(shape) log2fc = np.zeros(shape) for i in range(shape[0]): for j in range(shape[1]): vals1 = [m[i, j] for m in matrices1 if not np.isnan(m[i, j])] vals2 = [m[i, j] for m in matrices2 if not np.isnan(m[i, j])] if len(vals1) >= 2 and len(vals2) >= 2: if method == 'ttest': _, p = stats.ttest_ind(vals1, vals2) elif method == 'mannwhitneyu': _, p = stats.mannwhitneyu(vals1, vals2, alternative='two-sided') pvalues[i, j] = p log2fc[i, j] = np.log2((np.mean(vals2) + 1) / (np.mean(vals1) + 1)) return log2fc, pvalues # Example with replicates rep1_cond1 = [clr.matrix(balance=True).fetch(region) for clr in condition1_reps] rep1_cond2 = [clr.matrix(balance=True).fetch(region) for clr in condition2_reps] log2fc, pvalues = differential_test(rep1_cond1, rep1_cond2)
FDR Correction
from statsmodels.stats.multitest import multipletests # Flatten p-values, apply FDR pval_flat = pvalues.flatten() valid_mask = ~np.isnan(pval_flat) pval_valid = pval_flat[valid_mask] _, pval_adj, _, _ = multipletests(pval_valid, method='fdr_bh') # Reshape back pval_adj_full = np.full_like(pval_flat, np.nan) pval_adj_full[valid_mask] = pval_adj pvalues_adj = pval_adj_full.reshape(pvalues.shape) # Significant differential contacts sig_mask = (pvalues_adj < 0.05) & (np.abs(log2fc) > 1) print(f'Significant differential contacts: {sig_mask.sum()}')
Differential at Distance Bins
def differential_by_distance(log2fc_matrix, max_dist=100): '''Summarize differential contacts by genomic distance''' n = log2fc_matrix.shape[0] results = [] for d in range(max_dist): diag = np.diag(log2fc_matrix, d) valid = diag[~np.isnan(diag)] if len(valid) > 0: results.append({ 'distance': d, 'mean_log2fc': np.mean(valid), 'std_log2fc': np.std(valid), 'n_contacts': len(valid), }) return pd.DataFrame(results) dist_df = differential_by_distance(log2fc) plt.figure(figsize=(10, 4)) plt.errorbar(dist_df['distance'], dist_df['mean_log2fc'], yerr=dist_df['std_log2fc']/np.sqrt(dist_df['n_contacts']), alpha=0.5) plt.axhline(0, color='black', linestyle='--') plt.xlabel('Distance (bins)') plt.ylabel('Mean log2 fold change') plt.title('Differential contacts by distance') plt.savefig('differential_by_distance.png', dpi=150)
Compare Compartment Changes
# Load compartment eigenvectors view_df = bioframe.make_viewframe(clr1.chromsizes) _, eig1 = cooltools.eigs_cis(clr1, view_df=view_df, n_eigs=1) _, eig2 = cooltools.eigs_cis(clr2, view_df=view_df, n_eigs=1) # Merge and find switches merged = eig1.merge(eig2, on=['chrom', 'start', 'end'], suffixes=('_1', '_2')) merged['E1_diff'] = merged['E1_2'] - merged['E1_1'] merged['compartment_1'] = np.where(merged['E1_1'] > 0, 'A', 'B') merged['compartment_2'] = np.where(merged['E1_2'] > 0, 'A', 'B') merged['switched'] = merged['compartment_1'] != merged['compartment_2'] print(f"Compartment switches: {merged['switched'].sum()}") print(merged[merged['switched']][['chrom', 'start', 'end', 'E1_1', 'E1_2']].head(10))
Compare TAD Boundaries
# Compute insulation for both ins1 = cooltools.insulation(clr1, window_bp=[200000], ignore_diags=2) ins2 = cooltools.insulation(clr2, window_bp=[200000], ignore_diags=2) # Get boundaries bounds1 = set(ins1[ins1['is_boundary_200000']]['start']) bounds2 = set(ins2[ins2['is_boundary_200000']]['start']) shared = bounds1 & bounds2 only_cond1 = bounds1 - bounds2 only_cond2 = bounds2 - bounds1 print(f'Shared boundaries: {len(shared)}') print(f'Condition 1 specific: {len(only_cond1)}') print(f'Condition 2 specific: {len(only_cond2)}')
Differential Loop Analysis
# Call loops in both conditions dots1 = cooltools.dots(clr1, expected=expected1, view_df=view_df, max_loci_separation=2000000) dots2 = cooltools.dots(clr2, expected=expected2, view_df=view_df, max_loci_separation=2000000) def loops_overlap(l1, l2, tolerance=20000): return (l1['chrom1'] == l2['chrom1'] and abs(l1['start1'] - l2['start1']) < tolerance and abs(l1['start2'] - l2['start2']) < tolerance) # Find differential loops shared_loops = [] cond1_specific = [] for _, l1 in dots1.iterrows(): found = False for _, l2 in dots2.iterrows(): if loops_overlap(l1, l2): shared_loops.append(l1) found = True break if not found: cond1_specific.append(l1) print(f'Shared loops: {len(shared_loops)}') print(f'Condition 1 specific: {len(cond1_specific)}')
Export Differential Results
# Save log2FC matrix np.save('log2fc_matrix.npy', log2fc) # Save significant differential contacts as BED-like sig_contacts = [] for i in range(log2fc.shape[0]): for j in range(i, log2fc.shape[1]): if sig_mask[i, j]: sig_contacts.append({ 'bin1': i, 'bin2': j, 'log2fc': log2fc[i, j], 'pvalue': pvalues_adj[i, j], }) pd.DataFrame(sig_contacts).to_csv('differential_contacts.csv', index=False) # Save compartment switches merged[merged['switched']].to_csv('compartment_switches.csv', index=False)
Related Skills
- hic-data-io - Load Hi-C matrices
- matrix-operations - Normalize matrices
- compartment-analysis - Call compartments
- tad-detection - Call TADs for comparison
- loop-calling - Call loops for comparison