Datasets:

Liu-Hy
/

GenoTEX

	# Path Configuration
	from tools.preprocess import *

	# Processing context
	trait = "Intellectual_Disability"
	cohort = "GSE89594"

	# Input paths
	in_trait_dir = "../DATA/GEO/Intellectual_Disability"
	in_cohort_dir = "../DATA/GEO/Intellectual_Disability/GSE89594"

	# Output paths
	out_data_file = "./output/preprocess/3/Intellectual_Disability/GSE89594.csv"
	out_gene_data_file = "./output/preprocess/3/Intellectual_Disability/gene_data/GSE89594.csv"
	out_clinical_data_file = "./output/preprocess/3/Intellectual_Disability/clinical_data/GSE89594.csv"
	json_path = "./output/preprocess/3/Intellectual_Disability/cohort_info.json"

	# Get file paths
	soft_file_path, matrix_file_path = geo_get_relevant_filepaths(in_cohort_dir)

	# Get background info and clinical data
	background_info, clinical_data = get_background_and_clinical_data(matrix_file_path)

	# Get unique values for each clinical feature
	unique_values_dict = get_unique_values_by_row(clinical_data)

	# Print background information
	print("Background Information:")
	print(background_info)
	print("\nSample Characteristics:")
	print(json.dumps(unique_values_dict, indent=2))
	# 1. Gene Expression Data Availability
	# Based on background info, this is a gene expression study using peripheral blood
	is_gene_available = True

	# 2.1 Data Availability
	trait_row = 0 # "diagnosis" in row 0 contains trait info
	age_row = 2 # "age" in row 2
	gender_row = 3 # "gender" in row 3

	# 2.2 Data Type Conversion Functions
	def convert_trait(x):
	"""Convert trait status to binary"""
	if not isinstance(x, str):
	return None
	value = x.split(': ')[-1].lower()
	# Williams Syndrome is intellectual disability
	if 'williams syndrome' in value or 'ws' in value:
	return 1
	elif 'control' in value:
	return 0
	# ASD samples counted as None since not relevant
	return None

	def convert_age(x):
	"""Convert age to continuous values"""
	if not isinstance(x, str):
	return None
	value = x.split(': ')[-1].lower()
	try:
	# Extract numeric value before 'y'
	return float(value.replace('y',''))
	except:
	return None

	def convert_gender(x):
	"""Convert gender to binary (0=female, 1=male)"""
	if not isinstance(x, str):
	return None
	value = x.split(': ')[-1].lower()
	if 'female' in value:
	return 0
	elif 'male' in value:
	return 1
	return None

	# 3. Save Metadata
	is_trait_available = trait_row is not None
	validate_and_save_cohort_info(is_final=False,
	cohort=cohort,
	info_path=json_path,
	is_gene_available=is_gene_available,
	is_trait_available=is_trait_available)

	# 4. Clinical Feature Extraction
	if trait_row is not None:
	clinical_features = geo_select_clinical_features(
	clinical_df=clinical_data,
	trait=trait,
	trait_row=trait_row,
	convert_trait=convert_trait,
	age_row=age_row,
	convert_age=convert_age,
	gender_row=gender_row,
	convert_gender=convert_gender
	)

	# Preview the processed clinical data
	preview = preview_df(clinical_features)
	print("Preview of processed clinical data:")
	print(preview)

	# Save clinical features
	clinical_features.to_csv(out_clinical_data_file)
	# Extract gene expression data from the matrix file
	genetic_data = get_genetic_data(matrix_file_path)

	# Print first 20 row IDs
	print("First 20 row IDs:")
	print(genetic_data.index[:20].tolist())
	# Based on the provided sample row IDs which are just sequential numbers,
	# we need to map these identifiers to proper gene symbols
	requires_gene_mapping = True
	# Extract gene annotation data from SOFT file
	gene_metadata = get_gene_annotation(soft_file_path)

	# Display information about the annotation data
	print("Column names:")
	print(gene_metadata.columns.tolist())

	# Look at general data statistics
	print("\nData shape:", gene_metadata.shape)

	# Display non-NaN value counts for key gene identifier columns
	print("\nNumber of non-NaN values in key columns:")
	for col in ['ID', 'GENE_SYMBOL']:
	print(f"{col}: {gene_metadata[col].notna().sum()}")

	# Preview rows with actual gene information
	print("\nPreview of rows with gene information:")
	gene_rows = gene_metadata[gene_metadata['GENE_SYMBOL'].notna()].head()
	print(json.dumps(preview_df(gene_rows), indent=2))
	# 1. Identify mapping columns
	# ID in expression data corresponds to ID in annotation
	# GENE_SYMBOL contains gene symbols for mapping
	mapping_df = get_gene_mapping(gene_metadata, prob_col='ID', gene_col='GENE_SYMBOL')

	# 2. Apply mapping and aggregate to get gene expression data
	gene_data = apply_gene_mapping(genetic_data, mapping_df)

	# Preview the processed data
	print("\nPreview of mapped gene expression data:")
	print(f"Shape: {gene_data.shape}")
	print("\nFirst few gene symbols:")
	print(gene_data.index[:10].tolist())
	# 1. Normalize gene symbols
	gene_data = normalize_gene_symbols_in_index(gene_data)
	gene_data.to_csv(out_gene_data_file)

	# Get clinical features
	clinical_features = geo_select_clinical_features(
	clinical_data,
	trait=trait,
	trait_row=trait_row,
	convert_trait=convert_trait,
	age_row=age_row,
	convert_age=convert_age,
	gender_row=gender_row,
	convert_gender=convert_gender
	)

	# 2. Link clinical and genetic data
	linked_data = geo_link_clinical_genetic_data(clinical_features, gene_data)

	# 3. Handle missing values
	linked_data = handle_missing_values(linked_data, trait)

	# Early exit if trait values are all NaN
	if linked_data[trait].isna().all():
	is_biased = True
	linked_data = None
	else:
	# 4. Judge whether features are biased and remove biased demographic features
	is_biased, linked_data = judge_and_remove_biased_features(linked_data, trait)

	# 5. Final validation and save metadata
	note = "Dataset contains gene expression data from pediatric AML samples, focusing on Down syndrome cases versus other AML types."
	is_usable = validate_and_save_cohort_info(
	is_final=True,
	cohort=cohort,
	info_path=json_path,
	is_gene_available=True,
	is_trait_available=True,
	is_biased=is_biased,
	df=linked_data,
	note=note
	)

	# 6. Save the linked data only if it's usable
	if is_usable:
	os.makedirs(os.path.dirname(out_data_file), exist_ok=True)
	linked_data.to_csv(out_data_file)