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DiffLinker / app.py

igashov

handle nan values if linker size is small

c1152c1 almost 2 years ago

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	import argparse

	import gradio as gr
	import numpy as np
	import os
	import torch
	import subprocess
	import output

	from rdkit import Chem
	from src import const
	from src.visualizer import save_xyz_file
	from src.datasets import get_dataloader, collate_with_fragment_edges, parse_molecule
	from src.lightning import DDPM
	from src.linker_size_lightning import SizeClassifier

	N_SAMPLES = 5

	parser = argparse.ArgumentParser()
	parser.add_argument('--ip', type=str, default=None)
	args = parser.parse_args()

	device = torch.device("cuda" if torch.cuda.is_available() else "cpu")
	os.makedirs("results", exist_ok=True)
	os.makedirs("models", exist_ok=True)

	size_gnn_path = 'models/geom_size_gnn.ckpt'
	if not os.path.exists(size_gnn_path):
	print('Downloading SizeGNN model...')
	link = 'https://zenodo.org/record/7121300/files/geom_size_gnn.ckpt?download=1'
	subprocess.run(f'wget {link} -O {size_gnn_path}', shell=True)
	size_nn = SizeClassifier.load_from_checkpoint('models/geom_size_gnn.ckpt', map_location=device).eval().to(device)
	print('Loaded SizeGNN model')

	diffusion_path = 'models/geom_difflinker.ckpt'
	if not os.path.exists(diffusion_path):
	print('Downloading Diffusion model...')
	link = 'https://zenodo.org/record/7121300/files/geom_difflinker.ckpt?download=1'
	subprocess.run(f'wget {link} -O {diffusion_path}', shell=True)
	ddpm = DDPM.load_from_checkpoint('models/geom_difflinker.ckpt', map_location=device).eval().to(device)
	print('Loaded diffusion model')

	def read_molecule_content(path):
	with open(path, "r") as f:
	return "".join(f.readlines())


	def read_molecule(path):
	if path.endswith('.pdb'):
	return Chem.MolFromPDBFile(path, sanitize=False, removeHs=True)
	elif path.endswith('.mol'):
	return Chem.MolFromMolFile(path, sanitize=False, removeHs=True)
	elif path.endswith('.mol2'):
	return Chem.MolFromMol2File(path, sanitize=False, removeHs=True)
	elif path.endswith('.sdf'):
	return Chem.SDMolSupplier(path, sanitize=False, removeHs=True)[0]
	raise Exception('Unknown file extension')


	def show_input(input_file):
	if input_file is None:
	return ['', gr.Radio.update(visible=False, value='Sample 1')]
	if isinstance(input_file, str):
	path = input_file
	else:
	path = input_file.name
	extension = path.split('.')[-1]
	if extension not in ['sdf', 'pdb', 'mol', 'mol2']:
	msg = output.INVALID_FORMAT_MSG.format(extension=extension)
	return [
	output.IFRAME_TEMPLATE.format(html=msg),
	gr.Radio.update(visible=False)
	]

	try:
	molecule = read_molecule_content(path)
	except Exception as e:
	return [
	f'Could not read the molecule: {e}',
	gr.Radio.update(visible=False)
	]

	html = output.INITIAL_RENDERING_TEMPLATE.format(molecule=molecule, fmt=extension)
	return [
	output.IFRAME_TEMPLATE.format(html=html),
	gr.Radio.update(visible=False)
	]


	def draw_sample(idx, out_files):
	in_file = out_files[0]
	in_sdf = in_file if isinstance(in_file, str) else in_file.name

	out_file = out_files[idx + 1]
	out_sdf = out_file if isinstance(out_file, str) else out_file.name

	input_fragments_content = read_molecule_content(in_sdf)
	generated_molecule_content = read_molecule_content(out_sdf)
	html = output.SAMPLES_RENDERING_TEMPLATE.format(
	fragments=input_fragments_content,
	fragments_fmt='sdf',
	molecule=generated_molecule_content,
	molecule_fmt='sdf',
	)
	return output.IFRAME_TEMPLATE.format(html=html)


	def generate(input_file, n_steps, n_atoms):
	if input_file is None:
	return ''

	path = input_file.name
	extension = path.split('.')[-1]
	if extension not in ['sdf', 'pdb', 'mol', 'mol2']:
	msg = output.INVALID_FORMAT_MSG.format(extension=extension)
	return output.IFRAME_TEMPLATE.format(html=msg)

	try:
	molecule = read_molecule(path)
	molecule = Chem.RemoveAllHs(molecule)
	name = '.'.join(path.split('/')[-1].split('.')[:-1])
	inp_sdf = f'results/input_{name}.sdf'
	except Exception as e:
	return f'Could not read the molecule: {e}'

	if molecule.GetNumAtoms() > 50:
	return f'Too large molecule: upper limit is 50 heavy atoms'

	with Chem.SDWriter(inp_sdf) as w:
	w.write(molecule)

	positions, one_hot, charges = parse_molecule(molecule, is_geom=True)
	anchors = np.zeros_like(charges)
	fragment_mask = np.ones_like(charges)
	linker_mask = np.zeros_like(charges)
	print('Read and parsed molecule')

	dataset = [{
	'uuid': '0',
	'name': '0',
	'positions': torch.tensor(positions, dtype=const.TORCH_FLOAT, device=device),
	'one_hot': torch.tensor(one_hot, dtype=const.TORCH_FLOAT, device=device),
	'charges': torch.tensor(charges, dtype=const.TORCH_FLOAT, device=device),
	'anchors': torch.tensor(anchors, dtype=const.TORCH_FLOAT, device=device),
	'fragment_mask': torch.tensor(fragment_mask, dtype=const.TORCH_FLOAT, device=device),
	'linker_mask': torch.tensor(linker_mask, dtype=const.TORCH_FLOAT, device=device),
	'num_atoms': len(positions),
	}] * N_SAMPLES
	dataloader = get_dataloader(dataset, batch_size=N_SAMPLES, collate_fn=collate_with_fragment_edges)
	print('Created dataloader')

	ddpm.edm.T = n_steps
	assert ddpm.center_of_mass == 'fragments'

	if n_atoms == 0:
	def sample_fn(_data):
	out, _ = size_nn.forward(_data, return_loss=False)
	probabilities = torch.softmax(out, dim=1)
	distribution = torch.distributions.Categorical(probs=probabilities)
	samples = distribution.sample()
	sizes = []
	for label in samples.detach().cpu().numpy():
	sizes.append(size_nn.linker_id2size[label])
	sizes = torch.tensor(sizes, device=samples.device, dtype=torch.long)
	return sizes
	else:
	def sample_fn(_data):
	return torch.ones(_data['positions'].shape[0], device=device, dtype=torch.long) * n_atoms

	for data in dataloader:
	chain, node_mask = ddpm.sample_chain(data, sample_fn=sample_fn, keep_frames=1)
	print('Generated linker')
	x = chain[0][:, :, :ddpm.n_dims]
	h = chain[0][:, :, ddpm.n_dims:]

	# Put the molecule back to the initial orientation
	pos_masked = data['positions'] * data['fragment_mask']
	N = data['fragment_mask'].sum(1, keepdims=True)
	mean = torch.sum(pos_masked, dim=1, keepdim=True) / N
	x = x + mean * node_mask

	names = [f'output_{i+1}_{name}' for i in range(N_SAMPLES)]
	save_xyz_file('results', h, x, node_mask, names=names, is_geom=True, suffix='')
	print('Saved XYZ files')
	break

	out_files = []
	for i in range(N_SAMPLES):
	out_xyz = f'results/output_{i+1}_{name}_.xyz'
	out_sdf = f'results/output_{i+1}_{name}_.sdf'
	subprocess.run(f'obabel {out_xyz} -O {out_sdf}', shell=True)
	out_files.append(out_sdf)
	print('Converted to SDF')

	return [
	draw_sample(0, out_files),
	[inp_sdf] + out_files,
	gr.Radio.update(visible=True, value='Sample 1')
	]


	demo = gr.Blocks()
	with demo:
	gr.Markdown('# DiffLinker: Equivariant 3D-Conditional Diffusion Model for Molecular Linker Design')
	gr.Markdown(
	'Given a set of disconnected fragments in 3D, '
	'DiffLinker places missing atoms in between and designs a molecule incorporating all the initial fragments. '
	'Our method can link an arbitrary number of fragments, requires no information on the attachment atoms '
	'and linker size, and can be conditioned on the protein pockets.'
	)
	gr.Markdown(
	'[[Paper]](https://arxiv.org/abs/2210.05274) '
	'[[Code]](https://github.com/igashov/DiffLinker)'
	)
	with gr.Box():
	with gr.Row():
	with gr.Column():
	gr.Markdown('## Input Fragments')
	gr.Markdown('Upload the file with 3D-coordinates of the input fragments in .pdb, .mol2 or .sdf format:')
	input_file = gr.File(file_count='single', label='Input Fragments')
	n_steps = gr.Slider(minimum=10, maximum=500, label="Number of Denoising Steps", step=10)
	n_atoms = gr.Slider(
	minimum=0, maximum=20,
	label="Linker Size: DiffLinker will predict it if set to 0",
	step=1
	)
	examples = gr.Dataset(
	components=[gr.File(visible=False)],
	samples=[['examples/example_1.sdf'], ['examples/example_2.sdf']],
	type='index',
	)

	button = gr.Button('Generate Linker!')
	gr.Markdown('')
	gr.Markdown('## Output Files')
	gr.Markdown('Download files with the generated molecules here:')
	output_files = gr.File(file_count='multiple', label='Output Files', interactive=False)
	with gr.Column():
	gr.Markdown('## Visualization')
	# gr.Markdown('Below you will see input and output molecules')
	samples = gr.Radio(
	choices=['Sample 1', 'Sample 2', 'Sample 3', 'Sample 4', 'Sample 5'],
	value='Sample 1',
	type='index',
	show_label=False,
	visible=False,
	interactive=True,
	)
	visualization = gr.HTML()

	input_file.change(
	fn=show_input,
	inputs=[input_file],
	outputs=[visualization, samples],
	)
	input_file.clear(
	fn=lambda: [None, '', gr.Radio.update(visible=False)],
	inputs=[],
	outputs=[input_file, visualization, samples],
	)
	examples.click(
	fn=lambda idx: [f'examples/example_{idx+1}.sdf', 10, 0] + show_input(f'examples/example_{idx+1}.sdf'),
	inputs=[examples],
	outputs=[input_file, n_steps, n_atoms, visualization, samples]
	)
	button.click(
	fn=generate,
	inputs=[input_file, n_steps, n_atoms],
	outputs=[visualization, output_files, samples],
	)
	samples.change(
	fn=draw_sample,
	inputs=[samples, output_files],
	outputs=[visualization],
	)

	demo.launch(server_name=args.ip)