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from mpi4py import MPI |
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from mpi4py.futures import MPICommExecutor |
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import warnings |
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from Bio.PDB import PDBParser, PPBuilder, CaPPBuilder |
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from Bio.PDB.NeighborSearch import NeighborSearch |
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from Bio.PDB.Selection import unfold_entities |
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import numpy as np |
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import dask.array as da |
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from rdkit import Chem |
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from functools import partial |
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import os |
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import re |
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import sys |
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import io |
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import random |
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import gzip |
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import copy |
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from atomic_renamer import AtomicNamer |
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from prody import * |
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import webdataset as wd |
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amino_acids = {'L': 'LEU', 'A': 'ALA', 'G': 'GLY', 'V': 'VAL', 'E': 'GLU', 'S': 'SER', 'I': 'ILE', 'K': 'LYS', |
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'R': 'ARG', 'D': 'ASP', 'T': 'THR', 'P': 'PRO', 'N': 'ASN', 'Q': 'GLN', 'F': 'PHE', 'Y': 'TYR', |
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'M': 'MET', 'H': 'HIS', 'C': 'CYS', 'W': 'TRP'} |
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nfeat = 15 |
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punctuation_regex = r"""(\(|\)|\.|=|#|-|\+|\\|\/|:|~|@|\?|>>?|\*|\$|\%[0-9]{2}|[0-9])""" |
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molecule_regex = r"""(\[[^\]]+]|Br?|Cl?|N|O|S|P|F|I|b|c|n|o|s|p|\(|\)|\.|=|#|-|\+|\\|\/|:|~|@|\?|>>?|\*|\$|\%[0-9]{2}|[0-9])""" |
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def get_protein_sequence_and_coords(structure): |
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hv = structure.getHierView() |
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seq = '' |
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xyz = [] |
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resindex = [] |
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for chain in hv: |
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cid = chain.getChid() |
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calpha = structure.select(f'calpha chain {cid} icode _') |
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N = structure.select(f'name N chain {cid} icode _') |
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C = structure.select(f'name C chain {cid} icode _') |
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xyz += [(ca,n,c) for ca,n,c in zip(calpha.getCoords(), N.getCoords(), C.getCoords())] |
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seq += calpha.getSequence() |
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resindex += [ca.getResindex() for ca in calpha] |
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return seq, xyz, resindex |
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def get_pdb_components(pdb_id): |
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""" |
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Split a protein-ligand pdb into protein and ligand components |
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:param pdb_id: |
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:return: |
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""" |
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with open(pdb_id,'r') as f: |
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pdb = parsePDBStream(f,model=1) |
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protein = pdb.select('protein') |
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return protein |
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def rot_from_two_vecs(e0_unnormalized, e1_unnormalized): |
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"""Create rotation matrices from unnormalized vectors for the x and y-axes. |
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This creates a rotation matrix from two vectors using Gram-Schmidt |
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orthogonalization. |
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Args: |
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e0_unnormalized: vectors lying along x-axis of resulting rotation |
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e1_unnormalized: vectors lying in xy-plane of resulting rotation |
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Returns: |
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Rotations resulting from Gram-Schmidt procedure. |
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""" |
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e0 = e0_unnormalized / np.linalg.norm(e0_unnormalized) |
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c = np.dot(e1_unnormalized, e0) |
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e1 = e1_unnormalized - c * e0 |
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e1 = e1 / np.linalg.norm(e1) |
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e2 = np.cross(e0, e1) |
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return np.stack([e0,e1,e2]).T |
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def parse_complex(aa, data_dir, i_pdb_fns): |
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shard_idx, pdb_fns = i_pdb_fns |
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chunk_name = [] |
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chunk_smiles = [] |
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chunk_lig_xyz = [] |
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chunk_seq = [] |
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chunk_rec_xyz = [] |
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chunk_rec_R = [] |
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chunk_rec_feat = [] |
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for pdb_fn in pdb_fns: |
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try: |
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name = os.path.basename(pdb_fn) |
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protein = get_pdb_components(pdb_fn+'/'+name+'_protein.pdb') |
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seq, xyz, resindex = get_protein_sequence_and_coords(protein) |
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if len(seq) < 3: |
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raise ValueError |
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assert len(xyz) == len(seq), "sequence and coord mismatch" |
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R_receptor = [] |
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for t in xyz: |
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CA = np.array(t[0]) |
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N = np.array(t[1]) |
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C = np.array(t[2]) |
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R_receptor.append(rot_from_two_vecs(N-CA,C-CA).flatten().tolist()) |
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feat = np.zeros((len(resindex),nfeat,3),dtype=np.float32) |
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feat[:] = np.nan |
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for i,(n, res) in enumerate(zip(resindex, seq)): |
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atoms = protein.select(f'resindex {n}') |
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ss = io.StringIO() |
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prody.writePDBStream(ss, atoms) |
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try: |
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mol = Chem.MolFromPDBBlock(ss.getvalue()) |
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ref_aa = copy.deepcopy(aa[res]) |
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reflabels = [l.split()[0] for l in ref_aa.reflabels] |
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labels = [l.split()[0] for l in ref_aa.name(mol)] |
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pos = mol.GetConformer().GetPositions() |
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xyz_labels = sorted([(xyz, reflabels.index(l)) for xyz,l in zip(pos,labels) |
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if l in reflabels], key=lambda t: t[1]) |
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for r, j in xyz_labels: |
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feat[i,j,:] = r |
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except Exception as e: |
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print('Unsuccesful in assigning atoms to amino acid letter {}'.format(res),ss.getvalue(),e) |
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raise |
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suppl = Chem.SDMolSupplier(pdb_fn+'/'+name+'_ligand.sdf') |
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mol = next(suppl) |
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smi = Chem.MolToSmiles(mol) |
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atom_order = [int(s) for s in list(filter(None,re.sub(r'[\[\]]','',mol.GetProp("_smilesAtomOutputOrder")).split(',')))] |
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tokens = list(filter(None, re.split(molecule_regex, smi))) |
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masked_tokens = [re.sub(punctuation_regex,'',s) for s in tokens] |
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k = 0 |
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token_pos = [] |
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for i,token in enumerate(masked_tokens): |
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if token != '': |
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token_pos.append(tuple(mol.GetConformer().GetAtomPosition(atom_order[k]))) |
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k += 1 |
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else: |
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token_pos.append((np.nan, np.nan, np.nan)) |
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chunk_name.append(name) |
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chunk_seq.append(seq) |
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chunk_rec_xyz.append(np.array([np.array(t[0]).tolist() for t in xyz])) |
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chunk_rec_R.append(np.array(R_receptor)) |
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chunk_rec_feat.append(feat) |
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chunk_smiles.append(smi) |
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chunk_lig_xyz.append(token_pos) |
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except Exception as e: |
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print(e) |
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pass |
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try: |
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shard_idx = str(shard_idx) |
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with wd.TarWriter(f'{data_dir}/part-' + shard_idx + '.tar', compress=True) as sink: |
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for index in range(len(chunk_name)): |
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sink.write({ |
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'__key__': "%s_%06d" % (shard_idx, index), |
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'name.txt': chunk_name[index], |
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'seq.txt': chunk_seq[index], |
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'smiles.txt': chunk_smiles[index], |
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'rec_xyz.pyd': chunk_rec_xyz[index], |
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'rec_R.pyd': chunk_rec_R[index], |
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'rec_feat.pyd': chunk_rec_feat[index], |
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'lig_xyz.pyd': chunk_lig_xyz[index], |
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}) |
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return len(chunk_name) |
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except Exception as e: |
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print('Exception while writing', repr(e)) |
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if __name__ == '__main__': |
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import glob |
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filenames = glob.glob('data/pdbbind/v2020-other-PL/*') |
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filenames.extend(glob.glob('data/pdbbind/refined-set/*')) |
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filenames = sorted(filenames) |
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with open('split_direction/timesplit_no_lig_overlap_train','r') as f: |
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train_rec = f.read().split() |
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with open('split_direction/timesplit_no_lig_overlap_val','r') as f: |
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val_rec = f.read().split() |
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with open('split_direction/timesplit_test','r') as f: |
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test_rec = f.read().split() |
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train = [x for x in filenames if x.split('/')[-1] in train_rec] |
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val = [x for x in filenames if x.split('/')[-1] in val_rec] |
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test = [x for x in filenames if x.split('/')[-1] in test_rec] |
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print(f'Train has {len(train)} items and first 5 are {train[:5]}') |
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print(f'Val has {len(val)} items and first 5 are {val[:5]}') |
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print(f'Test has {len(test)} items and first 5 are {test[:5]}') |
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def chunks(lst, n): |
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"""Yield successive n-sized chunks from lst.""" |
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for i in range(0, len(lst), n): |
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yield lst[i:i + n] |
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comm = MPI.COMM_WORLD |
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with MPICommExecutor(comm, root=0) as executor: |
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if executor is not None: |
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aa = {k: AtomicNamer(v) for k,v in amino_acids.items()} |
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chunk_sizes = executor.map(partial(parse_complex, aa, 'train'), enumerate(chunks(train, 512))) |
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total_train_rows = 0 |
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for s in chunk_sizes: |
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total_train_rows += s |
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chunk_sizes = executor.map(partial(parse_complex, aa, 'val'), enumerate(chunks(val, 512))) |
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total_val_rows = 0 |
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for s in chunk_sizes: |
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total_val_rows += s |
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chunk_sizes = executor.map(partial(parse_complex, aa, 'test'), enumerate(chunks(test, 512))) |
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total_test_rows = 0 |
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for s in chunk_sizes: |
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total_test_rows += s |
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print('Total number of train rows {}'.format(total_train_rows)) |
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print('Total number of val rows {}'.format(total_val_rows)) |
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print('Total number of test rows {}'.format(total_test_rows)) |
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