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# -*- coding: utf-8 -*- """ .. currentmodule:: modlamp.descriptors .. moduleauthor:: modlab Alex Mueller ETH Zurich <alex.mueller@pharma.ethz.ch> This module incorporates different classes to calculate peptide descriptor values. The following classes are available: ============================= ============================================================================ Class Characteristics ============================= ============================================================================ :py:class:`GlobalDescriptor` Global one-dimensional peptide descriptors calculated from the AA sequence. :py:class:`PeptideDescriptor` AA scale based global or convoluted descriptors (auto-/cross-correlated). ============================= ============================================================================ .. seealso:: :class:`modlamp.core.BaseDescriptor` from which the classes in :mod:`modlamp.descriptors` inherit. """ import sys import numpy as np from scipy import stats from sklearn.externals.joblib import Parallel, delayed from plotWheels.core import ( BaseDescriptor, load_scale, count_aas, aa_weights, aa_energies, aa_formulas, ) __author__ = "Alex Müller, Gisela Gabernet" __docformat__ = "restructuredtext en" def _one_autocorr(seq, window, scale): """Private function used for calculating auto-correlated descriptors for 1 given sequence, window and an AA scale. This function is used by the :py:func:`calculate_autocorr` method of :py:class:`PeptideDescriptor`. :param seq: {str} amino acid sequence to calculate descriptor for :param window: {int} correlation-window size :param scale: {str} amino acid scale to be used to calculate descriptor :return: {numpy.array} calculated descriptor data """ try: m = list() # list of lists to store translated sequence values for l in range(len(seq)): # translate AA sequence into values m.append(scale[str(seq[l])]) # auto-correlation in defined sequence window seqdesc = list() for dist in range(window): # for all correlation distances for val in range( len(scale["A"]) ): # for all features of the descriptor scale valsum = list() cntr = 0.0 for pos in range(len(seq)): # for every position in the sequence if (pos + dist) < len( seq ): # check if corr distance is possible at that sequence position cntr += 1 # counter to scale sum valsum.append(m[pos][val] * m[pos + dist][val]) seqdesc.append( sum(valsum) / cntr ) # append scaled correlation distance values return seqdesc except ZeroDivisionError: print( "ERROR!\nThe chosen correlation window % i is larger than the sequence %s !" % (window, seq) ) def _one_crosscorr(seq, window, scale): """Private function used for calculating cross-correlated descriptors for 1 given sequence, window and an AA scale. This function is used by the :py:func:`calculate_crosscorr` method of :py:class:`PeptideDescriptor`. :param seq: {str} amino acid sequence to calculate descriptor for :param window: {int} correlation-window size :param scale: {str} amino acid scale to be used to calculate descriptor :return: {numpy.array} calculated descriptor data """ try: m = list() # list of lists to store translated sequence values for l in range(len(seq)): # translate AA sequence into values m.append(scale[str(seq[l])]) # auto-correlation in defined sequence window seqdesc = list() for val in range(len(scale["A"])): # for all features of the descriptor scale for cc in range(len(scale["A"])): # for every feature cross correlation if (val + cc) < len( scale["A"] ): # check if corr distance is in range of the num of features for dist in range(window): # for all correlation distances cntr = float() valsum = list() for pos in range( len(seq) ): # for every position in the sequence if (pos + dist) < len( seq ): # check if corr distance is possible at that sequence pos cntr += 1 # counter to scale sum valsum.append(m[pos][val] * m[pos + dist][val + cc]) seqdesc.append( sum(valsum) / cntr ) # append scaled correlation distance values return seqdesc except ZeroDivisionError: print( "ERROR!\nThe chosen correlation window % i is larger than the sequence %s !" % (window, seq) ) def _one_arc(seq, modality, scale): """Privat function used for calculating arc descriptors for one sequence and AA scale. This function is used by :py:func:`calculate_arc` method method of :py:class:`PeptideDescriptor`. :param seq: {str} amino acid sequence to calculate descriptor for :param scale: {str} amino acid scale to be used to calculate descriptor :return: {numpy.array} calculated descriptor data """ desc_mat = [] for aa in seq: desc_mat.append(scale[aa]) desc_mat = np.asarray(desc_mat) # Check descriptor dimension desc_dim = desc_mat.shape[1] # list to store descriptor values for all windows allwindows_arc = [] if len(seq) > 18: window = 18 # calculates number of windows in sequence num_windows = len(seq) - window else: window = len(seq) num_windows = 1 # loop through all windows for j in range(num_windows): # slices descriptor matrix into current window window_mat = desc_mat[j : j + window, :] # defines order of amino acids in helical projection order = [0, 11, 4, 15, 8, 1, 12, 5, 16, 9, 2, 13, 6, 17, 10, 3, 14, 7] # orders window descriptor matrix into helical projection order ordered = [] for pos in order: try: ordered.append(window_mat[pos, :]) except: # for sequences of len < 18 adding dummy vector with 2s, length of descriptor dimensions ordered.append([2] * desc_dim) ordered = np.asarray(ordered) window_arc = [] # loop through pharmacophoric features for m in range(desc_dim): all_arcs = ( [] ) # stores all arcs that can be found of a pharmacophoric feature arc = 0 for n in range( 18 ): # for all positions in helix, regardless of sequence length if ( ordered[n, m] == 0 ): # if position does not contain pharmacophoric feature all_arcs.append(arc) # append previous arc to all arcs list arc = 0 # arc is initialized elif ( ordered[n, m] == 1 ): # if position contains pharmacophoric feature(PF), elongate arc by 20° arc += 20 elif ordered[n, m] == 2: # if position doesn't contain amino acid: if ( ordered[n - 1, m] == 1 ): # if previous position contained PF add 10° arc += 10 elif ( ordered[n - 1, m] == 0 ): # if previous position didn't contain PF don't add anything arc += 0 elif ( ordered[n - 2, m] == 1 ): # if previous position is empty then check second previous for PF arc += 10 if ( n == 17 ): # if we are at the last position check for position n=0 instead of next position. if ordered[0, m] == 1: # if it contains PF add 10° extra arc += 10 else: # if next position contains PF add 10° extra if ordered[n + 1, m] == 1: arc += 10 elif ordered[n + 1, m] == 0: arc += 0 else: # if next position is empty check for 2nd next position if n == 16: if ordered[0, m] == 1: arc += 10 else: if ordered[n + 2, m] == 1: arc += 10 all_arcs.append(arc) if not arc == 360: arc0 = all_arcs.pop() + all_arcs[0] # join first and last arc together all_arcs = [arc0] + all_arcs[1:] window_arc.append( np.max(all_arcs) ) # append to window arcs the maximum arc of this PF allwindows_arc.append(window_arc) # append all PF arcs of this window allwindows_arc = np.asarray(allwindows_arc) if modality == "max": final_arc = np.max( allwindows_arc, axis=0 ) # calculate maximum / mean arc along all windows elif modality == "mean": final_arc = np.mean(allwindows_arc, axis=0) else: print('modality is unknown, please choose between "max" and "mean"\n.') sys.exit() return final_arc def _charge(seq, ph=7.0, amide=False): """Calculates charge of a single sequence. The method used is first described by Bjellqvist. In the case of amidation, the value for the 'Cterm' pKa is 15 (and Cterm is added to the pos_pks dictionary. The pKa scale is extracted from: http://www.hbcpnetbase.com/ (CRC Handbook of Chemistry and Physics, 96th ed). **pos_pks** = {'Nterm': 9.38, 'K': 10.67, 'R': 12.10, 'H': 6.04} **neg_pks** = {'Cterm': 2.15, 'D': 3.71, 'E': 4.15, 'C': 8.14, 'Y': 10.10} :param ph: {float} pH at which to calculate peptide charge. :param amide: {boolean} whether the sequences have an amidated C-terminus. :return: {array} descriptor values in the attribute :py:attr:`descriptor """ if amide: pos_pks = {"Nterm": 9.38, "K": 10.67, "R": 12.10, "H": 6.04} neg_pks = {"Cterm": 15.0, "D": 3.71, "E": 4.15, "C": 8.14, "Y": 10.10} else: pos_pks = {"Nterm": 9.38, "K": 10.67, "R": 12.10, "H": 6.04} neg_pks = {"Cterm": 2.15, "D": 3.71, "E": 4.15, "C": 8.14, "Y": 10.10} aa_content = count_aas(seq, scale="absolute") aa_content["Nterm"] = 1.0 aa_content["Cterm"] = 1.0 pos_charge = 0.0 for aa, pK in pos_pks.items(): c_r = 10 ** (pK - ph) partial_charge = c_r / (c_r + 1.0) pos_charge += aa_content[aa] * partial_charge neg_charge = 0.0 for aa, pK in neg_pks.items(): c_r = 10 ** (ph - pK) partial_charge = c_r / (c_r + 1.0) neg_charge += aa_content[aa] * partial_charge return round(pos_charge - neg_charge, 3) class GlobalDescriptor(BaseDescriptor): """ Base class for global, non-amino acid scale dependant descriptors. The following descriptors can be calculated by the **methods** linked below: - `Sequence Length <modlamp.html#modlamp.descriptors.GlobalDescriptor.length>`_ - `Molecular Formula <modlamp.html#modlamp.descriptors.GlobalDescriptor.formula>`_ - `Molecular Weight <modlamp.html#modlamp.descriptors.GlobalDescriptor.calculate_MW>`_ - `Sequence Charge <modlamp.html#modlamp.descriptors.GlobalDescriptor.calculate_charge>`_ - `Charge Density <modlamp.html#modlamp.descriptors.GlobalDescriptor.charge_density>`_ - `Isoelectric Point <modlamp.html#modlamp.descriptors.GlobalDescriptor.isoelectric_point>`_ - `Instability Index <modlamp.html#modlamp.descriptors.GlobalDescriptor.instability_index>`_ - `Aromaticity <modlamp.html#modlamp.descriptors.GlobalDescriptor.aromaticity>`_ - `Aliphatic Index <modlamp.html#modlamp.descriptors.GlobalDescriptor.aliphatic_index>`_ - `Boman Index <modlamp.html#modlamp.descriptors.GlobalDescriptor.boman_index>`_ - `Hydrophobic Ratio <modlamp.html#modlamp.descriptors.GlobalDescriptor.hydrophobic_ratio>`_ - `all of the above <modlamp.html#modlamp.descriptors.GlobalDescriptor.calculate_all>`_ """ def length(self, append=False): """ Method to calculate the length (total AA count) of every sequence in the attribute :py:attr:`sequences`. :param append: {boolean} whether the produced descriptor values should be appended to the existing ones in the attribute :py:attr:`descriptor`. :return: array of sequence lengths in the attribute :py:attr:`descriptor` :Example: >>> desc = GlobalDescriptor(['AFDGHLKI','KKLQRSDLLRTK','KKLASCNNIPPR']) >>> desc.length() >>> desc.descriptor array([[ 8.], [12.], [12.]]) """ desc = [] for seq in self.sequences: desc.append(float(len(seq.strip()))) desc = np.asarray(desc).reshape(len(desc), 1) if append: self.descriptor = np.hstack((self.descriptor, np.array(desc))) self.featurenames.append("Length") else: self.descriptor = np.array(desc) self.featurenames = ["Length"] def formula(self, amide=False, append=False): """Method to calculate the molecular formula of every sequence in the attribute :py:attr:`sequences`. :param amide: {boolean} whether the sequences are C-terminally amidated. :param append: {boolean} whether the produced descriptor values should be appended to the existing ones in the attribute :py:attr:`descriptor`. :return: array of molecular formulas {str} in the attribute :py:attr:`descriptor` :Example: >>> desc = GlobalDescriptor(['KADSFLSADGHSADFSLDKKLKERL', 'ERTILSDFPQWWFASLDFLNC', 'ACDEFGHIKLMNPQRSTVWY']) >>> desc.formula(amide=True) >>> for v in desc.descriptor: ... print(v[0]) C122 H197 N35 O39 C121 H168 N28 O33 S C106 H157 N29 O30 S2 .. seealso:: :py:func:`modlamp.core.aa_formulas()` .. versionadded:: v2.7.6 """ desc = [] formulas = aa_formulas() for seq in self.sequences: f = {"C": 0, "H": 0, "N": 0, "O": 0, "S": 0} for aa in seq: # loop over all AAs for k in f.keys(): f[k] += formulas[aa][k] # substract H2O for every peptide bond f["H"] -= 2 * (len(seq) - 1) f["O"] -= len(seq) - 1 if amide: # add C-terminal amide --> replace OH with NH2 f["O"] -= 1 f["H"] += 1 f["N"] += 1 if f["S"] != 0: val = "C%s H%s N%s O%s %s%s" % ( f["C"], f["H"], f["N"], f["O"], "S", f["S"], ) else: val = "C%s H%s N%s O%s" % (f["C"], f["H"], f["N"], f["O"]) desc.append([val]) if append: self.descriptor = np.hstack((self.descriptor, np.array(desc))) self.featurenames.append("Formula") else: self.descriptor = np.array(desc) self.featurenames = ["Formula"] def calculate_MW(self, amide=False, append=False): """Method to calculate the molecular weight [g/mol] of every sequence in the attribute :py:attr:`sequences`. :param amide: {boolean} whether the sequences are C-terminally amidated (subtracts 0.95 from the MW). :param append: {boolean} whether the produced descriptor values should be appended to the existing ones in the attribute :py:attr:`descriptor`. :return: array of descriptor values in the attribute :py:attr:`descriptor` :Example: >>> desc = GlobalDescriptor('IAESFKGHIPL') >>> desc.calculate_MW(amide=True) >>> desc.descriptor array([[ 1210.43]]) .. seealso:: :py:func:`modlamp.core.aa_weights()` .. versionchanged:: v2.1.5 amide option added """ desc = [] weights = aa_weights() for seq in self.sequences: mw = [] for aa in seq: # sum over aa weights mw.append(weights[aa]) desc.append( round(sum(mw) - 18.015 * (len(seq) - 1), 2) ) # sum over AA MW and subtract H20 MW for every # peptide bond desc = np.asarray(desc).reshape(len(desc), 1) if ( amide ): # if sequences are amidated, subtract 0.98 from calculated MW (OH - NH2) desc = [d - 0.98 for d in desc] if append: self.descriptor = np.hstack((self.descriptor, np.array(desc))) self.featurenames.append("MW") else: self.descriptor = np.array(desc) self.featurenames = ["MW"] def calculate_charge(self, ph=7.0, amide=False, append=False): """Method to overall charge of every sequence in the attribute :py:attr:`sequences`. The method used is first described by Bjellqvist. In the case of amidation, the value for the 'Cterm' pKa is 15 (and Cterm is added to the pos_pKs dictionary. The pKa scale is extracted from: http://www.hbcpnetbase.com/ (CRC Handbook of Chemistry and Physics, 96th ed). **pos_pKs** = {'Nterm': 9.38, 'K': 10.67, 'R': 12.10, 'H': 6.04} **neg_pKs** = {'Cterm': 2.15, 'D': 3.71, 'E': 4.15, 'C': 8.14, 'Y': 10.10} :param ph: {float} ph at which to calculate peptide charge. :param amide: {boolean} whether the sequences have an amidated C-terminus. :param append: {boolean} whether the produced descriptor values should be appended to the existing ones in the attribute :py:attr:`descriptor`. :return: array of descriptor values in the attribute :py:attr:`descriptor` :Example: >>> desc = GlobalDescriptor('KLAKFGKRSELVALSG') >>> desc.calculate_charge(ph=7.4, amide=True) >>> desc.descriptor array([[ 3.989]]) """ desc = [] for seq in self.sequences: desc.append( _charge(seq, ph, amide) ) # calculate charge with helper function desc = np.asarray(desc).reshape(len(desc), 1) if append: self.descriptor = np.hstack((self.descriptor, np.array(desc))) self.featurenames.append("Charge") else: self.descriptor = np.array(desc) self.featurenames = ["Charge"] def charge_density(self, ph=7.0, amide=False, append=False): """Method to calculate the charge density (charge / MW) of every sequences in the attributes :py:attr:`sequences` :param ph: {float} pH at which to calculate peptide charge. :param amide: {boolean} whether the sequences have an amidated C-terminus. :param append: {boolean} whether the produced descriptor values should be appended to the existing ones in the attribute :py:attr:`descriptor`. :return: array of descriptor values in the attribute :py:attr:`descriptor`. :Example: >>> desc = GlobalDescriptor('GNSDLLIEQRTLLASDEF') >>> desc.charge_density(ph=6, amide=True) >>> desc.descriptor array([[-0.00097119]]) """ self.calculate_charge(ph, amide) charges = self.descriptor self.calculate_MW(amide) masses = self.descriptor desc = charges / masses desc = np.asarray(desc).reshape(len(desc), 1) if append: self.descriptor = np.hstack((self.descriptor, np.array(desc))) self.featurenames.append("ChargeDensity") else: self.descriptor = np.array(desc) self.featurenames = ["ChargeDensity"] def isoelectric_point(self, amide=False, append=False): """ Method to calculate the isoelectric point of every sequence in the attribute :py:attr:`sequences`. The pK scale is extracted from: http://www.hbcpnetbase.com/ (CRC Handbook of Chemistry and Physics, 96th ed). **pos_pKs** = {'Nterm': 9.38, 'K': 10.67, 'R': 12.10, 'H': 6.04} **neg_pKs** = {'Cterm': 2.15, 'D': 3.71, 'E': 4.15, 'C': 8.14, 'Y': 10.10} :param amide: {boolean} whether the sequences have an amidated C-terminus. :param append: {boolean} whether the produced descriptor values should be appended to the existing ones in the attribute :py:attr:`descriptor`. :return: array of descriptor values in the attribute :py:attr:`descriptor` :Example: >>> desc = GlobalDescriptor('KLFDIKFGHIPQRST') >>> desc.isoelectric_point() >>> desc.descriptor array([[ 10.6796875]]) """ ph, ph1, ph2 = float(), float(), float() desc = [] for seq in self.sequences: # Bracket between ph1 and ph2 ph = 7.0 charge = _charge(seq, ph, amide) if charge > 0.0: ph1 = ph charge1 = charge while charge1 > 0.0: ph = ph1 + 1.0 charge = _charge(seq, ph, amide) if charge > 0.0: ph1 = ph charge1 = charge else: ph2 = ph break else: ph2 = ph charge2 = charge while charge2 < 0.0: ph = ph2 - 1.0 charge = _charge(seq, ph, amide) if charge < 0.0: ph2 = ph charge2 = charge else: ph1 = ph break # Bisection while ph2 - ph1 > 0.0001 and charge != 0.0: ph = (ph1 + ph2) / 2.0 charge = _charge(seq, ph, amide) if charge > 0.0: ph1 = ph else: ph2 = ph desc.append(ph) desc = np.asarray(desc).reshape(len(desc), 1) if append: self.descriptor = np.hstack((self.descriptor, np.array(desc))) self.featurenames.append("pI") else: self.descriptor = np.array(desc) self.featurenames = ["pI"] def instability_index(self, append=False): """ Method to calculate the instability of every sequence in the attribute :py:attr:`sequences`. The instability index is a prediction of protein stability based on the amino acid composition. ([1] K. Guruprasad, B. V Reddy, M. W. Pandit, Protein Eng. 1990, 4, 155–161.) :param append: {boolean} whether the produced descriptor values should be appended to the existing ones in the attribute :py:attr:`descriptor`. :return: array of descriptor values in the attribute :py:attr:`descriptor` :Example: >>> desc = GlobalDescriptor('LLASMNDLLAKRST') >>> desc.instability_index() >>> desc.descriptor array([[ 63.95714286]]) """ desc = [] dimv = load_scale("instability")[1] for seq in self.sequences: stabindex = float() for i in range(len(seq) - 1): stabindex += dimv[seq[i]][seq[i + 1]] desc.append((10.0 / len(seq)) * stabindex) desc = np.asarray(desc).reshape(len(desc), 1) if append: self.descriptor = np.hstack((self.descriptor, np.array(desc))) self.featurenames.append("InstabilityInd") else: self.descriptor = np.array(desc) self.featurenames = ["InstabilityInd"] def aromaticity(self, append=False): """ Method to calculate the aromaticity of every sequence in the attribute :py:attr:`sequences`. According to Lobry, 1994, it is simply the relative frequency of Phe+Trp+Tyr. :param append: {boolean} whether the produced descriptor values should be appended to the existing ones in the attribute :py:attr:`descriptor`. :return: array of descriptor values in the attribute :py:attr:`descriptor` :Example: >>> desc = GlobalDescriptor('GLFYWRFFLQRRFLYWW') >>> desc.aromaticity() >>> desc.descriptor array([[ 0.52941176]]) """ desc = [] for seq in self.sequences: f = seq.count("F") w = seq.count("W") y = seq.count("Y") desc.append(float(f + w + y) / len(seq)) desc = np.asarray(desc).reshape(len(desc), 1) if append: self.descriptor = np.hstack((self.descriptor, np.array(desc))) self.featurenames.append("Aromaticity") else: self.descriptor = np.array(desc) self.featurenames = ["Aromaticity"] def aliphatic_index(self, append=False): """ Method to calculate the aliphatic index of every sequence in the attribute :py:attr:`sequences`. According to Ikai, 1980, the aliphatic index is a measure of thermal stability of proteins and is dependant on the relative volume occupied by aliphatic amino acids (A,I,L & V). ([1] A. Ikai, J. Biochem. 1980, 88, 1895–1898.) :param append: {boolean} whether the produced descriptor values should be appended to the existing ones in the attribute :py:attr:`descriptor`. :return: array of descriptor values in the attribute :py:attr:`descriptor` :Example: >>> desc = GlobalDescriptor('KWLKYLKKLAKLVK') >>> desc.aliphatic_index() >>> desc.descriptor array([[ 139.28571429]]) """ desc = [] aa_dict = aa_weights() for seq in self.sequences: d = {aa: seq.count(aa) for aa in aa_dict.keys()} # count aa d = { k: (float(d[k]) / len(seq)) * 100 for k in d.keys() } # get mole percent of all AA desc.append( d["A"] + 2.9 * d["V"] + 3.9 * (d["I"] + d["L"]) ) # formula for calculating the AI (Ikai, 1980) desc = np.asarray(desc).reshape(len(desc), 1) if append: self.descriptor = np.hstack((self.descriptor, np.array(desc))) self.featurenames.append("AliphaticInd") else: self.descriptor = np.array(desc) self.featurenames = ["AliphaticInd"] def boman_index(self, append=False): """Method to calculate the boman index of every sequence in the attribute :py:attr:`sequences`. According to Boman, 2003, the boman index is a measure for protein-protein interactions and is calculated by summing over all amino acid free energy of transfer [kcal/mol] between water and cyclohexane,[2] followed by dividing by sequence length. ([1] H. G. Boman, D. Wade, I. a Boman, B. Wåhlin, R. B. Merrifield, *FEBS Lett*. **1989**, *259*, 103–106. [2] A. Radzick, R. Wolfenden, *Biochemistry* **1988**, *27*, 1664–1670.) .. seealso:: :py:func:`modlamp.core.aa_energies()` :param append: {boolean} whether the produced descriptor values should be appended to the existing ones in the attribute :py:attr:`descriptor`. :return: array of descriptor values in the attribute :py:attr:`descriptor` :Example: >>> desc = GlobalDescriptor('GLFDIVKKVVGALGSL') >>> desc.boman_index() >>> desc.descriptor array([[-1.011875]]) """ d = aa_energies() desc = [] for seq in self.sequences: val = [] for a in seq: val.append(d[a]) desc.append(sum(val) / len(val)) desc = np.asarray(desc).reshape(len(desc), 1) if append: self.descriptor = np.hstack((self.descriptor, np.array(desc))) self.featurenames.append("BomanInd") else: self.descriptor = np.array(desc) self.featurenames = ["BomanInd"] def hydrophobic_ratio(self, append=False): """ Method to calculate the hydrophobic ratio of every sequence in the attribute :py:attr:`sequences`, which is the relative frequency of the amino acids **A,C,F,I,L,M & V**. :param append: {boolean} whether the produced descriptor values should be appended to the existing ones in the attribute :py:attr:`descriptor`. :return: array of descriptor values in the attribute :py:attr:`descriptor` :Example: >>> desc = GlobalDescriptor('VALLYWRTVLLAIII') >>> desc.hydrophobic_ratio() >>> desc.descriptor array([[ 0.73333333]]) """ desc = [] aa_dict = aa_weights() for seq in self.sequences: pa = {aa: seq.count(aa) for aa in aa_dict.keys()} # count aa # formula for calculating the AI (Ikai, 1980): desc.append( (pa["A"] + pa["C"] + pa["F"] + pa["I"] + pa["L"] + pa["M"] + pa["V"]) / float(len(seq)) ) desc = np.asarray(desc).reshape(len(desc), 1) if append: self.descriptor = np.hstack((self.descriptor, np.array(desc))) self.featurenames.append("HydrophRatio") else: self.descriptor = np.array(desc) self.featurenames = ["HydrophRatio"] def calculate_all(self, ph=7.4, amide=True): """Method combining all global descriptors and appending them into the feature matrix in the attribute :py:attr:`descriptor`. :param ph: {float} pH at which to calculate peptide charge :param amide: {boolean} whether the sequences have an amidated C-terminus. :return: array of descriptor values in the attribute :py:attr:`descriptor` :Example: >>> desc = GlobalDescriptor('AFGHFKLKKLFIFGHERT') >>> desc.calculate_all(amide=True) >>> desc.featurenames ['Length', 'MW', 'ChargeDensity', 'pI', 'InstabilityInd', 'Aromaticity', 'AliphaticInd', 'BomanInd', 'HydRatio'] >>> desc.descriptor array([[ 18., 2.17559000e+03, 1.87167619e-03, 1.16757812e+01, ... 1.10555556e+00, 4.44444444e-01]]) >>> desc.save_descriptor('/path/to/outputfile.csv') # save the descriptor data (with feature names header) """ # This is a strange way of doing it. However, the append=True option excludes length and charge, no idea why! fn = [] self.length() # sequence length l = self.descriptor fn.extend(self.featurenames) self.calculate_MW(amide=amide) # molecular weight mw = self.descriptor fn.extend(self.featurenames) self.calculate_charge(ph=ph, amide=amide) # net charge c = self.descriptor fn.extend(self.featurenames) self.charge_density(ph=ph, amide=amide) # charge density cd = self.descriptor fn.extend(self.featurenames) self.isoelectric_point(amide=amide) # pI pi = self.descriptor fn.extend(self.featurenames) self.instability_index() # instability index si = self.descriptor fn.extend(self.featurenames) self.aromaticity() # global aromaticity ar = self.descriptor fn.extend(self.featurenames) self.aliphatic_index() # aliphatic index ai = self.descriptor fn.extend(self.featurenames) self.boman_index() # Boman index bi = self.descriptor fn.extend(self.featurenames) self.hydrophobic_ratio() # Hydrophobic ratio hr = self.descriptor fn.extend(self.featurenames) self.descriptor = np.concatenate((l, mw, c, cd, pi, si, ar, ai, bi, hr), axis=1) self.featurenames = fn class PeptideDescriptor(BaseDescriptor): """Base class for peptide descriptors. The following **amino acid descriptor scales** are available for descriptor calculation: - **AASI** (An amino acid selectivity index scale for helical antimicrobial peptides, *[1] D. Juretić, D. Vukicević, N. Ilić, N. Antcheva, A. Tossi, J. Chem. Inf. Model. 2009, 49, 2873–2882.*) - **ABHPRK** (modlabs inhouse physicochemical feature scale (Acidic, Basic, Hydrophobic, Polar, aRomatic, Kink-inducer) - **argos** (Argos hydrophobicity amino acid scale, *[2] Argos, P., Rao, J. K. M. & Hargrave, P. A., Eur. J. Biochem. 2005, 128, 565–575.*) - **bulkiness** (Amino acid side chain bulkiness scale, *[3] J. M. Zimmerman, N. Eliezer, R. Simha, J. Theor. Biol. 1968, 21, 170–201.*) - **charge_phys** (Amino acid charge at pH 7.0 - Hystidine charge +0.1.) - **charge_acid** (Amino acid charge at acidic pH - Hystidine charge +1.0.) - **cougar** (modlabs inhouse selection of global peptide descriptors) - **eisenberg** (the Eisenberg hydrophobicity consensus amino acid scale, *[4] D. Eisenberg, R. M. Weiss, T. C. Terwilliger, W. Wilcox, Faraday Symp. Chem. Soc. 1982, 17, 109.*) - **Ez** (potential that assesses energies of insertion of amino acid side chains into lipid bilayers, *[5] A. Senes, D. C. Chadi, P. B. Law, R. F. S. Walters, V. Nanda, W. F. DeGrado, J. Mol. Biol. 2007, 366, 436–448.*) - **flexibility** (amino acid side chain flexibilitiy scale, *[6] R. Bhaskaran, P. K. Ponnuswamy, Int. J. Pept. Protein Res. 1988, 32, 241–255.*) - **grantham** (amino acid side chain composition, polarity and molecular volume, *[8] Grantham, R. Science. 185, 862–864 (1974).*) - **gravy** (GRAVY hydrophobicity amino acid scale, *[9] J. Kyte, R. F. Doolittle, J. Mol. Biol. 1982, 157, 105–132.*) - **hopp-woods** (Hopp-Woods amino acid hydrophobicity scale,*[10] T. P. Hopp, K. R. Woods, Proc. Natl. Acad. Sci. 1981, 78, 3824–3828.*) - **ISAECI** (Isotropic Surface Area (ISA) and Electronic Charge Index (ECI) of amino acid side chains, *[11] E. R. Collantes, W. J. Dunn, J. Med. Chem. 1995, 38, 2705–2713.*) - **janin** (Janin hydrophobicity amino acid scale, *[12] J. L. Cornette, K. B. Cease, H. Margalit, J. L. Spouge, J. A. Berzofsky, C. DeLisi, J. Mol. Biol. 1987, 195, 659–685.*) - **kytedoolittle** (Kyte & Doolittle hydrophobicity amino acid scale, *[13] J. Kyte, R. F. Doolittle, J. Mol. Biol. 1982, 157, 105–132.*) - **levitt_alpha** (Levitt amino acid alpha-helix propensity scale, extracted from http://web.expasy.org/protscale. *[14] M. Levitt, Biochemistry 1978, 17, 4277-4285.*) - **MSS** (A graph-theoretical index that reflects topological shape and size of amino acid side chains, *[15] C. Raychaudhury, A. Banerjee, P. Bag, S. Roy, J. Chem. Inf. Comput. Sci. 1999, 39, 248–254.*) - **MSW** (Amino acid scale based on a PCA of the molecular surface based WHIM descriptor (MS-WHIM), extended to natural amino acids, *[16] A. Zaliani, E. Gancia, J. Chem. Inf. Comput. Sci 1999, 39, 525–533.*) - **pepArc** (modlabs pharmacophoric feature scale, dimensions are: hydrophobicity, polarity, positive charge, negative charge, proline.) - **pepcats** (modlabs pharmacophoric feature based PEPCATS scale, *[17] C. P. Koch, A. M. Perna, M. Pillong, N. K. Todoroff, P. Wrede, G. Folkers, J. A. Hiss, G. Schneider, PLoS Comput. Biol. 2013, 9, e1003088.*) - **polarity** (Amino acid polarity scale, *[18] J. M. Zimmerman, N. Eliezer, R. Simha, J. Theor. Biol. 1968, 21, 170–201.*) - **PPCALI** (modlabs inhouse scale derived from a PCA of 143 amino acid property scales, *[19] C. P. Koch, A. M. Perna, M. Pillong, N. K. Todoroff, P. Wrede, G. Folkers, J. A. Hiss, G. Schneider, PLoS Comput. Biol. 2013, 9, e1003088.*) - **refractivity** (Relative amino acid refractivity values, *[20] T. L. McMeekin, M. Wilensky, M. L. Groves, Biochem. Biophys. Res. Commun. 1962, 7, 151–156.*) - **t_scale** (A PCA derived scale based on amino acid side chain properties calculated with 6 different probes of the GRID program, *[21] M. Cocchi, E. Johansson, Quant. Struct. Act. Relationships 1993, 12, 1–8.*) - **TM_tend** (Amino acid transmembrane propensity scale, extracted from http://web.expasy.org/protscale, *[22] Zhao, G., London E. Protein Sci. 2006, 15, 1987-2001.*) - **z3** (The original three dimensional Z-scale, *[23] S. Hellberg, M. Sjöström, B. Skagerberg, S. Wold, J. Med. Chem. 1987, 30, 1126–1135.*) - **z5** (The extended five dimensional Z-scale, *[24] M. Sandberg, L. Eriksson, J. Jonsson, M. Sjöström, S. Wold, J. Med. Chem. 1998, 41, 2481–2491.*) Further, amino acid scale independent methods can be calculated with help of the :class:`GlobalDescriptor` class. """ def __init__(self, seqs, scalename="Eisenberg"): """ :param seqs: a .fasta file with sequences, a list of sequences or a single sequence as string to calculate the descriptor values for. :param scalename: {str} name of the amino acid scale (one of the given list above) used to calculate the descriptor values :return: initialized attributes :py:attr:`sequences`, :py:attr:`names` and dictionary :py:attr:`scale` with amino acid scale values of the scale name in :py:attr:`scalename`. :Example: >>> AMP = PeptideDescriptor('KLLKLLKKLLKLLK','pepcats') >>> AMP.sequences ['KLLKLLKKLLKLLK'] >>> seqs = PeptideDescriptor('/Path/to/file.fasta', 'eisenberg') # load sequences from .fasta file >>> seqs.sequences ['AFDGHLKI','KKLQRSDLLRTK','KKLASCNNIPPR'...] """ super(PeptideDescriptor, self).__init__(seqs) self.scalename, self.scale = load_scale(scalename.lower()) self.all_moms = list() # for passing hydrophobic moments to calculate_profile self.all_globs = list() # for passing global to calculate_profile def load_scale(self, scalename): """Method to load amino acid values from a given scale :param scalename: {str} name of the amino acid scale to be loaded. :return: loaded amino acid scale values in a dictionary in the attribute :py:attr:`scale`. .. seealso:: :func:`modlamp.core.load_scale()` """ self.scalename, self.scale = load_scale(scalename.lower()) def calculate_autocorr(self, window, append=False): """Method for auto-correlating the amino acid values for a given descriptor scale :param window: {int} correlation window for descriptor calculation in a sliding window approach :param append: {boolean} whether the produced descriptor values should be appended to the existing ones in the attribute :py:attr:`descriptor`. :return: calculated descriptor numpy.array in the attribute :py:attr:`descriptor`. :Example: >>> AMP = PeptideDescriptor('GLFDIVKKVVGALGSL','PPCALI') >>> AMP.calculate_autocorr(7) >>> AMP.descriptor array([[ 1.28442339e+00, 1.29025116e+00, 1.03240901e+00, .... ]]) >>> AMP.descriptor.shape (1, 133) .. versionchanged:: v.2.3.0 """ desc = Parallel(n_jobs=-1)( delayed(_one_autocorr)(seq, window, self.scale) for seq in self.sequences ) if append: self.descriptor = np.hstack((self.descriptor, np.array(desc))) else: self.descriptor = np.array(desc) def calculate_crosscorr(self, window, append=False): """Method for cross-correlating the amino acid values for a given descriptor scale :param window: {int} correlation window for descriptor calculation in a sliding window approach :param append: {boolean} whether the produced descriptor values should be appended to the existing ones in the attribute :py:attr:`descriptor`. :return: calculated descriptor numpy.array in the attribute :py:attr:`descriptor`. :Example: >>> AMP = PeptideDescriptor('GLFDIVKKVVGALGSL','pepcats') >>> AMP.calculate_crosscorr(7) >>> AMP.descriptor array([[ 0.6875 , 0.46666667, 0.42857143, 0.61538462, 0.58333333, ... ]]) >>> AMP.descriptor.shape (1, 147) """ desc = Parallel(n_jobs=-1)( delayed(_one_crosscorr)(seq, window, self.scale) for seq in self.sequences ) if append: self.descriptor = np.hstack((self.descriptor, np.array(desc))) else: self.descriptor = np.array(desc) def calculate_moment(self, window=1000, angle=100, modality="max", append=False): """Method for calculating the maximum or mean moment of the amino acid values for a given descriptor scale and window. :param window: {int} amino acid window in which to calculate the moment. If the sequence is shorter than the window, the length of the sequence is taken. So if the default window of 1000 is chosen, for all sequences shorter than 1000, the **global** hydrophobic moment will be calculated. Otherwise, the maximal hydrophiobic moment for the chosen window size found in the sequence will be returned. :param angle: {int} angle in which to calculate the moment. **100** for alpha helices, **180** for beta sheets. :param modality: {'all', 'max' or 'mean'} Calculate respectively maximum or mean hydrophobic moment. If all, moments for all windows are returned. :param append: {boolean} whether the produced descriptor values should be appended to the existing ones in the attribute :py:attr:`descriptor`. :return: Calculated descriptor as a numpy.array in the attribute :py:attr:`descriptor` and all possible global values in :py:attr:`all_moms` (needed for the :py:func:`calculate_profile` method) :Example: >>> AMP = PeptideDescriptor('GLFDIVKKVVGALGSL', 'eisenberg') >>> AMP.calculate_moment() >>> AMP.descriptor array([[ 0.48790226]]) """ if self.scale["A"] == list: print( "\n Descriptor moment calculation is only possible for one dimensional descriptors.\n" ) else: desc = [] for seq in self.sequences: wdw = min( window, len(seq) ) # if sequence is shorter than window, take the whole sequence instead mtrx = [] mwdw = [] for aa in range(len(seq)): mtrx.append(self.scale[str(seq[aa])]) for i in range(len(mtrx) - wdw + 1): mwdw.append(sum(mtrx[i : i + wdw], [])) mwdw = np.asarray(mwdw) rads = ( angle * (np.pi / 180) * np.asarray(range(wdw)) ) # calculate actual moment (radial) vcos = (mwdw * np.cos(rads)).sum(axis=1) vsin = (mwdw * np.sin(rads)).sum(axis=1) moms = np.sqrt(vsin**2 + vcos**2) / wdw if modality == "max": # take window with maximal value moment = np.max(moms) elif modality == "mean": # take average value over all windows moment = np.mean(moms) elif modality == "all": moment = moms else: print( '\nERROR!\nModality parameter is wrong, please choose between "all", "max" and "mean".\n' ) return desc.append(moment) self.all_moms.append(moms) desc = np.asarray(desc).reshape(len(desc), 1) # final descriptor array if append: self.descriptor = np.hstack((self.descriptor, np.array(desc))) else: self.descriptor = np.array(desc) def calculate_global(self, window=1000, modality="max", append=False): """Method for calculating a global / window averaging descriptor value of a given AA scale :param window: {int} amino acid window in which to calculate the moment. If the sequence is shorter than the window, the length of the sequence is taken. :param modality: {'max' or 'mean'} Calculate respectively maximum or mean hydrophobic moment. :param append: {boolean} whether the produced descriptor values should be appended to the existing ones in the attribute :py:attr:`descriptor`. :return: Calculated descriptor as a numpy.array in the attribute :py:attr:`descriptor` and all possible global values in :py:attr:`all_globs` (needed for the :py:func:`calculate_profile` method) :Example: >>> AMP = PeptideDescriptor('GLFDIVKKVVGALGSL','eisenberg') >>> AMP.calculate_global(window=1000, modality='max') >>> AMP.descriptor array([[ 0.44875]]) """ desc = list() for n, seq in enumerate(self.sequences): wdw = min( window, len(seq) ) # if sequence is shorter than window, take the whole sequence instead mtrx = [] mwdw = [] for l in range(len(seq)): # translate AA sequence into values mtrx.append(self.scale[str(seq[l])]) for i in range(len(mtrx) - wdw + 1): mwdw.append( sum(mtrx[i : i + wdw], []) ) # list of all the values for the different windows mwdw = np.asarray(mwdw) glob = np.sum(mwdw, axis=1) / float(wdw) outglob = float() if modality in ["max", "mean"]: if modality == "max": outglob = np.max( glob ) # returned moment will be the maximum of all windows elif modality == "mean": outglob = np.mean( glob ) # returned moment will be the mean of all windows else: print( 'Modality parameter is wrong, please choose between "max" and "mean"\n.' ) return desc.append(outglob) self.all_globs.append(glob) desc = np.asarray(desc).reshape(len(desc), 1) if append: self.descriptor = np.hstack((self.descriptor, np.array(desc))) else: self.descriptor = np.array(desc) def calculate_profile(self, prof_type="uH", window=7, append=False): """Method for calculating hydrophobicity or hydrophobic moment profiles for given sequences and fitting for slope and intercept. The hydrophobicity scale used is "eisenberg" :param prof_type: prof_type of profile, available: 'H' for hydrophobicity or 'uH' for hydrophobic moment :param window: {int} size of sliding window used (odd-numbered). :param append: {boolean} whether the produced descriptor values should be appended to the existing ones in the attribute :py:attr:`descriptor`. :return: Fitted slope and intercept of calculated profile for every given sequence in the attribute :py:attr:`descriptor`. :Example: >>> AMP = PeptideDescriptor('KLLKLLKKVVGALG','kytedoolittle') >>> AMP.calculate_profile(prof_type='H') >>> AMP.descriptor array([[ 0.03731293, 0.19246599]]) """ if prof_type == "uH": self.calculate_moment(window=window) y_vals = self.all_moms elif prof_type == "H": self.calculate_global(window=window) y_vals = self.all_globs else: print( 'prof_type parameter is unknown, choose "uH" for hydrophobic moment or "H" for hydrophobicity\n.' ) sys.exit() desc = list() for n, seq in enumerate(self.sequences): x_vals = range(len(seq))[int((window - 1) / 2) : -int((window - 1) / 2)] if len(seq) <= window: slope, intercept, r_value, p_value, std_err = [0, 0, 0, 0, 0] else: slope, intercept, r_value, p_value, std_err = stats.linregress( x_vals, y_vals[n] ) desc.append([slope, intercept]) if append: self.descriptor = np.hstack((self.descriptor, np.array(desc))) else: self.descriptor = np.array(desc) def calculate_arc(self, modality="max", append=False): """Method for calculating property arcs as seen in the helical wheel plot. Use for binary amino acid scales only. :param modality: modality of the arc to calculate, to choose between "max" and "mean". :param append: if true, append to current descriptor stored in the descriptor attribute. :return: calculated descriptor as numpy.array in the descriptor attribute. :Example: >>> arc = PeptideDescriptor("KLLKLLKKLLKLLK", scalename="peparc") >>> arc.calculate_arc(modality="max", append=False) >>> arc.descriptor array([[200, 160, 160, 0, 0]]) """ desc = Parallel(n_jobs=-1)( delayed(_one_arc)(seq, modality, self.scale) for seq in self.sequences ) # Converts each of the amino acids to descriptor vector for seq in self.sequences: # desc_mat = [] # for aa in seq: # desc_mat.append(self.scale[aa]) # desc_mat = np.asarray(desc_mat) # # # Check descriptor dimension # desc_dim = desc_mat.shape[1] # # # list to store descriptor values for all windows # allwindows_arc = [] # # if len(seq) > 18: # window = 18 # # calculates number of windows in sequence # num_windows = len(seq) - window # else: # window = len(seq) # num_windows = 1 # # # loop through all windows # for j in range(num_windows): # # slices descriptor matrix into current window # window_mat = desc_mat[j:j + window, :] # # # defines order of amino acids in helical projection # order = [0, 11, 4, 15, 8, 1, 12, 5, 16, 9, 2, 13, 6, 17, 10, 3, 14, 7] # # # orders window descriptor matrix into helical projection order # ordered = [] # for pos in order: # try: # ordered.append(window_mat[pos, :]) # except: # # for sequences of len < 18 adding dummy vector with 2s, length of descriptor dimensions # ordered.append([2] * desc_dim) # ordered = np.asarray(ordered) # # window_arc = [] # # # loop through pharmacophoric features # for m in range(desc_dim): # all_arcs = [] # stores all arcs that can be found of a pharmacophoric feature # arc = 0 # # for n in range(18): # for all positions in helix, regardless of sequence length # if ordered[n, m] == 0: # if position does not contain pharmacophoric feature # all_arcs.append(arc) # append previous arc to all arcs list # arc = 0 # arc is initialized # elif ordered[n, m] == 1: # if position contains pharmacophoric feature(PF), elongate arc by 20° # arc += 20 # elif ordered[n, m] == 2: # if position doesn't contain amino acid: # if ordered[n - 1, m] == 1: # if previous position contained PF add 10° # arc += 10 # elif ordered[n - 1, m] == 0: # if previous position didn't contain PF don't add anything # arc += 0 # elif ordered[ # n - 2, m] == 1: # if previous position is empty then check second previous for PF # arc += 10 # if n == 17: # if we are at the last position check for position n=0 instead of next position. # if ordered[0, m] == 1: # if it contains PF add 10° extra # arc += 10 # else: # if next position contains PF add 10° extra # if ordered[n + 1, m] == 1: # arc += 10 # elif ordered[n + 1, m] == 0: # arc += 0 # else: # if next position is empty check for 2nd next position # if n == 16: # if ordered[0, m] == 1: # arc += 10 # else: # if ordered[n + 2, m] == 1: # arc += 10 # # all_arcs.append(arc) # if not arc == 360: # arc0 = all_arcs.pop() + all_arcs[0] # join first and last arc together # all_arcs = [arc0] + all_arcs[1:] # # window_arc.append(np.max(all_arcs)) # append to window arcs the maximum arc of this PF # allwindows_arc.append(window_arc) # append all PF arcs of this window # # allwindows_arc = np.asarray(allwindows_arc) # # if modality == 'max': # final_arc = np.max(allwindows_arc, axis=0) # calculate maximum / mean arc along all windows # elif modality == 'mean': # final_arc = np.mean(allwindows_arc, axis=0) # else: # print('modality is unknown, please choose between "max" and "mean"\n.') # sys.exit() if append: self.descriptor = np.hstack((self.descriptor, np.array(desc))) else: self.descriptor = np.array(desc)