Metadata-Version: 2.1
Name: biobrigit
Version: 0.0.7
Summary: Computational tool for the prediction of metal-binding loading paths in proteins using deep convolutional neural networks.
Home-page: https://github.com/insillichem/BioBrigit
Author: Raúl Fernández Díaz
Author-email: raul.fernandezdiaz@ucdconnect.ie
License: BSD license
Keywords: biobrigit
Requires-Python: >=3.6
Description-Content-Type: text/markdown
License-File: LICENSE
License-File: AUTHORS.rst
Requires-Dist: scikit-learn
Requires-Dist: torch
Requires-Dist: moleculekit
Requires-Dist: lightning
Requires-Dist: pdb2pqr

BioBrigit
===============

BioBrigit is a computational tool designed for the prediction of metal diffusion pathways through a protein. It uses a novel scoring function that combines deep learning and previous domain knowledge regarding bioinorganic interactions as described in [Sánchez-Aparicio et al. (2017)](https://chemrxiv.org/engage/chemrxiv/article-details/60c74de1469df46a86f44378). The deep learning part of our hybrid approach consists on a 3D Convolutional Neural Network trained to interpret the biochemical environment to distinguish between metal-binding and non-binding protein regions.
 
<picture>
  <source media="(prefers-color-scheme: dark)" srcset="https://raw.githubusercontent.com/RaulFD-creator/biobrigit/master/docs/figures/BioBrigit_dark_border.png" width="850" class="center">
  <source media="(prefers-color-scheme: light)" srcset="https://raw.githubusercontent.com/RaulFD-creator/biobrigit/master/docs/figures/BioBrigit_light.png" width="850" class="center">
  <img alt="Shows an stylised anvil with a neural network upon it." src=""https://raw.githubusercontent.com/RaulFD-creator/biobrigit/master/docs/figures/BioBrigit_light.png">
</picture>


Features
--------
**Diferent options for customizing the search:**

* Search for the paths of specific metals.
* Provide a score that indicates how strong the protein-metal interaction will be in different positions.
* Scan the whole protein or only a region (in PDB format).

**Possible applications:**

* Identification of probable metal diffusion pathways through a protein.
* Identification of conformational changes that alter the formation of such paths.
* Metalloenzyme and metallodrug design.
* Aid in developing hypothesis in molecular physiopathology.
* Drug discovery.

**Modular design:**

* The modular design of this package allows for its use as a command-line application or to be integrated into a larger Python program or pipeline. In the [script](https://github.com/insilichem/BioBrigit/tree/main/scripts) directory are some of examples on how to integrate the program within a wider pipeline.

Installation
------------

It can be directly installed in any conda environment by

```bash
conda create -n biobrigit python
conda activate biobrigit
pip install biobrigit
```


Usage
-----
Once the environment is properly set-up the use of the program is relatively simple. The easiest example is:

```bash
biobrigit target metal
```

There are many parameters that can be also tuned, though default use is reccomended.

* `--model`: Which CNN model is to be used. Two options are currently available: `BrigitCNN` which is the default model and `TinyBrigit`, which is a smaller model for improved computational efficiency, though it has lower accuracy.
* `--device`: Whether to use GPU acceleration (`cuda`) or not (`cpu`). By default, it uses GPU if available.
* `--device_id`: Which of the available GPU devices should be used for the calculations in case that there are more than one GPU available. By default, it uses the device labelled as 0.
* `--outputfile`: Name of the outputfiles. The file extensions (`.txt` and `.pdb`) will be added automatically.
* `--max_coordinators`: Number of maximum coordinators expected. By default, 2. It only affects the range of values assigned to the probes.
* `--residues`: Number of most likely coordinating residues. By default, 10.
* `--stride`: Step at which the voxelized representation of the protein should be parsed. By default, 1. The greater the stride, the greater the computational efficiency; however, the resolution of the predictions will be affected.
* `--cluster_radius`: Radius of the clusters to be generated in armstrongs. By default, 5.
* `--cnn_threshold`: Threshold for considering CNN points as possible coordinations. Lower values will impact computational efficiency; greater values, may hide possible coordinating regions. By default, 0.5. Values should be within the range [0, 1].
* `--combined_threshold`: Threshold for considering predictions combining BioMetAll and CNN scores as positive. By default, 0.5. Values should be within the range [0, 1].
* `--threads`: Number of threads available for multithreading calculation. By default it will create 2 threads per physical core.
* `--verbose`: Information that will be displayed. 0: Only Moleculekit, 1: All. By default, 1.
* `--residue score`: Scoring function for residue coordination analysis. Can be either `discrete`, that only considers how likely is a residue to bind to a certain metal (more computationally efficient); or `gaussian`, that also considers the fitness of the geometrical descriptors for a certain residue and metal. By default, `gaussian`.

The following parameters can also be tuned, but their modification is **not** reccomended as it may translate in unreliable predictions.
* `--cnn_weight`: Importance of the CNN score in the final score in relations to the BioMetAll score. By default, 0.5. Values should be within the range [0, 1].
* `--voxelsize`: Resolution of the 3D representation. In Arnstrongs. By default, 1 A.
* `--pH`: pH of the medium at which the structure is to be evaluated. By default, 7.4.

**Examples:**

Searching for copper.

```bash
biobrigit 1dhy Cu
```

Searching with generic metal.

```bash
biobrigit 1dhy generic
```

Searching for multiple metals simultanously.

```bash
biobrigit 1dhy fe,generic
```

Fast preliminar exploration for binding sites with 4 coordinations, no GPU, and only considering the 4 most likely coordinating residues.

```bash
biobrigit 1dhy Cu --stride 2 --model TinyBrigit --max_coordinators 4 --device cpu --residues 4
```

Search for small clusters at acidic pH (5.2).

```bash
biobrigit 1dhy Cu --cluster_radius 3 --pH 5.2
```

Output
------
The program generates 2 output files. 

1. A `.txt` file that contains information regarding the clusters of probes ordered by the predicted strength of the interaction between protein and metal. This file also displays a list of possible coordinating residues. 
2. A `.pdb` file that contains the coordinates of all probes with a score greater than `combined_threshold` and is the recommended output format for visualizing the predicted paths. The probes are represented as He atoms and the centers of their clusters as Ar atoms. To easily visualise the score for each probe, simply colour the probes by their $\beta$-factor using your protein visualization tool of choice.

License
-------
BioBrigit is an open-source software licensed under the BSD-3 Clause License. Check the details in the [LICENSE](https://github.com/raulfd-creator/biobrigit/blob/master/LICENSE) file.

Documentation
-------------
More information in the official documentation, [here](https://github.com/insilichem/BioBrigit/blob/main/docs/UsersGuide.pdf).


History of versions
-------------------
* **v.0.0.1:** First operative release version.

OS Compatibility
----------------
BioBrigit is currently only compatible with Linux, due to some of its dependencies.

If you find some dificulties when installing it in a concrete distribution, please use the issues page to report them.

Credits
-------

This package was created with [Cookiecutter](https://github.com/audreyr/cookiecutter) and the [audreyr/cookiecutter-pypackage](https://github.com/audreyr/cookiecutter-pypackage) project template. 

Special thanks to [Silvia González López](https://www.linkedin.com/in/silvia-gonz%C3%A1lez-l%C3%B3pez-717558221/) for designing the BioBrigit logo.
