Structural Biology Software Database
Application IndexSort by [ Name | Last Update ]
| Category: Protein Structure Analysis and Verification (35 entries) | | This is a collection of analysis tools for protein such as 3-D structure comparison, binding site identification, noncovalent bond finder, dimensions of pore of an ion channel etc. |
| 123D | 123D is a web-based program which combines substitution matrix, secondary structure prediction, and contact capacity potentials to thread a sequence throught the set of structures.
View Application Entry for 123D |
| ANALYZE | ANALYZE is free program which can analyze conformations obtained from global searches. It includes capabability to compare NMR intensites and coupling constants to experimental data. ANALYZE has been tested on IBM, IBM SP2, SUN workstations and Pentium machines running RedHat Linux. The program does not run well on SGI platforms.
View Application Entry for ANALYZE |
| CATH | CATH is a novel hierarchical classification of protein domain structures, which clusters proteins at four major levels, class(C), architecture(A), topology(T) and homologous superfamily (H). Class, derived from secondary structure content, is assigned for more than 90% of protein structures automatically. Architecture, which describes the gross orientation of secondary structures, independent of connectivities, is currently assigned manually. The topology level clusters structures according to their toplogical connections and numbers of secondary structures. The homologous superfamilies cluster proteins with highly similar structures and functions. The assignments of structures to toplogy families and homologous superfamilies are made by sequence and structure comparisons.
View Application Entry for CATH |
| CE/CL | CE and CL are web-based software for 3-D structure comparison and alignment by Combinatorial Extension (CE) and by Compound Likeness (CL) respectively.
View Application Entry for CE/CL |
| COMPOSER | COMPOSER module provides the tools needed for knowledge-based homology modeling of protein structures. Based on the program developed by Professor Thomas Blundell and colleagues at Birkbeck College, England, Composer uses both sequence and structural information from known families of proteins to predict the 3D structure of an unknown. It is especially useful for extracting all the structural information resident in the members of a family of homologs, and has been shown to build complete, accurate models for proteins with as low as 30% sequence homology. Composer has been shown to generate more complete, accurate models than many of its competitors. Composer is integrated into the SYBYL Molecular Modeling Environment and requires both SYBYL/Base and Biopolymer modules. Analysis of resulting models is enhanced and simplified by the ProTable module. The new GeneFold module uses Composer to build model proteins based on sequence threading technologies.
View Application Entry for COMPOSER |
| CONCOORD | CONCOORD is a method to generate protein conformations around a known structure based on distance restrictions. Principal component analyses of Molecular Dynamics (MD) simulations of proteins have indicated that collective degrees of freedom dominate protein conformational fluctuations. These large-scale collective motions have been shown essential to protein function in a number of cases. The notion that internal constraints and other configurational barriers restrict protein dynamics to a limited number of collective degrees of freedom has led to the design of the CONCOORD method to predict these modes without doing explicit, more CPU intensive, MD simulations.
View Application Entry for CONCOORD |
| Dyndom | Dyndom is a program that determines protein domains, hinge axes and amino acid residues involved in the hinge bending motion. It requires two conformations to perform this task. It is fully automated and applicable to multi-domain proteins.
View Application Entry for Dyndom |
| ECEPPAK | ECEPPAK is a free software which can perform the following calculations:
- Single Energy Evaluation
- Single Energy Minimization
- Energy evaluation of Multiple Input Conformations
- Energy Minimization of Multiple Input Conformations
- Monte Carlo Search using a generalized MCM (EDMC) algorithm.
- PRODUCE an energy map for a pair of dihedral angles.
- Carry out an rms deviations analysis.
- Variable Target Function Procedure for structure determination
It is available on IBM RS/6000 and SP, SGI.
View Application Entry for ECEPPAK |
| ESPript (Easy Sequencing in Postscript) | ESPript is a utility to generate a pretty PostScript output from aligned sequences. Its main input is an ASCII file of pre-aligned sequences. Optional files allow further rendering. The program calculates a similarity score for each residue of the aligned sequences. The program can also be run via the web site.
View Application Entry for ESPript (Easy Sequencing in Postscript) |
| HOLE | HOLE was written at Birkbeck College from April 1992 to allow the visualization and analysis of the holes through atomic models of ion channels. A
number of people have suggested that it may prove to be useful to other scientists working on ion channel models and it is being publicly distributed with
that hope. Its initial application is to four experimentally determined structures of gramicidin A.
View Application Entry for HOLE |
| IMCLite | IMCLite is a Molecular graphics program supporting manual docking, interactive model building, structure analysis and comparison. It is vailable for most UNIX systems, LINUX and WinNT.
View Application Entry for IMCLite |
| LOOPP (Learning, Observing and Outputting Protein Patterns) | LOOPP is a free program for PROTEIN RECOGNITION and design of PROTEIN FOLDING potentials. LOOPP (Learning, Observing and Outputting Protein Patterns) evolved from the previous LOOPP (Linear Optimization of Protein Potentials). As suggested by the new/old name there is some continuity, but there are also many new features. LOOPP is available on IBM RS/6000 and SP, Windows NT (to be run from a command prompt - no graphical interface), SGI, SUN SOLARIS and LINUX.
View Application Entry for LOOPP (Learning, Observing and Outputting Protein Patterns) |
| MaxSprout | MaxSprout is a fast database algorithm for generating protein backbone and side chain co-ordinates from a C(alpha) trace. The backbone is assembled from fragments taken from known structures. Side chain conformations are optimized in rotamer space using a rough potential energy function to avoid clashes.
View Application Entry for MaxSprout |
| MINT | MINT is a graphical user interface to Andrej Sali Modeller program. It allows only the basic homology modelling
functions of Modeller to be used, but saves you from having to use the Modeller control language. The latest MINT
V3.0 is compatible with the latest version of Modeller known as Modeller-3.
MINT is written in Tcl/Tk. It provides you with a simple GUI where you enter the name of your sequence file, the
PDB codes being used as parents and optionallay an alignment file. A limited number of additional parameters may
also be set. You then simply click the Run button to write a Modeller control file and spawn the Modeller program.
MINT is freely available for use by not-for-profit organisations. Commercial use is not permitted without
express permission from the author. It may not be distributed without the author permission, but must be
obtained from the site. It is supplied as a gzipped tar file of Tcl/Tk code.
View Application Entry for MINT |
| MolSurfer | MolSurfer is a tool that provides two-dimensional maps of protein interfaces that can be used to explore three-dimensional structures of protein complexes and their interfaces.
View Application Entry for MolSurfer |
| Mol_Volume | This program calculates the volume of a macromolecule by a method somewhat akin to the Monte Carlo method, namely, by measuring how many vertices of a dense regular grid happen to be within the probe radius of the molecular atoms. The Volume is then calculated as
V = V_grid * N_near / N_total = N_near * V_per_node.
View Application Entry for Mol_Volume |
| Mpex (Membrane Protein Explorer) | Mpex is a java based program that can be used to analyze membrone protein sequences for possible trans membrane sequences.
The program can also calculate the free energies of partitioning of a protein between water/octanol as well as water/membrane-interface
Also. it can be used to draw helical wheel diagrams.
View Application Entry for Mpex (Membrane Protein Explorer) |
| PDBtool | PDBtool supports the browsing querying and verification (mainly geometry) of macromolecular structure data as found in files from the Protein Data Back (PDB).
View Application Entry for PDBtool |
| PROCHECK | PROCHECK is a program that checks the stereochemical quality of a protein structure. It is free and is available for Unix or Windows NT.
View Application Entry for PROCHECK |
| PROTARCH | PROTARCH is a free system of programs for hierarchical prediction of protein structure based on the thermodynamic hypothesis. At present three hardware platforms are supported: IBM SP2, Linux and MS Windows NT/2000.
View Application Entry for PROTARCH |
| SARF (Spatial ARrangement of backbone Fragments) | SARF is a free program which searches for similar structural motifs in protein structures via an analysis of backbone fragments. If the two proteins are in the PDB then the program can also be run directly from the website. Otherwise it has to be downloaded to your local machine. PLATFORM : SGI or DEC computer; If the two proteins are in the PDB then it can be run directly from any computer having a web browser.
View Application Entry for SARF (Spatial ARrangement of backbone Fragments) |
| SQUID | SQUID is a software for the analysis of protein structures and molecular dynamics simulations. It is free for academic research. The program can be installed onon an SGI on IRIX6.2 an higher or on a PC running Linux.
View Application Entry for SQUID |
| SSBOND | SSBOND predicts locations where disulphide bonds can be introduced in proteins
of known structure. It generates a list of pairs of residues that, if mutated
to cysteines, will form proper disulphide bonds. The program will list the
dihedral angles that describe the disulfide bond conformation and an energy
estimate of the strain that is introduced.
View Application Entry for SSBOND |
| SURFNET | The SURFNET program generates surfaces and void regions between surfaces from coordinate data supplied in a PDB file. It can computevan der Waals surfaces, gaps between molecules, Clefts, cavities and binding sites, 3D density distributions and sidechain-sidechain interactions. This program is available free to academic institutions.
View Application Entry for SURFNET |
| TOP (protein TOPological comparison program) | TOP is a free program which compares protein structures and performs 3d database search. The program is written in standard FORTRAN 77 so in principle the executable code can be installed on any computers with FORTRAN compiler, hing via Internet. A server system has also been built up for running the program via Web.
View Application Entry for TOP (protein TOPological comparison program) |
| TORSIONS | TORSIONS is a simple program to read a PDB file and calculate backbone torsion angles. It calculates phi, psi and
omega and can also calculate C-alpha pseudo-torsions.
View Application Entry for TORSIONS |
| TRITON | TRITON is graphical tool for modelling protein mutants and assessment of their activities. Protein mutants are modelled based on the wild type structure by homology modelling using the external program MODELLER. Chemical reactions taking place in the mutants active site are modelled using the semi-empirical quantum mechanic program MOPAC. Semi-quantitative predictions of mutants activities can be achieved by evaluating the changes in energies of the system and partial atomic charges of the active site residues during the reaction. The program TRITON offers graphical tools for the preparation of the input data files, for calculation and for the analysis of the generated output data. Implementation ensures the overall integrity of consecutive steps of the modelling of mutants and calculation of reaction coordinates, but the program can also be used simply for combinatorial generation of multiple mutants by homology modelling.
View Application Entry for TRITON |
| VAST (Vector Alignment Search Tool) | VAST Search is structure-structure similarity search service of NCBI. It compares 3D coordinates of a newly determined protein structure to those in the MMDB/PDB database. VAST Search computes a list of structure neighbors that you may browse interactively, viewing superpositions and alignments by molecular graphics.
View Application Entry for VAST (Vector Alignment Search Tool) |
| WHAT IF | WHAT IF is a versatile protein structure analysis program that can be used for mutant prediction, structure verification, molecular graphics, etc. It is available commercially for unix and windows users.
View Application Entry for WHAT IF |
| WHAT_CHECK | WHAT_CHECK is a system for protein structure validation derived from the WHAT IF program. This program is available for free and can be used on Silicon Graphics machine or DEC ALPHA running OSF/1.
View Application Entry for WHAT_CHECK |
Submit a new application to the database moderatorsThis page generated by SoftDB, developed by the Theoretical Biophysics Group at the University of Illinois.
Please contact biosoftdb@ks.uiuc.edu with questions or suggestions.
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