NUPACK

Secondary structure model

The secondary structure of multiple interacting strands is defined by a list of base pairs. A polymer graph for a secondary structure can be constructed by ordering the strands around a circle, drawing the backbones in succession from 5’ to 3’ around the circumference with a nick between each strand, and drawing straight lines connecting paired bases. A secondary structure is pseudoknotted if every strand ordering corresponds to a polymer graph with crossing lines. A secondary structure is connected if no subset of the strands is free of the others. Algorithms are formulated in terms of ordered complexes, each corresponding to the structural ensemble of all connected polymer graphs with no crossing lines for a particular ordering of a set of strands. The free energy of an unpseudoknotted secondary structure is calculated using nearest-neighbor empirical parameters for RNA in 1M Na+ or for DNA in user-specified Na+ and Mg++ concentrations; added parameters are employed for the analysis of pseudoknots (single RNA strands only).

Analysis

The Analysis page allows users to analyze the thermodynamic properties of a dilute solution of interacting nucleic acid strands in the absence of pseudoknots (e.g., a test tube of DNA or RNA strand species). For a dilute solution containing multiple strand species interacting to form multiple species of ordered complexes, NUPACK calculates for each ordered complex:

including rigorous treatment of distinguishability issues that arise in the multi-stranded setting.

Design

The Design page allows users to design sequences for one or more strands intended to adopt an unpseudoknotted target secondary structure at equilibrium. Sequence design is formulated as an optimization problem with the goal of reducing the ensemble defect below a user-specified stop condition. For a candidate sequence and a given target secondary structure, the ensemble defect is the average number of incorrectly paired over the structural ensemble of the ordered complex. For a target secondary structure with N nucleotides, the algorithm seeks to achieve an ensemble defect below N/100. Empirically, the design algorithm exhibits asymptotic optimality as N increases: for sufficiently large N, the cost of sequence design is typically only 4/3 the cost of a single evaluation of the ensemble defect.

Utilities

The Utilities page allows users to evaluate, display, and annotate the equilibrium properties of a complex of interacting nucleic acid strands. The page accepts as input either sequence information, structure information, or both, performing diverse functions based on the information provided, including automatic layout and rendering of secondary structures with or without ideal helical geometry. In either case, the structure layout can be edited dynamically within the web application.

Implementation

The NUPACK web application is programmed within the Ruby on Rails framework, employing Ajax and the Dojo Toolkit to implement dynamic features and interactive graphics. Plots and graphics are generated using NumPy and matplotlib. The site is supported on current versions of the web browsers Safari, Chrome, and Firefox. The NUPACK library of analysis and design algorithms is written in the programming language C. Dynamic programs are parallelized using Message Passing Interface (MPI).

Terms of use

The NUPACK web server and NUPACK source code are provided for non-commercial research purposes and is with this restriction not Free and open source software.

Funding

NUPACK development is funded by the National Science Foundation via the Molecular Programming Project and by the Beckman Institute at the California Institute of Technology (Caltech).