scholarly journals Implications of SARS-CoV-2 mutations for genomic RNA structure and host microRNA targeting

2020 ◽  
Author(s):  
Ali Hosseini Rad SM ◽  
Alexander D. McLellan
Keyword(s):  
Secondary Structure ◽  
Rna Structure ◽  
Rna Secondary Structure ◽  
Viral Fitness ◽  
Host Cells ◽  
Splice Sites ◽  
Genomic Rna ◽  
Zoonotic Pathogen ◽  
Viral Attenuation ◽  
The Impact

AbstractThe SARS-CoV-2 virus is a recently-emerged zoonotic pathogen already well adapted to transmission and replication in humans. Although the mutation rate is limited, recently introduced mutations in SARS-CoV-2 have the potential to alter viral fitness. In addition to amino acid changes, mutations could affect RNA secondary structure critical to viral life cycle, or interfere with sequences targeted by host miRNAs. We have analysed subsets of genomes from SARS-CoV-2 isolates from around the globe and show that several mutations introduce changes in Watson-Crick pairing, with resultant changes in predicted secondary structure. Filtering to targets matching miRNAs expressed in SARS-CoV-2 permissive host cells, we identified twelve separate target sequences in the SARS-CoV-2 genome; eight of these targets have been lost through conserved mutations. A genomic site targeted by the highly abundant miR-197-5p, overexpressed in patients with cardiovascular disease, is lost by a conserved mutation. Our results are compatible with a model that SARS-CoV-2 replication within the human host could be constrained by host miRNA defence. The impact of these and further mutations on secondary structures, miRNA targets or potential splice sites offers a new context in which to view future SARS-CoV-2 evolution, and a potential platform for engineered viral attenuation and antigen presentation.

scholarly journals Implications of SARS-CoV-2 Mutations for Genomic RNA Structure and Host microRNA Targeting

2020 ◽  
Vol 21 (13) ◽  
pp. 4807 ◽  
Author(s):  
Ali Hosseini Rad SM ◽  
Alexander D. McLellan
Keyword(s):  
Secondary Structure ◽  
Rna Structure ◽  
Rna Secondary Structure ◽  
Vaccine Development ◽  
Viral Fitness ◽  
Host Cells ◽  
Splice Sites ◽  
Genomic Rna ◽  
Zoonotic Pathogen ◽  
The Impact

The SARS-CoV-2 virus is a recently-emerged zoonotic pathogen already well adapted to transmission and replication in humans. Although the mutation rate is limited, recently introduced mutations in SARS-CoV-2 have the potential to alter viral fitness. In addition to amino acid changes, mutations could affect RNA secondary structure critical to viral life cycle, or interfere with sequences targeted by host miRNAs. We have analysed subsets of genomes from SARS-CoV-2 isolates from around the globe and show that several mutations introduce changes in Watson–Crick pairing, with resultant changes in predicted secondary structure. Filtering to targets matching miRNAs expressed in SARS-CoV-2-permissive host cells, we identified ten separate target sequences in the SARS-CoV-2 genome; three of these targets have been lost through conserved mutations. A genomic site targeted by the highly abundant miR-197-5p, overexpressed in patients with cardiovascular disease, is lost by a conserved mutation. Our results are compatible with a model that SARS-CoV-2 replication within the human host is constrained by host miRNA defences. The impact of these and further mutations on secondary structures, miRNA targets or potential splice sites offers a new context in which to view future SARS-CoV-2 evolution, and a potential platform for engineering conditional attenuation to vaccine development, as well as providing a better understanding of viral tropism and pathogenesis.

scholarly journals Amount of RNA secondary structure required to induce an alternative splice.

1987 ◽  
Vol 7 (9) ◽  
pp. 3194-3198 ◽  
Author(s):  
D Solnick ◽  
S I Lee
Keyword(s):  
Alternative Splicing ◽  
Secondary Structure ◽  
Alternative Splice ◽  
Rna Secondary Structure ◽  
Secondary Structures ◽  
Splice Sites ◽  
Perfect Complementarity ◽  
Set Up

We set up an alternative splicing system in vitro in which the relative amounts of two spliced RNAs, one containing and the other lacking a particular exon, were directly proportional to the length of an inverted repeat inserted into the flanking introns. We then used the system to measure the effect of intramolecular complementarity on alternative splicing in vivo. We found that an alternative splice was induced in vivo only when the introns contained more than approximately 50 nucleotides of perfect complementarity, that is, only when the secondary structure was much more stable than most if not all possible secondary structures in natural mRNA precursors. We showed further that intron insertions containing long complements to splice sites and a branch point inhibited splicing in vitro but not in vivo. These results raise the possibility that in cells most pre-mRNA secondary structures either are not maintained long enough to influence splicing choices, or never form at all.

Predicting RNA Secondary Structure Using a Improved BPSO Based on Stem Combination

2013 ◽  
Vol 325-326 ◽  
pp. 1551-1554
Author(s):  
Yi Qi
Keyword(s):  
Secondary Structure ◽  
Sensitivity And Specificity ◽  
Rna Structure ◽  
Structure Prediction ◽  
Rna Secondary Structure ◽  
Experimental Results ◽  
New Method ◽  
Rna Structure Prediction ◽  
New Strategies

In this paper, we present an improved BPSO to predict RNA secondary structure to improve the performance with two new strategies. First one is to reduce the searching space of PSO through super stem set construction. Second is to modify the general BPSO updating process to settle stem permutation and combination problems. The experimental results show that the new method is effective for RNA structure prediction in terms of sensitivity and specificity by different sequence datasets including simple pseudoknot.

scholarly journals Bioinformatic and Physical Characterizations of Genome-Scale Ordered RNA Structure in Mammalian RNA Viruses

2008 ◽  
Vol 82 (23) ◽  
pp. 11824-11836 ◽  
Author(s):  
Matthew Davis ◽  
Selena M. Sagan ◽  
John P. Pezacki ◽  
David J. Evans ◽  
Peter Simmonds
Keyword(s):  
Secondary Structure ◽  
Rna Structure ◽  
Rna Secondary Structure ◽  
Large Scale ◽  
Rna Viruses ◽  
Plant Viruses ◽  
Large Set ◽  
Conserved Sequence ◽  
Evolutionarily Conserved ◽  
Genome Scale

ABSTRACT By the analysis of thermodynamic RNA secondary structure predictions, we previously obtained evidence for evolutionarily conserved large-scale ordering of RNA virus genomes (P. Simmonds, A. Tuplin, and D. J. Evans, RNA 10:1337-1351, 2004). Genome-scale ordered RNA structure (GORS) was widely distributed in many animal and plant viruses, much greater in extent than RNA structures required for viral translation or replication, but in mammalian viruses was associated with host persistence. To substantiate the existence of large-scale RNA structure differences between viruses, a large set of alignments of mammalian RNA viruses and rRNA sequences as controls were examined by thermodynamic methods (to calculate minimum free energy differences) and by algorithmically independent RNAz and Pfold methods. These methods produced generally concordant results and identified substantial differences in the degrees of evolutionarily conserved, sequence order-dependent RNA secondary structure between virus genera and groups. A probe hybridization accessibility assay was used to investigate the physical nature of GORS. Transcripts of hepatitis C virus (HCV), hepatitis G virus/GB virus-C (HGV/GBV-C), and murine norovirus, which are predicted to be structured, were largely inaccessible to hybridization in solution, in contrast to the almost universal binding of probes to a range of unstructured virus transcripts irrespective of G+C content. Using atomic force microscopy, HCV and HGV/GBV-C RNA was visualized as tightly compacted prolate spheroids, while under the same experimental conditions the predicted unstructured poliovirus and rubella virus RNA were pleomorphic and had extensively single-stranded RNA on deposition. Bioinformatic and physical characterization methods both identified fundamental differences in the configurations of viral genomic RNA that may modify their interactions with host cell defenses and their ability to persist.

scholarly journals Quantitative high-throughput tests of ubiquitous RNA secondary structure prediction algorithms via RNA/protein binding

2019 ◽  
Author(s):  
Winston R. Becker ◽  
Inga Jarmoskaite ◽  
Kalli Kappel ◽  
Pavanapuresan P. Vaidyanathan ◽  
Sarah K. Denny ◽  
...  
Keyword(s):  
Secondary Structure ◽  
Protein Binding ◽  
Rna Structure ◽  
Structure Prediction ◽  
Rna Secondary Structure ◽  
Nearest Neighbor ◽  
Secondary Structure Prediction ◽  
Structural Features ◽  
Vast Number ◽  
Prediction Algorithms

AbstractNearest-neighbor (NN) rules provide a simple and powerful quantitative framework for RNA structure prediction that is strongly supported for canonical Watson-Crick duplexes from a plethora of thermodynamic measurements. Predictions of RNA secondary structure based on nearest-neighbor (NN) rules are routinely used to understand biological function and to engineer and control new functions in biotechnology. However, NN applications to RNA structural features such as internal and terminal loops rely on approximations and assumptions, with sparse experimental coverage of the vast number of possible sequence and structural features. To test to what extent NN rules accurately predict thermodynamic stabilities across RNAs with non-WC features, we tested their predictions using a quantitative high-throughput assay platform, RNA-MaP. Using a thermodynamic assay with coupled protein binding, we carried out equilibrium measurements for over 1000 RNAs with a range of predicted secondary structure stabilities. Our results revealed substantial scatter and systematic deviations between NN predictions and observed stabilities. Solution salt effects and incorrect or omitted loop parameters contribute to these observed deviations. Our results demonstrate the need to independently and quantitatively test NN computational algorithms to identify their capabilities and limitations. RNA-MaP and related approaches can be used to test computational predictions and can be adapted to obtain experimental data to improve RNA secondary structure and other prediction algorithms.Significance statementRNA secondary structure prediction algorithms are routinely used to understand, predict and design functional RNA structures in biology and biotechnology. Given the vast number of RNA sequence and structural features, these predictions rely on a series of approximations, and independent tests are needed to quantitatively evaluate the accuracy of predicted RNA structural stabilities. Here we measure the stabilities of over 1000 RNA constructs by using a coupled protein binding assay. Our results reveal substantial deviations from the RNA stabilities predicted by popular algorithms, and identify factors contributing to the observed deviations. We demonstrate the importance of quantitative, experimental tests of computational RNA structure predictions and present an approach that can be used to routinely test and improve the prediction accuracy.

scholarly journals Clinico-Genomic Analysis Reveals Mutations Associated with COVID-19 Disease Severity: Possible Modulation by RNA Structure

Pathogens ◽  
2021 ◽  
Vol 10 (9) ◽  
pp. 1109
Author(s):  
Priyanka Mehta ◽  
Shanmukh Alle ◽  
Anusha Chaturvedi ◽  
Aparna Swaminathan ◽  
Sheeba Saifi ◽  
...  
Keyword(s):  
Rna Structure ◽  
Rna Secondary Structure ◽  
Clinical Phenotype ◽  
Genomic Analysis ◽  
Medical Support ◽  
N Protein ◽  
Protein Levels ◽  
Genetic Components ◽  
Clinical Presentations ◽  
The Impact

Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) manifests a broad spectrum of clinical presentations, varying in severity from asymptomatic to mortality. As the viral infection spread, it evolved and developed into many variants of concern. Understanding the impact of mutations in the SARS-CoV-2 genome on the clinical phenotype and associated co-morbidities is important for treatment and preventionas the pandemic progresses. Based on the mild, moderate, and severe clinical phenotypes, we analyzed the possible association between both, the clinical sub-phenotypes and genomic mutations with respect to the severity and outcome of the patients. We found a significant association between the requirement of respiratory support and co-morbidities. We also identified six SARS-CoV-2 genome mutations that were significantly correlated with severity and mortality in our cohort. We examined structural alterations at the RNA and protein levels as a result of three of these mutations: A26194T, T28854T, and C25611A, present in the Orf3a and N protein. The RNA secondary structure change due to the above mutations can be one of the modulators of the disease outcome. Our findings highlight the importance of integrative analysis in which clinical and genetic components of the disease are co-analyzed. In combination with genomic surveillance, the clinical outcome-associated mutations could help identify individuals for priority medical support.

scholarly journals RNA Secondary Structurome Revealed Distinct Thermoregulation in Plasmodium falciparum

2022 ◽  
Vol 9 ◽  
Author(s):  
Yanwei Qi ◽  
Yuhong Zhang ◽  
Quankai Mu ◽  
Guixing Zheng ◽  
Mengxin Zhang ◽  
...  
Keyword(s):  
Plasmodium Falciparum ◽  
Secondary Structure ◽  
Rna Structure ◽  
Rna Secondary Structure ◽  
Structural Changes ◽  
Environmental Changes ◽  
Parasite Development ◽  
Temperature Dependent ◽  
Trophozoite Stage ◽  
Temperature Changes

The development of Plasmodium parasites, a causative agent of malaria, requests two hosts and the completion of 11 different parasite stages during development. Therefore, an efficient and fast response of parasites to various complex environmental changes, such as ambient temperature, pH, ions, and nutrients, is essential for parasite development and survival. Among many of these environmental changes, temperature is a decisive factor for parasite development and pathogenesis, including the thermoregulation of rRNA expression, gametogenesis, and parasite sequestration in cerebral malaria. However, the exact mechanism of how Plasmodium parasites rapidly respond and adapt to temperature change remains elusive. As a fundamental and pervasive regulator of gene expression, RNA structure can be a specific mechanism for fine tuning various biological processes. For example, dynamic and temperature-dependent changes in RNA secondary structures can control the expression of different gene programs, as shown by RNA thermometers. In this study, we applied the in vitro and in vivo transcriptomic-wide secondary structurome approach icSHAPE to measure parasite RNA structure changes with temperature alteration at single-nucleotide resolution for ring and trophozoite stage parasites. Among 3,000 probed structures at different temperatures, our data showed structural changes in the global transcriptome, such as S-type rRNA, HRPII gene, and the erythrocyte membrane protein family. When the temperature drops from 37°C to 26°C, most of the genes in the trophozoite stage cause significantly more changes to the RNA structure than the genes in the ring stage. A multi-omics analysis of transcriptome data from RNA-seq and RNA structure data from icSHAPE reveals that the specific RNA secondary structure plays a significant role in the regulation of transcript expression for parasites in response to temperature changes. In addition, we identified several RNA thermometers (RNATs) that responded quickly to temperature changes. The possible thermo-responsive RNAs in Plasmodium falciparum were further mapped. To this end, we identified dynamic and temperature-dependent RNA structural changes in the P. falciparum transcriptome and performed a comprehensive characterization of RNA secondary structures over the course of temperature stress in blood stage development. These findings not only contribute to a better understanding of the function of the RNA secondary structure but may also provide novel targets for efficient vaccines or drugs.

scholarly journals Pervasive RNA Secondary Structure in the Genomes of SARS-CoV-2 and Other Coronaviruses

mBio ◽  
2020 ◽  
Vol 11 (6) ◽  
Author(s):  
P. Simmonds
Keyword(s):  
Secondary Structure ◽  
Rna Structure ◽  
Rna Secondary Structure ◽  
Large Scale ◽  
Rna Viruses ◽  
Shielding Effect ◽  
Cellular Interactions ◽  
Folding Energy ◽  
Base Pairing ◽  
Positive Strand Rna

ABSTRACT The ultimate outcome of the coronavirus disease 2019 (COVID-19) pandemic is unknown and is dependent on a complex interplay of its pathogenicity, transmissibility, and population immunity. In the current study, severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) was investigated for the presence of large-scale internal RNA base pairing in its genome. This property, termed genome-scale ordered RNA structure (GORS) has been previously associated with host persistence in other positive-strand RNA viruses, potentially through its shielding effect on viral RNA recognition in the cell. Genomes of SARS-CoV-2 were remarkably structured, with minimum folding energy differences (MFEDs) of 15%, substantially greater than previously examined viruses such as hepatitis C virus (HCV) (MFED of 7 to 9%). High MFED values were shared with all coronavirus genomes analyzed and created by several hundred consecutive energetically favored stem-loops throughout the genome. In contrast to replication-associated RNA structure, GORS was poorly conserved in the positions and identities of base pairing with other sarbecoviruses—even similarly positioned stem-loops in SARS-CoV-2 and SARS-CoV rarely shared homologous pairings, indicative of more rapid evolutionary change in RNA structure than in the underlying coding sequences. Sites predicted to be base paired in SARS-CoV-2 showed less sequence diversity than unpaired sites, suggesting that disruption of RNA structure by mutation imposes a fitness cost on the virus that is potentially restrictive to its longer evolution. Although functionally uncharacterized, GORS in SARS-CoV-2 and other coronaviruses represents important elements in their cellular interactions that may contribute to their persistence and transmissibility. IMPORTANCE The detection and characterization of large-scale RNA secondary structure in the genome of SARS-CoV-2 indicate an extraordinary and unsuspected degree of genome structural organization; this could be effectively visualized through a newly developed contour plotting method that displays positions, structural features, and conservation of RNA secondary structure between related viruses. Such RNA structure imposes a substantial evolutionary cost; paired sites showed greater restriction in diversity and represent a substantial additional constraint in reconstructing its molecular epidemiology. Its biological relevance arises from previously documented associations between possession of structured genomes and persistence, as documented for HCV and several other RNA viruses infecting humans and mammals. Shared properties potentially conferred by large-scale structure in SARS-CoV-2 include increasing evidence for prolonged infections and induced immune dysfunction that prevents development of protective immunity. The findings provide an additional element to cellular interactions that potentially influences the natural history of SARS-CoV-2, its pathogenicity, and its transmission.

DSARna: RNA Secondary Structure Alignment Based on Digital Sequence Representation

2020 ◽  
Vol 23 ◽  
Author(s):  
Longjian Gao ◽  
Chengzhen Xu ◽  
Wangan Song ◽  
Feng Xiao ◽  
Xiaomin Wu ◽  
...  
Keyword(s):  
Secondary Structure ◽  
Rna Structure ◽  
Rna Secondary Structure ◽  
High Throughput Sequencing ◽  
Structural Information ◽  
Dynamic Programming Algorithm ◽  
Structure Alignment ◽  
Programming Algorithm ◽  
Structure Information ◽  
Alignment Algorithms

Background: With increasing applications and development of high-throughput sequencing, knowledge of the primary structure of RNA has expanded exponentially. Moreover, the function of RNA is determined by the secondary or higher RNA structure, and similar structures are related to similar functions, such as the secondary clover structure of tRNA. Therefore, RNA structure alignment is an important subject in computational biology and bioinformatics to accurately predict function. However, the traditional RNA structure alignment algorithms have some drawbacks such as high complexity and easy loss of secondary structure information. Objective: To study RNA secondary structure alignment according to the shortcomings of existing secondary structure alignment algorithms and the characteristics of RNA secondary structure. Method: We propose a new digital sequence RNA structure representation algorithm named “DSARna” . Then based on a dynamic programming algorithm, the scoring matrix and binary path matrix are simultaneously constructed. The backtracking path is identified in the path matrix, and the optimal result is predicted according to the path length. Conclusions: Upon comparison with the existing SimTree algorithm through experimental analysis, the proposed method showed higher accuracy and could ensure that the structural information is not easily lost in terms of improved specificity, sensitivity, and the Matthews correlation coefficient.

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