Sindbis Virus: Difference between revisions

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=3. Genome structure=
=3. Genome structure=
Describe the size and content of the genome. How many chromosomes? Circular or linear? Other interesting features? What is known about its sequence?
The genome of SINV is a single-stranded positive sense RNA molecule (4). Among the 44 strains that have been sequenced, the genome ranges from 11-12 kilobases and is additionally capped at the 5' end and polyadenylated at the 3' end (4, 5, 6). The highest variance between SINV strains at the amino acid level was 22.2% and currently breaks down into 5 genotypic groups: SIN-I (Europe and Africa), SIN-II (Australia), SIN-III (East Asia), SIN-IV (Azerbaijan and China), and SIN-V (New Zealand) (7). The viral genome encodes mRNA for five structural proteins and four nonstructural proteins (2).
The small plaque, heat resistant strain of SINV has a genome that is 11,703 nucleotides long. The genome has 59 nucleotides of 5' untranslated regions from the 5’ cap (4). Following the 5’ untranslated region are 7539 nucleotides of open reading frame that encode nonstructural polypeptides (nsPs), nsP1, nsP2, nsP3, and nsP4, which are involved in transcription and translation of the viral genome (4). Two different polyprotein precursors can be produced from this part of the genome, either P123 or P1234 (Figure 1) (4, 8). The nonstructural proteins then work in the replication complex to create complementary RNAs in the process of viral genome replication (8, 9). Following the first open reading frame are 48 untranslated nucleotides located between the sequence encoding the nonstructural proteins and the structural proteins (4).
After the 48 untranslated nucleotides, the next 3735 nucleotides of the open reading frame encode structural proteins which are translated to a polypeptide precursor from the mRNA (4). This precursor is then processed through protein breakdown into the nucleocapsid protein, two integral membrane glycoproteins, and two small peptides (the last two are not found in the mature virus particle). These proteins are named capsid, E1 and E2, and E3 and 6K, respectively (4, 10). Found at the end are 322 nucleotides of the 3' untranslated region (4).
 
=4. Cell structure=
=4. Cell structure=
Interesting features of cell structure. Can be combined with “metabolic processes”
Interesting features of cell structure. Can be combined with “metabolic processes”

Revision as of 14:37, 6 December 2021

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1. Classification

Sindbis virus is a species that occupies human, invertebrate and vertebrate hosts (1).

Domain: Viruses; Realm: Riboviria; Kingdom: Orthornavirae; Phylum: Kitrinoviricota; Class: Alsuviricetes; Order: Martellivirales; Family: Togaviridae; Genus: Alphavirus

2. Introduction

Sindbis virus (SINV) is a disease-causing RNA virus transferred from animals to humans that is most often observed in Northern Europe and South Africa (2). The clinical infection of SINV is known as Pogosta disease in Finland, Ockelbo disease in Sweden, and Karelian fever in Russia. Symptoms of infection include joint pain, rash, fever, and myalgia; in many patients, these symptoms can continue for months or years and become debilitating (2). After diagnosis, there is no specific treatment available but pain management is typically used to alleviate symptoms through anti-inflammatory drugs (2). Potential cancer therapies have been developed using a viral vector of SINV to introduce specific genomic information into a host cell (3). However, it is unknown whether SINV vectors are effective in a clinical setting outside of a lab (2). It is also not yet well understood how host cells signal and respond to infection of SINV (2). Current research is focused on understanding the pathophysiology of SINV so that effective prevention and treatment methods for the virus can be developed (3), as well as expanding the phylogenetic tree of different SINV strains (4).

3. Genome structure

The genome of SINV is a single-stranded positive sense RNA molecule (4). Among the 44 strains that have been sequenced, the genome ranges from 11-12 kilobases and is additionally capped at the 5' end and polyadenylated at the 3' end (4, 5, 6). The highest variance between SINV strains at the amino acid level was 22.2% and currently breaks down into 5 genotypic groups: SIN-I (Europe and Africa), SIN-II (Australia), SIN-III (East Asia), SIN-IV (Azerbaijan and China), and SIN-V (New Zealand) (7). The viral genome encodes mRNA for five structural proteins and four nonstructural proteins (2). The small plaque, heat resistant strain of SINV has a genome that is 11,703 nucleotides long. The genome has 59 nucleotides of 5' untranslated regions from the 5’ cap (4). Following the 5’ untranslated region are 7539 nucleotides of open reading frame that encode nonstructural polypeptides (nsPs), nsP1, nsP2, nsP3, and nsP4, which are involved in transcription and translation of the viral genome (4). Two different polyprotein precursors can be produced from this part of the genome, either P123 or P1234 (Figure 1) (4, 8). The nonstructural proteins then work in the replication complex to create complementary RNAs in the process of viral genome replication (8, 9). Following the first open reading frame are 48 untranslated nucleotides located between the sequence encoding the nonstructural proteins and the structural proteins (4). After the 48 untranslated nucleotides, the next 3735 nucleotides of the open reading frame encode structural proteins which are translated to a polypeptide precursor from the mRNA (4). This precursor is then processed through protein breakdown into the nucleocapsid protein, two integral membrane glycoproteins, and two small peptides (the last two are not found in the mature virus particle). These proteins are named capsid, E1 and E2, and E3 and 6K, respectively (4, 10). Found at the end are 322 nucleotides of the 3' untranslated region (4).

4. Cell structure

Interesting features of cell structure. Can be combined with “metabolic processes”

5. Metabolic processes

Describe important sources of energy, electrons, and carbon (i.e. trophy) for the organism/organisms you are focusing on, as well as important molecules it/they synthesize(s).

6. Ecology

Habitat; symbiosis; contributions to the environment.

7. Pathology

How does this organism cause disease? Human, animal, plant hosts? Virulence factors, as well as patient symptoms.

8. Current Research

Include information about how this microbe (or related microbes) are currently being studied and for what purpose

9. References

It is required that you add at least five primary research articles (in same format as the sample reference below) that corresponds to the info that you added to this page. [Sample reference] Faller, A., and Schleifer, K. "Modified Oxidase and Benzidine Tests for Separation of Staphylococci from Micrococci". Journal of Clinical Microbiology. 1981. Volume 13. p. 1031-1035.