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Cat# | Product Name | Swiss Prot# | Size | Price (US$) | Order |
PN0269 | Recombinant Protein-Coxsackievirus A16 Protein VP0 (a.a.2 to 323) | Q9QF31 | 100 µg | 1195 | |
PN0270 | Recombinant Protein-Coxsackievirus A16 Protein VP2 (a.a.70 to 323) | Q9QF31 | 100 µg | 1195 | |
PN0271 | Recombinant Protein-Coxsackievirus A16 Protein VP3 (a.a.324 to 565) | Q9QF31 | 100 µg | 1195 | |
PN0272 | Recombinant Protein-Coxsackievirus A16 Protein VP1 (a.a.591 to 862) | Q9QF31 | 100 µg | 1195 | |
PN0273 | Recombinant Protein-Coxsackievirus A16 Picornain 2A (a.a.863 to 1012) | Q9QF31 | 100 µg | 1195 | |
PN0274 | Recombinant Protein-Coxsackievirus A16 Protein 2C (a.a.1112 to 1440) | Q9QF31 | 100 µg | 1195 | |
PN0275 | Recombinant Protein-Coxsackievirus A16 Picornain 3C (a.a.1549 to 1731) | Q9QF31 | 100 µg | 1195 | |
PN0276 | Recombinant Protein-Coxsackievirus A21 Protein VP2 (a.a.70 to 341) | P22055 | 100 µg | 1195 | |
PN0277 | Recombinant Protein-Coxsackievirus A21 Protein VP3 (a.a.361 to 581) | P22055 | 100 µg | 1195 | |
PN0278 | Recombinant Protein-Coxsackievirus A21 Protein VP1 (a.a.593 to 879) | P22055 | 100 µg | 1195 | |
PN0279 | Recombinant Protein-Coxsackievirus A21 Picornain 2A (a.a.880 to 1028) | P22055 | 100 µg | 1195 | |
PN0280 | Recombinant Protein-Coxsackievirus A21 Picornain 3C (a.a.1563 to 1745) | P22055 | 100 µg | 1195 | |
PN0281 | Recombinant Protein-Coxsackievirus A21 Protein 2B (a.a.1029 to 1125) | P22055 | 100 µg | 1195 | |
PN0282 | Recombinant Protein-Coxsackievirus B3 Protein VP2 (a.a.70 to 332) | Q66282 | 100 µg | 1195 | |
PN0283 | Recombinant Protein-Coxsackievirus B3 Protein VP3 (a.a.333 to 570) | Q66282 | 100 µg | 1195 | |
PN0284 | Recombinant Protein-Coxsackievirus B3 Protein VP1 (a.a.571 to 851) | Q66282 | 100 µg | 1195 | |
PN0285 | Recombinant Protein-Coxsackievirus B3 Picornain 2A (a.a.852 to 1001) | Q66282 | 100 µg | 1195 | |
PN0286 | Recombinant Protein-Coxsackievirus B3 Protein 2C (a.a.1153 to 1429) | Q66282 | 100 µg | 1195 | |
RPN0269 | cDNA-Coxsackievirus A16 Protein VP0 (a.a.2 to 323) | Q9QF31 | 2 µg | 1605 | |
RPN0270 | cDNA-Coxsackievirus A16 Protein VP2 (a.a.70 to 323) | Q9QF31 | 2 µg | 1265 | |
RPN0271 | cDNA-Coxsackievirus A16 Protein VP3 (a.a.324 to 565) | Q9QF31 | 2 µg | 1205 | |
RPN0272 | cDNA-Coxsackievirus A16 Protein VP1 (a.a.591 to 862) | Q9QF31 | 2 µg | 1355 | |
RPN0273 | cDNA-Coxsackievirus A16 Picornain 2A (a.a.863 to 1012) | Q9QF31 | 2 µg | 745 | |
RPN0274 | cDNA-Coxsackievirus A16 Protein 2C (a.a.1112 to 1440) | Q9QF31 | 2 µg | 1640 | |
RPN0275 | cDNA-Coxsackievirus A16 Picornain 3C (a.a.1549 to 1731) | Q9QF31 | 2 µg | 910 | |
RPN0276 | cDNA-Coxsackievirus A21 Protein VP2 (a.a.70 to 341) | P22055 | 2 µg | 1355 | |
RPN0277 | cDNA-Coxsackievirus A21 Protein VP3 (a.a.361 to 581) | P22055 | 2 µg | 1100 | |
RPN0278 | cDNA-Coxsackievirus A21 Protein VP1 (a.a.593 to 879) | P22055 | 2 µg | 1430 | |
RPN0279 | cDNA-Coxsackievirus A21 Picornain 2A (a.a.880 to 1028) | P22055 | 2 µg | 740 | |
RPN0280 | cDNA-Coxsackievirus A21 Picornain 3C (a.a.1563 to 1745) | P22055 | 2 µg | 910 | |
RPN0281 | cDNA-Coxsackievirus A21 Protein 2B (a.a.1029 to 1125) | P22055 | 2 µg | 800 | |
RPN0282 | cDNA-Coxsackievirus B3 Protein VP2 (a.a.70 to 332) | Q66282 | 2 µg | 1310 | |
RPN0283 | cDNA-Coxsackievirus B3 Protein VP3 (a.a.333 to 570) | Q66282 | 2 µg | 1185 | |
RPN0284 | cDNA-Coxsackievirus B3 Protein VP1 (a.a.571 to 851) | Q66282 | 2 µg | 1400 | |
RPN0285 | cDNA-Coxsackievirus B3 Picornain 2A (a.a.852 to 1001) | Q66282 | 2 µg | 745 | |
RPN0286 | cDNA-Coxsackievirus B3 Protein 2C (a.a.1153 to 1429) | Q66282 | 2 µg | 1380 |
Coxsackievirus cDNA and recombinant antigen
Coxsackievirus is a group of RNA viruses that cause a variety of illnesses, including hand, foot and mouth disease, myocarditis, and meningitis. The virus is highly contagious and spreads through contact with contaminated surfaces or through respiratory droplets from an infected person. Symptoms can range from mild to severe and can include fever, sore throat, muscle pain, and blister-like lesions on the hands, feet, and mouth. There is no specific treatment for coxsackievirus infection, but in most cases, the symptoms resolve on their own within 7-10 days. Prevention measures include frequent hand washing and avoiding close contact with infected individuals.
The coxsackievirus genome is the genetic material of the coxsackievirus. It is composed of RNA (ribonucleic acid) and codes to produce viral proteins, enzymes, and other components needed for the replication and spread of the virus. The coxsackievirus genome is linear and consists of a single strand of RNA, which is approximately 7,500-8,000 nucleotides in length. Understanding the coxsackievirus genome is important for developing diagnostic tools, treatments, and vaccines for coxsackievirus infections. Studying the genetic sequence of coxsackieviruses can also provide insights into the evolution and diversity of this group of viruses.
Coxsackievirus antigen refers to a substance or molecule that is specifically recognized by the immune system and triggers an immune response. In the context of coxsackievirus infection, the antigen is typically a viral protein or other component of the virus that is recognized by the immune system. Detection of coxsackievirus antigens can be used as a diagnostic tool to identify the presence of the virus in an individual. Antigen tests for coxsackievirus are generally faster and less expensive than other forms of testing, such as PCR, but may not be as sensitive.
The Coxsackievirus genome encodes several viral proteins, including:
VP0, VP1, VP2, and VP3: These are the four structural proteins that make up the viral capsid. VP0 is cleaved by a viral protease to produce VP2 and VP4 during virus maturation.
Picornain 2A: This is a viral protease that cleaves the viral polyprotein to generate mature viral proteins.
Protein 2C: This is a non-structural protein that is involved in viral RNA replication and the formation of viral replication complexes.
Picornain 3C: This is another viral protease that cleaves the viral polyprotein to generate mature viral proteins.
The structural proteins VP1, VP2, and VP3 are important targets for the host immune response and are involved in the attachment and entry of the virus into host cells. The non-structural proteins, including Picornain 2A, Protein 2C, and Picornain 3C, are involved in viral replication and the modulation of host cell processes to facilitate viral replication and pathogenesis.
Coxsackieviruses are associated with a range of diseases, including hand, foot, and mouth disease, aseptic meningitis, and myocarditis. The various Coxsackievirus serotypes differ in their ability to cause disease and can exhibit different tissue tropisms and clinical manifestations.
The use of recombinant proteins/cDNA in academic research and therapeutic applications has skyrocketed. However, in heterologous expression systems, successful recombinant protein expression is dependent on a variety of factors, including codon preference, RNA secondary structure, and GC content. When compared to pre-optimization, more and more experimental results demonstrated that the expression level was dramatically increased, ranging from two to hundred times depending on the gene. Bioclone has created a proprietary technology platform that has resulted in the creation of over 6,000 artificially synthesized codon-optimized cDNA clones (cloned in E. coli expression Vector), which are ready for production of the recombinant proteins.
Coxsackievirus cDNA and recombinant antigens can be used in a variety of applications, including diagnostic tests, vaccine development, and gene therapy. In diagnostic tests, the cDNA can be used to detect the presence of the virus in a sample. Recombinant antigens can be used to produce antibodies to detect the presence of the virus in a sample.
In vaccine development, cDNA and recombinant antigens can be used to produce vaccines that can prevent infection by the virus. This can be achieved by introducing the cDNA or antigen into a viral vector, which can be used to produce a weakened form of the virus that can be safely administered to an individual.
In gene therapy, the cDNA or antigen can be used to introduce genetic material into a cell that can be used to correct a genetic defect. This can be accomplished by using the cDNA or antigen to introduce a healthy version of the gene into the cell, which can then be used to replace the defective gene.
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