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Cat# | Product Name | Swiss Prot# | Size | Price (US$) | Order |
PN0167 | Recombinant Protein-Bunyavirus La Crosse Nucleocapsid protein (a.a.21 to 222) | O39107 | 100 µg | 1195 | |
PN0168 | Recombinant Protein-Bunyavirus La Crosse M polyprotein (a.a.71 to 450) | A5HC97 | 100 µg | 1195 | |
PN0169 | Recombinant Protein-Bunyavirus La Crosse G2 glycoprotein (a.a.14 to 299) | Q83001 | 100 µg | 1195 | |
PN0170 | Recombinant Protein-Bunyavirus La Crosse Polyprotein (a.a.474 to 774) | Q83001 | 100 µg | 1195 | |
PN0171 | Recombinant Protein-Bunyavirus La Crosse Nucleoprotein (a.a.21 to 235) | P04873 | 100 µg | 1195 | |
PN0172 | Recombinant Protein-Bunyavirus La Crosse Non-structural protein NSm (a.a.300 to 473) | P09612 | 100 µg | 1195 | |
PN0173 | Recombinant Protein-Bunyavirus La Crosse Glycoprotein G2 (a.a.22 to 299) | P09612 | 100 µg | 1195 | |
RPN0167 | cDNA-Bunyavirus La Crosse Nucleocapsid protein (a.a.21 to 222) | O39107 | 2 µg | 1005 | |
RPN0168 | cDNA-Bunyavirus La Crosse M polyprotein (a.a.71 to 450) | A5HC97 | 2 µg | 1895 | |
RPN0169 | cDNA-Bunyavirus La Crosse G2 glycoprotein (a.a.14 to 299) | Q83001 | 2 µg | 1425 | |
RPN0170 | cDNA-Bunyavirus La Crosse Polyprotein (a.a.474 to 774) | Q83001 | 2 µg | 1500 | |
RPN0171 | cDNA-Bunyavirus La Crosse Nucleoprotein (a.a.21 to 235) | P04873 | 2 µg | 1070 | |
RPN0172 | cDNA-Bunyavirus La Crosse Non-structural protein NSm (a.a.300 to 473) | P09612 | 2 µg | 865 | |
RPN0173 | cDNA-Bunyavirus La Crosse Glycoprotein G2 (a.a.22 to 299) | P09612 | 2 µg | 1385 |
Bunyavirus La Crosse cDNA and recombinant antigen
Bunyavirus La Crosse (LACV) is a virus that is transmitted to humans through the bite of infected mosquitoes and causes La Crosse encephalitis, a serious and sometimes fatal disease of the central nervous system. La Crosse encephalitis is primarily a pediatric disease and occurs mainly in the midwestern and eastern United States. The virus is maintained in a cycle between mosquitoes and small mammals, particularly chipmunks and squirrels. Control measures for LACV include reducing mosquito populations using insecticides, wearing protective clothing and using mosquito repellents when spending time outdoors, and removing standing water sources that serve as breeding sites for mosquitoes. There is no specific treatment for LACV infection, and supportive care is typically provided for affected individuals.
The Bunyavirus La Crosse (LACV) genome refers to the complete genetic material of the virus. LACV is a negative-sense single-stranded RNA virus, and its genome size is approximately 19 kilobases. The LACV genome encodes for several structural and non-structural proteins that are involved in viral replication and pathogenesis. Analysis of the LACV genome has provided important insights into the molecular biology and evolution of the virus and has facilitated the development of improved diagnostic tools and vaccines for controlling LACV infection.
Bunyavirus La Crosse (LACV) antigen refers to any substance that is recognized and specifically reacted with by the immune system of a human, usually from a vaccine, to produce an immune response. In the context of LACV, the antigen is typically a protein or viral particle that is used in a vaccine to stimulate the production of antibodies that protect against LACV infection. Currently, there is no commercially available vaccine for LACV, and control measures primarily involve reducing exposure to infected mosquitoes with protective clothing and insect repellents and removing standing water sources that serve as breeding sites for mosquitoes.
Bunyavirus La Crosse is a member of the Bunyaviridae family and is the causative agent of La Crosse encephalitis, a disease that affects humans and other mammals. The virus has several important proteins that play critical roles in its replication and pathogenesis.
The nucleocapsid protein is a structural protein that encapsidates the viral RNA genome, forming the viral nucleocapsid.
The M polyprotein, also known as the matrix protein, is involved in the assembly and release of the virus from the host cell.
The G2 glycoprotein, also known as the envelope glycoprotein, is a surface protein that is involved in viral attachment to host cells, as well as fusion of the viral envelope with the host cell membrane during entry.
The polyprotein is a large precursor protein that is cleaved into multiple smaller proteins during viral replication.
The nucleoprotein is another structural protein that binds to the viral RNA genome and is involved in RNA replication and transcription.
The non-structural protein NSm is involved in viral replication and assembly.
The glycoprotein G2, as mentioned earlier, is a surface protein that is involved in viral attachment and entry.
The utilization of recombinant proteins/cDNA in both scholarly research and medical applications has recently surged. However, successful expression of the recombinant protein within heterologous expression systems is contingent upon an array of factors, including the preference of codons, secondary structure of RNA, and GC content. An increase in the level of expression by up to one hundred times, relying on the gene, was indicated through various experimental results when compared to pre-optimization. Through a specialized technological platform developed by Bioclone, over six thousand codon-optimized cDNA clones, which have been artificially synthesized and cloned in an E. coli expression vector, are now readily available for the creation of recombinant proteins.
Bunyavirus La Crosse cDNA and the recombinant antigen have various applications, including diagnostic assays designed to detect La Crosse virus, the development of vaccines, and examination of the genetic framework of the virus.
Diagnostic assays: The cDNA and recombinant antigen can be employed to create diagnostic assays capable of identifying the La Crosse virus’s existence within a sample. Such assays can recognize individuals infected with the virus and keep track of its transmission throughout the population.
Vaccine development: The cDNA and recombinant antigen can aid in the development of a potent vaccine against the La Crosse virus, which can safeguard individuals against infection and limit its spread among the population.
Studying the genetic structure of the virus: The cDNA and recombinant antigen can also be used to study the genetic composition of the virus, allowing researchers to gain insight into its functionality and transmission mechanisms.
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