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| Size | 100ug, 1MG |
|---|---|
| Isotype | Human IgG1 |
| Brand | ProteoGenix |
| Product type | Primary Antibodies |
| Clonality | Monoclonal Antibody |
| Expression system | Mammalian cells |
| Applications | Elisa, WB |
| Product name | RSV-neutralizing Human Antibody Biosimilar - Anti-Respipatory syncytial virus mAb - Research Grade |
|---|---|
| Species | Humanized |
| Purity | >85% |
| Buffer | PBS buffer pH7.5 |
| Delivery condition | Blue ice (+4°C) |
| Delivery Time | 3-5 days if in stock; 3-5 weeks if production needed |
| Storage condition | store at -80°C |
| Brand | ProteoGenix |
| Aliases /Synonyms | RSV-neutralizing Human Antibody ,0,Respipatory syncytial virus,anti-Respipatory syncytial virus |
| Reference | PX-TA1628 |
| Note | For research use only. Not suitable for clinical or therapeutic use. |
| Isotype | Human IgG1 |
| Clonality | Monoclonal Antibody |
Respiratory syncytial virus (RSV) is a common respiratory pathogen that causes severe illness in infants, older adults, and immunocompromised individuals. Despite decades of research, there is still no licensed vaccine or effective treatment for RSV infection. However, recent advances in biotechnology have led to the development of RSV-neutralizing human antibody biosimilars, such as the Anti-RSV mAb, which holds great promise as a therapeutic option for RSV infection. In this article, we will provide a scientific description of the structure, activity, and potential applications of this biosimilar.
The Anti-RSV mAb is a monoclonal antibody (mAb) that specifically targets the fusion (F) protein of RSV. This protein is essential for the virus to enter and infect host cells. The Anti-RSV mAb is a biosimilar, meaning it is highly similar to an already approved reference product, in this case, the FDA-approved palivizumab. It is produced using recombinant DNA technology, where the gene encoding the antibody is inserted into a host cell, such as Chinese hamster ovary (CHO) cells, to produce large quantities of the antibody.
The Anti-RSV mAb is a humanized antibody, meaning it is derived from human antibodies but has been modified to reduce the risk of immune reactions in patients. It is composed of two identical heavy chains and two identical light chains, connected by disulfide bonds. The heavy chains consist of four constant domains (CH1, CH2, CH3, and CH4) and one variable domain (VH), while the light chains contain one constant domain (CL) and one variable domain (VL). The variable domains are responsible for binding to the F protein of RSV, while the constant domains provide stability and effector functions.
The primary function of the Anti-RSV mAb is to neutralize RSV by binding to the F protein and preventing it from fusing with host cells. This prevents the virus from entering and replicating in the cells, thus halting the infection. The Anti-RSV mAb has been shown to be highly effective in neutralizing a broad range of RSV strains, including both subtypes A and B.
In addition to neutralization, the Anti-RSV mAb also has effector functions, such as antibody-dependent cell-mediated cytotoxicity (ADCC) and complement-dependent cytotoxicity (CDC). These functions involve the recruitment and activation of immune cells, such as natural killer (NK) cells and macrophages, to kill RSV-infected cells. This enhances the overall antiviral activity of the antibody.
The Anti-RSV mAb is currently being evaluated as a potential therapeutic option for RSV infection. It is being studied in both prophylactic and therapeutic settings, with promising results. In a phase III clinical trial, the Anti-RSV mAb showed a 55% reduction in hospitalization due to RSV infection in high-risk infants compared to placebo. It has also been shown to be safe and well-tolerated in clinical trials.
In addition to its potential as a treatment for RSV infection, the Anti-RSV mAb also has the potential to be used as a prophylactic agent. It can be administered to high-risk individuals, such as premature infants and older adults, to prevent RSV infection. This could significantly reduce the burden of RSV-related hospitalizations and deaths, especially in vulnerable populations.
In summary, the Anti-RSV mAb is a promising biosimilar that specifically targets the F protein of RSV. Its structure, activity, and potential applications make it a valuable therapeutic option for RSV infection. Further research and clinical trials are needed to fully evaluate its efficacy and safety, but the Anti-RSV mAb holds great potential in the fight against RSV.
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