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Small interfering RNA (siRNA) is an emerging tool to silence genes that cause disease progression, especially cancer. Compared to existing small molecule and antibody drugs, siRNA drugs have greater potential for development because of their fast target screening, high development success rate, less susceptibility to drug resistance, broader therapeutic area, and long-lasting efficacy. siRNAs are considered a promising drug for the treatment of brain tumors including glioblastoma (GBM).
Alfa Cytology offers brain tumor drug development services targeting siRNAs using multiple development strategies and providing clients with diverse development targets. In addition, we are also trying to chemically modify siRNAs to improve their resistance to nuclease degradation and enhance the stability of siRNAs without affecting their efficacy. We can encapsulate siRNA in nano-delivery bodies such as liposomes, inorganic nanocarriers, or polymeric materials such as dendrimers and polymeric micelles to improve siRNA stability. This can effectively avoid the intravascular degradation of siRNA molecules and reduce the potential immunotoxicity of siRNA molecules, which can greatly improve the pharmacokinetic characteristics of siRNA drugs.
Drug development strategy | Our offer of drug development targets |
Targeted silencing of the RTP801 gene resulted in the downregulation of hypoxia-inducible factor-1 (HIF-1) to control cell proliferation and angiogenesis. |
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Development of functionalized intracellular environment-responsive siRNA nanocapsules as a safe and effective RNAi agent to facilitate siRNA-based treatment of brain tumors (especially GBM). |
If you are interested in our services or if you have a unique target for siRNAs development, please feel free to contact us, and the Alfa Cytology team will respond to your questions or assess the feasibility of your proposed target development. We look forward to collaborating with you in this area.