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This application note demonstrates how Twist’s precisely synthesized Site-Saturation Variant Libraries (SSVLs) offer a scalable and precise platform to dissect complex mutation interactions and their functional consequences. Using the SARS-CoV-2 spike protein’s receptor binding domain (RBD) as a case study, the Starr Lab at the University of Utah applied SSVLs to rapidly generate and test every possible amino acid substitution across multiple variant backgrounds.
所得结果特定于获得该结果的机构,可能无法反映在其他机构可实现的结果。
仅供研究使用,不适用于诊断程序。
