Quantifying Residual DNA in Biotherapeutic Manufacturing

Application Focus Quantifying Residual DNA in a Biotherapeutic Manufacturing Workflow Author Summary Ilaria Scarfone Residual host cell and plasmid DNA can survive purification methods in biotherapeutic development and manufacture, affecting safety and efficacy of the final product. Thermo Fisher Scientific’s fully integrated commercial kits for residual DNA analysis deliver rapid, reliable and highly consistent solutions for quality control (QC) and lot release. The challenge of residual DNA Biotherapeutics are manufactured by modifying living cells in order to create therapeutic products, such as gene therapies and vaccines. During manufacture, low levels of cellular DNA from the host cell, or plasmid DNA derived from the manufacturing reagents, can survive the purification process. This is known as residual DNA, and transference to the patient in biotherapeutic products may lead to an increased risk of oncogenicity and immunogenicity. In light of these safety concerns, regulatory guidance for products produced in cell culture specifies that residual DNA content in the final product must be as low as possible, as quantified by a highly sensitive, reliable testing method. While many laboratories opt to develop in-house protocols for residual DNA analytical methods, this can result in multiple challenges and a considerable investment of time, resources and specialized expertise. Controls and standards must be highly robust, ensuring material stability and linearity of the standards. In addition, all standard operating procedures (SOPs) must be validated under the ICH Q2 (R1) guidance for analytical procedures.