B cells engineered to express pathogen-specific antibodies protect against infection.
Howell F MoffettCarson K HarmsKristin S FitzpatrickMarti R TooleyJim BoonyaratanakornkitJustin James TaylorPublished in: Science immunology (2020)
Effective vaccines inducing lifelong protection against many important infections such as respiratory syncytial virus (RSV), HIV, influenza virus, and Epstein-Barr virus (EBV) are not yet available despite decades of research. As an alternative to a protective vaccine, we developed a genetic engineering strategy in which CRISPR-Cas9 was used to replace endogenously encoded antibodies with antibodies targeting RSV, HIV, influenza virus, or EBV in primary human B cells. The engineered antibodies were expressed efficiently in primary B cells under the control of endogenous regulatory elements, which maintained normal antibody expression and secretion. Using engineered mouse B cells, we demonstrated that a single transfer of B cells engineered to express an antibody against RSV resulted in potent and durable protection against RSV infection in RAG1-deficient mice. This approach offers the opportunity to achieve sterilizing immunity against pathogens for which traditional vaccination has failed to induce or maintain protective antibody responses.
Keyphrases
- respiratory syncytial virus
- epstein barr virus
- diffuse large b cell lymphoma
- antiretroviral therapy
- crispr cas
- hiv positive
- human immunodeficiency virus
- hiv infected
- hiv testing
- hepatitis c virus
- respiratory tract
- endothelial cells
- hiv aids
- poor prognosis
- genome editing
- gene expression
- dna methylation
- genome wide
- drug delivery
- copy number
- gram negative
- anti inflammatory
- multidrug resistant
- binding protein
- induced pluripotent stem cells