Affiliation:
1. Department of Clinical Medicine Aarhus University Aarhus Denmark
2. Department of Molecular Biology and Genetics Aarhus University Aarhus Denmark
3. Department of Infectious Diseases Aarhus University Hospital Aarhus Denmark
4. Department of Biomedicine Aarhus University Aarhus Denmark
Abstract
AbstractThe complement system which is part of the innate immune response against invading pathogens represents a powerful mechanism for killing of infected cells. Utilizing direct complement recruitment for complement‐mediated elimination of HIV‐1‐infected cells is underexplored. We developed a novel therapeutic modality to direct complement activity to the surface of HIV‐1‐infected cells. This bispecific complement engager (BiCE) is comprised of a nanobody recruiting the complement‐initiating protein C1q, and single‐chain variable fragments of broadly neutralizing antibodies (bNAbs) targeting the HIV‐1 envelope (Env) protein. Here, we show that two anti‐HIV BiCEs targeting the V3 loop and the CD4 binding site, respectively, increase C3 deposition and mediate complement‐dependent cytotoxicity (CDC) of HIV‐1 Env‐expressing Raji cells. Furthermore, anti‐HIV BiCEs trigger complement activation on primary CD4 T cells infected with laboratory‐adapted HIV‐1 strain and facilitates elimination of HIV‐1‐infected cells over time. In summary, we present a novel approach to direct complement deposition to the surface of HIV‐1‐infected cells leading to complement‐mediated killing of these cells.
Funder
Danmarks Frie Forskningsfond
Novo Nordisk Fonden
Publisher
Springer Science and Business Media LLC
Cited by
5 articles.
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