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Engineered B cells expressing an anti-HIV antibody enable memory retention, isotype switching and clonal expansion.


ABSTRACT: HIV viremia can be controlled by chronic antiretroviral therapy. As a potentially single-shot alternative, B cells engineered by CRISPR/Cas9 to express anti-HIV broadly neutralizing antibodies (bNAbs) are capable of secreting high antibody titers. Here, we show that, upon immunization of mice, adoptively transferred engineered B cells home to germinal centers (GC) where they predominate over the endogenous response and differentiate into memory and plasma cells while undergoing class switch recombination (CSR). Immunization with a high affinity antigen increases accumulation in GCs and CSR rates. Boost immunization increases the rate of engineered B cells in GCs and antibody secretion, indicating memory retention. Finally, antibody sequences of engineered B cells in the spleen show patterns of clonal selection. Therefore, B cells can be engineered into what could be a living and evolving drug.

SUBMITTER: Nahmad AD 

PROVIDER: S-EPMC7673991 | biostudies-literature | 2020 Nov

REPOSITORIES: biostudies-literature

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Engineered B cells expressing an anti-HIV antibody enable memory retention, isotype switching and clonal expansion.

Nahmad Alessio D AD   Raviv Yuval Y   Horovitz-Fried Miriam M   Sofer Ilan I   Akriv Tal T   Nataf Daniel D   Dotan Iris I   Carmi Yaron Y   Burstein David D   Wine Yariv Y   Benhar Itai I   Barzel Adi A  

Nature communications 20201117 1


HIV viremia can be controlled by chronic antiretroviral therapy. As a potentially single-shot alternative, B cells engineered by CRISPR/Cas9 to express anti-HIV broadly neutralizing antibodies (bNAbs) are capable of secreting high antibody titers. Here, we show that, upon immunization of mice, adoptively transferred engineered B cells home to germinal centers (GC) where they predominate over the endogenous response and differentiate into memory and plasma cells while undergoing class switch reco  ...[more]

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