Nanobody-based CAR NK cells for possible immunotherapy of MICA+ tumors

Author:

Verhaar Elisha R12ORCID,van Keizerswaard Willemijn J C1ORCID,Knoflook Anouk1ORCID,Balligand Thomas1ORCID,Ploegh Hidde L12ORCID

Affiliation:

1. Program in Cellular and Molecular Medicine, Boston Children's Hospital, Harvard Medical School , Boston, MA 02115 , USA

2. Department of Cell and Chemical Biology, Leiden University Medical Centre , 2333 ZA Leiden , The Netherlands

Abstract

Abstract The glycoproteins MICA and MICB are upregulated on the surface of cells undergoing stress, for instance due to (viral) infection or malignant transformation. MICA/B are the ligands for the activating receptor NKG2D, found on cytotoxic immune cells like NK cells, CD8+ T cells, and γδ T cells. Upon engagement of NKG2D, these cells are activated to eradicate the MICA/B-positive targets, assisted by the secretion of cytokines. Nanobodies, or VHHs, are derived from the variable regions of camelid heavy-chain only immunoglobulins. Nanobodies are characterized by their small size, ease of production, stability, and specificity of recognition. We generated nanobodies that recognize membrane-bound MICA with high affinity. Here, we use these nanobodies as building blocks for a chimeric antigen receptor (CAR) to establish VHH-based CAR NK cells. These anti-MICA nanobody-based CAR NK cells recognize and selectively kill MICA-positive tumor cells in vitro and in vivo. We track localization of the VHH-based CAR NK cells to MICA-positive lung metastases by immuno-positron emission tomography imaging.

Funder

NIH

Belgian American Educational Foundation

Wallonie-Bruxelles International

Publisher

Oxford University Press (OUP)

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