Systemic and Intra-Nodal Activation of NK Cells After Rituximab Monotherapy for Follicular Lymphoma

Overview

Journal Front Immunol

Specialty Allergy & Immunology

Date 2019 Oct 2

PMID 31572357

Citations 13

Authors

Monika Enqvist

Benedikt Jacobs

Henna R Junlen

Marie Schaffer

Christopher M Melen

Danielle Friberg

Bjorn Engelbrekt Wahlin

Karl-Johan Malmberg

Affiliations

Soon will be listed here.

Abstract

Monotherapy with the anti-CD20 monoclonal antibody rituximab can induce complete responses (CR) in patients with follicular lymphoma (FL). Resting FcRγIII (CD16) natural killer (NK) cells respond strongly to rituximab-coated target cells . Yet, the contribution of NK cells in the therapeutic effect remains unknown. Here, we followed the NK cell repertoire dynamics in the lymph node and systemically during rituximab monotherapy in patients with FL. At baseline, NK cells in the tumor lymph node had a naïve phenotype albeit they were more differentiated than NK cells derived from control tonsils as determined by the frequency of CD56 NK cells and the expression of killer cell immunoglobulin-like receptors (KIR), CD57 and CD16. Rituximab therapy induced a rapid drop in NK cell numbers coinciding with a relative increase in the frequency of Ki67 NK cells both in the lymph node and peripheral blood. The Ki67 NK cells had slightly increased expression of CD16, CD57 and higher levels of granzyme A and perforin. The activation of NK cells was paralleled by a temporary loss of functionality, primarily manifested as decreased IFNγ production in response to rituximab-coated targets. However, patients with pre-existing NKG2C adaptive NK cell subsets showed less Ki67 upregulation and were refractory to the loss of functionality. These data reveal variable imprints of rituximab monotherapy on the NK cell repertoire, which may depend on pre-existing repertoire diversity.

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