Alterations of NK Cell Phenotype in the Disease Course of Multiple Myeloma

Pazina, Tatiana and MacFarlane, Alexander W. and Bernabei, Luca and Dulaimi, Essel and Kotcher, Rebecca and Yam, Clinton and Bezman, Natalie A. and Robbins, Michael D. and Ross, Eric A. and Campbell, Kerry S. and Cohen, Adam D. (2021) Alterations of NK Cell Phenotype in the Disease Course of Multiple Myeloma. Cancers, 13 (2). p. 226. ISSN 2072-6694

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Abstract

Accumulating evidence demonstrates important roles for natural killer (NK) cells in controlling multiple myeloma (MM). A prospective flow cytometry-based analysis of NK cells in the blood and bone marrow (BM) of MM patient subgroups was performed (smoldering (SMM), newly diagnosed (ND), relapsed/refractory, (RR) and post-stem cell transplantation (pSCT)). Assessments included the biomarker expression and function of NK cells, correlations between the expression of receptors on NK cells with their ligands on myeloma cells, and comparisons between MM patient subgroups and healthy controls. The most striking differences from healthy controls were found in RR and pSCT patients, in which NK cells were less mature and expressed reduced levels of the activating receptors DNAM-1, NKG2D, and CD16. These differences were more pronounced in the BM than in blood, including upregulation of the therapeutic targets TIM3, TIGIT, ICOS, and GITR. Their expression suggests NK cells became exhausted upon chronic encounters with the tumor. A high expression of SLAMF7 on blood NK cells correlated with shorter progression-free survival. This correlation was particularly evident in ND patients, including on mature CD56dim NK cells in the BM. Thus, our NK cell analysis identified possible therapeutic targets in MM and a biomarker with prognostic potential for disease progression.

Item Type: Article
Subjects: Academic Digital Library > Medical Science
Depositing User: Unnamed user with email info@academicdigitallibrary.org
Date Deposited: 23 Jan 2023 07:03
Last Modified: 22 Feb 2024 03:58
URI: http://publications.article4sub.com/id/eprint/245

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