iPSC-derived cells lack immune tolerance to autologous NK-cells due to imbalance in ligands for activating and inhibitory NK-cell receptors

Margarita E Bogomiakova; Elizaveta K Sekretova; Ksenia S Anufrieva; Polina O Khabarova; Anastasia N Kazakova; Pavel A Bobrovsky; Tatiana V Grigoryeva; Artem V Eremeev; Olga S Lebedeva; Alexandra N Bogomazova; Maria A Lagarkova

doi:10.1186/s13287-023-03308-5

iPSC-derived cells lack immune tolerance to autologous NK-cells due to imbalance in ligands for activating and inhibitory NK-cell receptors

Stem Cell Res Ther. 2023 Apr 11;14(1):77. doi: 10.1186/s13287-023-03308-5.

Authors

Margarita E Bogomiakova^{1

2

3}, Elizaveta K Sekretova^{4

5}, Ksenia S Anufrieva^{4

6}, Polina O Khabarova⁵, Anastasia N Kazakova⁴, Pavel A Bobrovsky^{4

6}, Tatiana V Grigoryeva⁷, Artem V Eremeev^{4

6}, Olga S Lebedeva^{4

6}, Alexandra N Bogomazova^{4

6}, Maria A Lagarkova^{4

5}

Affiliations

¹ Lopukhin Federal Research and Clinical Center of Physical-Chemical Medicine of Federal Medical Biological Agency, 1a Malaya Pirogovskaya, Moscow, Russia, 119435. margbog@rcpcm.org.
² Faculty of Biology, Lomonosov Moscow State University, 1-12 Leninskie Gory, Moscow, Russia, 119991. margbog@rcpcm.org.
³ Center for Precision Genome Editing and Genetic Technologies for Biomedicine, Lopukhin Federal Research and Clinical Center of Physical-Chemical Medicine of Federal Medical Biological Agency, 1a Malaya Pirogovskaya, Moscow, Russia, 119435. margbog@rcpcm.org.
⁴ Lopukhin Federal Research and Clinical Center of Physical-Chemical Medicine of Federal Medical Biological Agency, 1a Malaya Pirogovskaya, Moscow, Russia, 119435.
⁵ Faculty of Biology, Lomonosov Moscow State University, 1-12 Leninskie Gory, Moscow, Russia, 119991.
⁶ Center for Precision Genome Editing and Genetic Technologies for Biomedicine, Lopukhin Federal Research and Clinical Center of Physical-Chemical Medicine of Federal Medical Biological Agency, 1a Malaya Pirogovskaya, Moscow, Russia, 119435.
⁷ Kazan Federal University, 18 Kremlyovskaya Street, Kazan, Russia, 420008.

Abstract

Background: Dozens of transplants generated from pluripotent stem cells are currently in clinical trials. The creation of patient-specific iPSCs makes personalized therapy possible due to their main advantage of immunotolerance. However, some reports have claimed recently that aberrant gene expression followed by proteome alterations and neoantigen formation can result in iPSCs recognition by autologous T-cells. Meanwhile, the possibility of NK-cell activation has not been previously considered. This study focused on the comparison of autologous and allogeneic immune response to iPSC-derived cells and isogeneic parental somatic cells used for reprogramming.

Methods: We established an isogeneic cell model consisting of parental dermal fibroblasts, fibroblast-like iPSC-derivatives (iPS-fibro) and iPS-fibro lacking beta-2-microglobulin (B2M). Using the cells obtained from two patients, we analyzed the activation of autologous and allogeneic T-lymphocytes and NK-cells co-cultured with target cells.

Results: Here we report that cells differentiated from iPSCs can be recognized by NK-cells rather than by autologous T-cells. We observed that iPS-fibro elicited a high level of NK-cell degranulation and cytotoxicity, while isogeneic parental skin fibroblasts used to obtain iPSCs barely triggered an NK-cell response. iPSC-derivatives with B2M knockout did not cause an additional increase in NK-cell activation, although they were devoid of HLA-I, the major inhibitory molecules for NK-cells. Transcriptome analysis revealed a significant imbalance of ligands for activating and inhibitory NK-cell receptors in iPS-fibro. Compared to parental fibroblasts, iPSC-derivatives had a reduced expression of HLA-I simultaneously with an increased gene expression of major activating ligands, such as MICA, NECTIN2, and PVR. The lack of inhibitory signals might be due to insufficient maturity of cells differentiated from iPSCs. In addition, we showed that pretreatment of iPS-fibro with proinflammatory cytokine IFNγ restored the ligand imbalance, thereby reducing the degranulation and cytotoxicity of NK-cells.

Conclusion: In summary, we showed that iPSC-derived cells can be sensitive to the cytotoxic potential of autologous NK-cells regardless of HLA-I status. Thus, the balance of ligands for NK-cell receptors should be considered prior to iPSC-based cell therapies. Trial registration Not applicable.

Keywords: Autologous iPSCs; Beta-2-microglobulin; Differentiation; HLA-I; Immune tolerance; Immunogenicity; NK-cells.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Humans
Immune Tolerance
Induced Pluripotent Stem Cells* / metabolism
Killer Cells, Natural
Ligands
Receptors, Natural Killer Cell / metabolism

Substances

Receptors, Natural Killer Cell
Ligands