Immune status and expression of HLA-E, HLA-G and HLA-DR molecules on conventional T lymphocytes in patients with multiple myeloma before and after autologous hematopoietic stem cell transplantation

Ivan P. Skachkov; Скачков Иван Павлович; Alina A. Aktanova; Актанова Алина Александровна; Vera V. Denisova; Денисова Вера Васильевна; Ekaterina A. Pashkina; Пашкина Екатерина Александровна

doi:10.46235/1028-7221-17253-ISA

Immune status and expression of HLA-E, HLA-G and HLA-DR molecules on conventional T lymphocytes in patients with multiple myeloma before and after autologous hematopoietic stem cell transplantation

Authors: Skachkov I.P.¹^,2, Aktanova A.A.¹^,2, Denisova V.V.², Pashkina E.A.¹^,2
Affiliations:
1. Research Institute of Fundamental and Clinical Immunology
2. Novosibirsk State Medical University
Issue: Vol 28, No 4 (2025)
Pages: 939-946
Section: SHORT COMMUNICATIONS
URL: https://journals.rcsi.science/1028-7221/article/view/333254
DOI: https://doi.org/10.46235/1028-7221-17253-ISA
ID: 333254

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Abstract

Multiple myeloma (MM) is an incurable disease with common recurrence after treatment, including high-dose chemotherapy (HDC) followed by autologous hematopoietic stem cell transplantation (auto-HSCT). Tumor microenvironment is a factor of achieving long-term remission. Its immunosuppressive effects are mediated due to non-classical HLA class Ib molecules, i.e., HLA-E and HLA-G. These molecules interact with inhibitory receptors (NKG2A/CD94 for HLA-E; ILT2, ILT4, KIR2DL4 for HLA-G) on the surface of NK and T lymphocytes, blocking their cytotoxic activity and facilitating tumor evasion from immune surveillance. In contrast, the classical HLA-DR molecule plays an opposite role, enhancing antitumor immunity through the activation of CD4⁺T helpers. In this study, a comparative analysis of HLA-G/E/DR expression and counts of main immunocompetent cell populations (CD4⁺, CD8⁺, NK, NKT cells, B lymphocytes, monocytes) were performed by flow cytometry method in 10 patients with MM before and after HDC with auto-HSCT, and in 8 healthy volunteers. The results showed that, after therapy, the patients had a significant decrease of total CD3⁺T lymphocyte counts, including CD8⁺ and CD4⁺HLA-G⁺ subpopulations (p < 0.05), thus reflecting a cumulative immunosuppressive effect of melphalan-based conditioning. A decreased number of CD4⁺HLA-G⁺ cells, which have regulatory properties and are capable of suppressing the immune response, may indicate partial destruction of the tumor niche. At the same time, a paradoxically increased proportion of CD8⁺T lymphocytes, along with general lymphopenia, may be associated with clonal expansion of antigen-specific populations with “exhausted” T cell phenotype which requires further study. The results obtained suggest a dualistic role of HLA molecules in pathogenesis of MM: HLA-E/G act as key mediators of immunosuppression, while HLA-DR potentiates antitumor response. The discovered imbalance opens up new prospects for further studies of a role of HLA molecules in the tumor process, which may be applied to personalized therapy, including targeted blockade of NKG2A/LILRB1 receptors or HLA Ib molecules, and development of prognostic models based on a comprehensive analysis of HLA-G/E/DR expression.

Keywords

multiple myeloma, HLA-G, HLA-E, HLA-DR, high-dose chemotherapy, hematopoietic stem cell transplantation autologous, immunosuppression, flow cytometry

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About the authors

Ivan P. Skachkov

Research Institute of Fundamental and Clinical Immunology; Novosibirsk State Medical University

Email: pavania02@gmail.com
ORCID iD: 0009-0000-0530-3818

Student, Junior Researcher, Laboratory of Regulation of the Immune Response

Russian Federation, 14 Yadrintsevskaya St, Novosibirsk, 630099; Novosibirsk

Alina A. Aktanova

Research Institute of Fundamental and Clinical Immunology; Novosibirsk State Medical University

Author for correspondence.
Email: aktanova_al@mail.ru
ORCID iD: 0000-0002-2075-8551

Junior Researcher, Laboratory of Clinical Immunopathology, Assistant Professor, Department of Immunology, Faculty of Medicine

Russian Federation, 14 Yadrintsevskaya St, Novosibirsk, 630099; Novosibirsk

Vera V. Denisova

Novosibirsk State Medical University

Email: verden@bk.ru
ORCID iD: 0000-0003-1951-2260

PhD (Medicine), Head, Hematology Department with the Bone Marrow Transplantation, Clinic of Immunopathology

Russian Federation, Novosibirsk

Ekaterina A. Pashkina

Research Institute of Fundamental and Clinical Immunology; Novosibirsk State Medical University

Email: pashkina.e.a@yandex.ru
ORCID iD: 0000-0002-4912-5512

PhD (Biology), Senior Researcher, Head, Laboratory of Immune Response Regulation, Associate Professor

Russian Federation, 14 Yadrintsevskaya St, Novosibirsk, 630099; Novosibirsk

References

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2. Figure 1. Relative number of CD3+T lymphocytes (A), CD8+T lymphocytes (B), CD4+HLA-G+T lymphocytes (C) 7 days before autologous hematopoietic stem cell transplantation (auto-HSCT) and on day 14 after auto-HSCT. Note. Wilcoxon test, data are presented as median with interquartile range – Me (Q0.25-Q0.75). *, statistically significant differences (p < 0.05).

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3. Figure 2. Relative number of NK cells (A) and NKT cells (B) in patients with multiple myeloma 7 days before auto-HSCT compared to conditionally healthy donors. Note. Mann–Whitney test, data are presented as Me (Q0.25-Q0.75), where P – patients, D – donors. *, statistically significant differences (p < 0.05).

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4. Figure 3. Relative number of CD8+T lymphocytes (A) and B lymphocytes (B) in patients with multiple myeloma 7 days before auto-HSCT in comparison with conditionally healthy donors. Note. Mann–Whitney test, data are presented as Me (Q0.25-Q0.75), where P – patients, D – donors. p = 0.08, significance criterion at the trend level.

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