Abstract

Objective : to evaluate the effect of different biological agents (BAs), including rituximab (RTM) and belimumab (BLM) combination therapy, on B-lymphocyte subpopulations during a follow-up of patients with systemic lupus erythematosus (SLE). Patients and methods . The investigation enrolled 64 patients with a verified diagnosis of SLE with high and moderate disease activities according to the Systemic Lupus Erythromatosus Disease Activity Index (SLEDAI)-2K scores; 47patients of them took RTM, 10 used BLM, and 7 received RTM + BLM combination therapy. Peripheral blood B-lymphocyte subpopulations were measured by multicolor flow cytofluorom-etry, using a panel of monoclonal antibodies to B-lymphocyte surface membrane markers. The results were assessed using the SLEDAI-2K scores and the British Isles Lupus Assessment Group (BILAG) index. Results and discussion . RTM therapy led to a marked decrease in major B-lymphocyte populations, the residual cells being naXve B-cells and different memory B cell populations, the percentage of which depended on the degree of depletion after a RTM cycle. Incomplete B-lymphocyte depletion was associated with the large baseline numbers of plasma cells (PCs) (>0.2%). One year after initiation of therapy, the percentage ratio of B-lymphocyte subpopulations returned almost completely to baseline values, except the whole memory B-cellpopulation. BLM therapy resulted in a decrease in PCs and plasmablasts (PBs) to the point of their complete depletion. There were reductions in total CD19+ B-lym-phocytes and naive B lymphocytes. The use of the combination of BAs permitted the monitoring of the total B-lymphocyte population; its slower recovery was seen in patients with its complete depletion after a rituximab cycle. The therapy promoted maintenance of low concentrations of PCs and PBs, total memory B-cell and naive B-cell populations. Conclusion. In patients with SLE, all the three therapy with BAs demonstrated a good efficiency manifested by a decrease in clinical and laboratory disease activity. The found time course of changes in B-lymphocyte subpopulations can be used for the selection of therapy and for the evaluation of its efficacy.

Highlights

  • Цель исследования – оценка влияния различных генно-инженерных биологических препаратов (ГИБП), включая комбинированное лечение ритуксимабом (РТМ) и белимумабом (БЛМ), на субпопуляции В-лимфоцитов при динамическом наблюдении пациентов с системной красной волчанкой (СКВ)

  • RTM therapy led to a marked decrease in major B-lymphocyte populations, the residual cells being naХve B-cells and different memory B cell populations, the percentage of which depended on the degree of depletion after a RTM cycle

  • Incomplete B-lymphocyte depletion was associated with the large baseline numbers of plasma cells (PCs) (>0.2%)

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Summary

Results and discussion

RTM therapy led to a marked decrease in major B-lymphocyte populations, the residual cells being naХve B-cells and different memory B cell populations, the percentage of which depended on the degree of depletion after a RTM cycle. Неудивительно, что повышение эффективности лечения СКВ связано с внедрением в терапию генно-инженерных биологических препаратов (ГИБП) – ритуксимаба (РТМ) и белимумаба (БЛМ), ориентированных на подавление В-лимфоцитов. Поскольку В-клетки играют огромную роль в развитии СКВ, а современные методы терапии ГИБП ориентированы на их подавление, определение роли отдельных субпопуляций В-лимфоцитов у больных имеет большое значение для определения прогноза заболевания. Данных об исходном составе субпопуляций В-лимфоцитов у пациентов с СКВ и их динамике на фоне лечения ГИБП немного, но накопленный исследователями материал позволяет выделить их как важный инструмент для оценки течения СКВ и исходов терапии. После активации часть наивных В-лимфоцитов дифференцируется в короткоживущие ПК (CD19+, CD38high+, CD20–, CD27high), которые секретируют при СКВ преимущественно антитела к двуспиральной ДНК (дсДНК) [3, 8]

BILAG total
На момент включения и каждые
Отсутствие деплеции
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