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Effect of pinocembrin on thymocyte proliferation and death

عنوان مقاله: Effect of pinocembrin on thymocyte proliferation and death
شناسه ملی مقاله: JR_HERM-13-1_015
منتشر شده در در سال 1403
مشخصات نویسندگان مقاله:

Gulnoza Toshtemirova
Sarvinoz Rustamova
Nargiza Tsiferova
Galina Maksimcheva
Petr Merzlyak
Ranohon Kurbannazarova
Ravshan Sabirov

خلاصه مقاله:
Introduction: Cell volume regulation is critical for cellular proliferation and death. Pinocembrin effectively suppresses the volume regulation in thymocytes under hypoosmotic stress by blocking the volume-sensitive anion channel. This study aims to evaluate the effects of this flavonoid on thymocyte proliferation and death. Methods: Thymocytes were cultured in RPMI-۱۶۴۰ medium supplemented with ۱۰% fetal bovine serum, and the cell number was determined by cloud-based automated cell counting (Corning). Necrotic and apoptotic cell death were evaluated by propidium iodide- and annexin V-staining, respectively. Results: Pinocembrin at ۱۰–۵۰ μM caused suppression of primary cultured thymocyte proliferation with a half-maximal effect of ۲۸.۴ ± ۰.۲ μM. The cell counts did not fall below the control level at the doses of ۱۰۰–۱۵۰ μM. The fraction of spontaneously necrotic cells was ~۲۶% of the total population and increased to ~۵۱% in the presence of dexamethasone. The fraction of spontaneously apoptotic cells increased by this glucocorticoid from ۳.۶% to ۱۶.۷%. Pinocembrin protected thymocytes from necrosis both in spontaneous and dexamethasone-induced death, reducing the fraction of necrotic cells by ~۴۰–۵۰% at ۱۵۰ μM. Pinocembrin attenuated dexamethasone-induced apoptotic death, reducing the fraction of annexin-positive cells to the control (spontaneous) level. Conclusion: Our results suggest that pinocembrin arrests thymocyte proliferation without essential killing. Under conditions of massive death (e.g., during inflammation, when the level of glucocorticoids increases sharply both physiologically and as a result of pharmacotherapy), pinocembrin protects immuno-competent cells from necrotic and apoptotic death.

صفحه اختصاصی مقاله و دریافت فایل کامل: https://civilica.com/doc/1910479/