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首页> 外文期刊>Hematological oncology >Different effects of cyclic AMP and butyrate on eosinophilic differentiation, apoptosis and bcl-2 expression of a human eosinophilic leukemia cell line, EoL-1.
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Different effects of cyclic AMP and butyrate on eosinophilic differentiation, apoptosis and bcl-2 expression of a human eosinophilic leukemia cell line, EoL-1.

机译:环状AMP和丁酸对人嗜酸性粒细胞EoL-1的嗜酸性分化,凋亡和bcl-2表达的不同影响。

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摘要

A human eosinophilic leukemia cell line, EoL-1, stopped proliferating at the G1 phase, differentiated into eosinophilic granule-containing cells, and died by apoptosis when stimulated with dibutyryl cyclic AMP (dbcAMP). To clarify the effects of dbcAMP, the effects of butyrate and cAMP-increasing reagents, prostaglandin E2 (PGE2) and forskolin, on EoL-1 cellular differentiation and apoptosis were examined and compared. PGE2 and forskolin but not butyrate induced differentiation to eosinophilic granule-containing cells, suggesting that cAMP played a primary role in eosinophilic differentiation of EoL-1 cells. PGE2, forskolin and butyrate, when used alone, did not induce apoptosis of EoL-1 cells significantly at the concentrations used, but sequential stimulation of EoL-1 cells with the cAMP-increasing reagents and butyrate showed that butyrate induced further maturation and apoptosis of cAMP-induced eosinophilic granule-containing cells. These results showed that cAMP and butyrate have different effectson eosinophilic differentiation and apoptosis of EoL-1 cells. The cAMP-increasing reagents and butyrate also showed different effects on expression of members of the bcl-2 family; PGE2 decreased bcl-2 and bax levels, whereas butyrate increased the bcl-2 level. PGE2 or PGE2+butyrate, but not butyrate alone, induced bcl-XS expression. EoL-1 cells constitutively expressed Fas and anti-Fas antibody induced EoL-1 cell death, but the Fas/Fas ligand system was not involved in dbcAMP-induced EoL-1 cell apoptosis. The EoL-1 cell line is thus a useful model in which to examine differentiation and apoptosis of eosinophilic leukemia cells.
机译:人类嗜酸性白血病细胞系EoL-1在G1期停止增殖,分化为含嗜酸性颗粒的细胞,并在用二丁酰环AMP(dbcAMP)刺激时因凋亡而死亡。为了阐明dbcAMP的作用,检查并比较了丁酸和cAMP增加剂,前列腺素E2(PGE2)和毛喉素对EoL-1细胞分化和凋亡的作用。 PGE 2和福司可林但不丁酸酯诱导分化为含嗜酸性颗粒的细胞,这表明cAMP在EoL-1细胞的嗜酸性分化中起主要作用。当单独使用PGE2,福司可林和丁酸酯时,在所使用的浓度下不会显着诱导EoL-1细胞的凋亡,但是用增加cAMP的试剂和丁酸酯对EoL-1细胞的顺序刺激表明丁酸酯可诱导EoL-1细胞进一步成熟和凋亡。 cAMP诱导的嗜酸性粒细胞。这些结果表明,cAMP和丁酸盐对EoL-1细胞的嗜酸性细胞分化和凋亡具有不同的作用。增加cAMP的试剂和丁酸对bcl-2家族成员的表达也有不同的影响。 PGE2降低bcl-2和bax水平,而丁酸升高bcl-2水平。 PGE2或PGE2 +丁酸酯(而不是单独的丁酸酯)诱导bcl-XS表达。 EoL-1细胞组成性表达Fas和抗Fas抗体诱导EoL-1细胞死亡,但Fas / Fas配体系统不参与dbcAMP诱导的EoL-1细胞凋亡。因此,EoL-1细胞系是检查嗜酸性粒细胞的分化和凋亡的有用模型。

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