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首页> 外文期刊>Experimental Biology and Medicine: Journal of the Society for Experimental Biology and Medicine >Dietary lactoferrin does not prevent dextran sulfate sodium induced murine intestinal lymphocyte death.
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Dietary lactoferrin does not prevent dextran sulfate sodium induced murine intestinal lymphocyte death.

机译:饮食中的乳铁蛋白不能阻止硫酸葡聚糖钠诱导的鼠肠淋巴细胞死亡。

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摘要

Dextran sulfate sodium (DSS) induced intestinal inflammation is characterized by pronounced mucosal and epithelial cell damage. Bovine lactoferrin (bLf), a common dietary protein, influences inflammatory cytokines and intestinal lymphocyte (IL) apoptosis. The objectives of this study were to determine if 1) DSS induces IL necrotic or apoptotic death, 2) dietary bLf affects DSS induced IL death and 3) bLf alters cytokine profiles during DSS induced inflammation. Female C57BL/6 mice were randomized to 2% or 0% bLf diets for 12 d and within diets to 5% or 0% DSS in the drinking water for 4 d after which intestinal histology, IL number, IL apoptosisecrosis, IL phenotypes, protein levels of pro-inflammatory cytokine (TNF-alpha) and transcription factor (NFkappaB), apoptotic (caspase 3, Bax) proteins, anti-inflammatory cytokine (IL-10) and anti-apoptotic (Bcl-2) protein in IL were evaluated. DSS treatment resulted in shortened intestinal length, decreased body weight and widespread mucosal damage as well as increased IL death as determined by a decreased percentage of viable (PI-/ANN-, P<0.005) and increased percentage of necrotic/late apoptotic (PI+/ ANN+, P<0.05) and necrotic (PI+/ANN-, P<0.05) IL. DSS exposure increased caspase 3 (P<0.05) and decreased Bcl-2 (P<0.01) protein levels in mouse IL. Dietary bLf did not influence these cell death outcome measures. However, bLf reduced protein levels of the pro-inflammatory transcription factor, NFkappaB, in IL (P<0.05) and was associated with a 34%, albeit non-significant, reduction in TNF-alpha relative to non-bLf fed mice. DSS treatment increased apoptosis and necrosis of mouse IL and elevated pro-apoptotic and reduced anti-apoptotic protein levels in these cells. Dietary bLf did not influence necrosis or apoptosis of IL but may provide limited protection in the intestine by affecting the pro-inflammatory transcription factor NFkappaB, and potentially, cytokine expression.
机译:硫酸葡聚糖钠(DSS)诱导的肠道炎症的特征是明显的粘膜和上皮细胞损伤。牛乳铁蛋白(bLf)是一种常见的饮食蛋白,会影响炎症细胞因子和肠淋巴细胞(IL)的细胞凋亡。这项研究的目的是确定1)DSS是否诱导IL坏死或凋亡死亡; 2)饮食中bLf影响DSS诱导的IL死亡; 3)bLf在DSS诱导的炎症过程中改变细胞因子谱。将雌性C57BL / 6小鼠随机分配到2%或0%bLf饮食中12 d,并且在饮食中随机给5%或0%DSS饮用水中的4 d,之后肠道组织学,IL数目,IL凋亡/坏死,IL表型,IL中的促炎细胞因子(TNF-alpha)和转录因子(NFkappaB),凋亡(胱天蛋白酶3,Bax)蛋白,抗炎细胞因子(IL-10)和抗凋亡(Bcl-2)蛋白水平被评估。 DSS治疗导致肠道长度缩短,体重减轻和广泛的粘膜损伤,以及IL死亡增加,这取决于存活率降低(PI- / ANN-,P <0.005)和坏死/晚期凋亡百分比(PI + / ANN +,P <0.05)和坏死(PI + / ANN-,P <0.05)IL。 DSS暴露可增加小鼠IL中胱天蛋白酶3(P <0.05)并降低Bcl-2(P <0.01)蛋白水平。膳食bLf不会影响这些细胞死亡结果指标。然而,bLf降低了IL中促炎性转录因子NFkappaB的蛋白水平(P <0.05),并且与非bLf喂养的小鼠相比,TNF-α降低了34%,尽管无显着性。 DSS处理增加了小鼠IL的凋亡和坏死,并增加了这些细胞的促凋亡和降低了抗凋亡蛋白水平。饮食中的bLf不会影响IL的坏死或凋亡,但可能通过影响促炎转录因子NFkappaB以及潜在地影响细胞因子的表达而在肠道中提供有限的保护。

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