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首页> 外文期刊>BMC Musculoskeletal Disorders >Aging enhances serum cytokine response but not task-induced grip strength declines in a rat model of work-related musculoskeletal disorders
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Aging enhances serum cytokine response but not task-induced grip strength declines in a rat model of work-related musculoskeletal disorders

机译:在与工作有关的肌肉骨骼疾病的大鼠模型中,衰老可增强血清细胞因子反应,但不会导致任务诱发的握力下降

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Background We previously reported early tissue injury, increased serum and tissue inflammatory cytokines and decreased grip in young rats performing a moderate demand repetitive task. The tissue cytokine response was transient, the serum response and decreased grip were still evident by 8 weeks. Thus, here, we examined their levels at 12 weeks in young rats. Since aging is known to enhance serum cytokine levels, we also examined aged rats. Methods Aged and young rats, 14 mo and 2.5 mo of age at onset, respectfully, were trained 15 min/day for 4 weeks, and then performed a high repetition, low force (HRLF) reaching and grasping task for 2 hours/day, for 12 weeks. Serum was assayed for 6 cytokines: IL-1alpha, IL-6, IFN-gamma, TNF-alpha, MIP2, IL-10. Grip strength was assayed, since we have previously shown an inverse correlation between grip strength and serum inflammatory cytokines. Results were compared to na?ve (grip), and normal, food-restricted and trained-only controls. Results Serum cytokines were higher overall in aged than young rats, with increases in IL-1alpha, IFN-gamma and IL-6 in aged Trained and 12-week HRLF rats, compared to young Trained and HRLF rats (p < 0.05 and p < 0.001, respectively, each). IL-6 was also increased in aged 12-week HRLF versus aged normal controls (p < 0.05). Serum IFN-gamma and MIP2 levels were also increased in young 6-week HRLF rats, but no cytokines were above baseline levels in young 12-week HRLF rats. Grip strength declined in both young and aged 12-week HRLF rats, compared to na?ve and normal controls (p < 0.05 each), but these declines correlated only with IL-6 levels in aged rats (r = -0.39). Conclusion Aging enhanced a serum cytokine response in general, a response that was even greater with repetitive task performance. Grip strength was adversely affected by task performance in both age groups, but was apparently influenced by factors other than serum cytokine levels in young rats.
机译:背景我们以前曾报道过,在执行中度需求重复任务的幼鼠中,早期组织损伤,血清和组织炎性细胞因子增加以及抓地力降低。组织细胞因子反应是短暂的,到8周时血清反应和抓地力下降仍很明显。因此,在这里,我们检查了幼鼠在第12周时的水平。由于已知衰老会增强血清细胞因子水平,因此我们还检查了衰老大鼠。方法分别训练成年和成年年龄分别为14 mo和2.5 mo的成年和年轻大鼠,每天15分钟,训练4周,然后每天进行2小时/天的高重复,低力量(HRLF)达到和抓握任务,持续12周。测定血清中的6种细胞因子:IL-1α,IL-6,IFN-γ,TNF-α,MIP2,IL-10。由于我们先前已经显示出握力与血清炎性细胞因子之间呈负相关,因此测定了握力。将结果与单纯(抓地力)和正常,食物受限且仅受过训练的对照进行比较。结果老年训练和12周HRLF大鼠的血清细胞因子总体上比幼鼠高,IL-1alpha,IFN-γ和IL-6的增加,与青年训练和HRLF大鼠相比(p <0.05和p <分别为0.001)。与正常对照组相比,在12周龄HRLF中IL-6也升高(p <0.05)。 6周龄年轻HRLF大鼠的血清IFN-γ和MIP2水平也升高,但12周龄年轻LFLF大鼠的细胞因子均未高于基线水平。与幼稚和正常对照组相比,年轻和老年的12周HRLF大鼠的握力都下降了(每只P <0.05),但是这些下降仅与老年大鼠的IL-6水平相关(r = -0.39)。结论衰老一般会增强血清细胞因子的反应,这种反应在重复性任务表现中甚至更高。握力强度在两个年龄组中均受任务绩效的不利影响,但显然受幼鼠血清细胞因子水平以外的因素影响。

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