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微重力对成骨细胞生长的影响。

Effects of microgravity on osteoblast growth.

作者信息

Hughes-Fulford M, Tjandrawinata R, Fitzgerald J, Gasuad K, Gilbertson V

机构信息

Laboratory of Cell Growth and Differentiation, Veteran's Administration Medical Center, San Francisco, CA, USA.

出版信息

Gravit Space Biol Bull. 1998 May;11(2):51-60.

Abstract

Studies from space flights over the past two decades have demonstrated that basic physiological changes occur in humans during space flight. These changes include cephalic fluid shifts, loss of fluid and electrolytes, loss of muscle mass, space motion sickness, anemia, reduced immune response, and loss of calcium and mineralized bone. The cause of most of these manifestations is not known and until recently, the general approach was to investigate general systemic changes, not basic cellular responses to microgravity. Recently analyzed data from the 1973-1974 Skylabs disclose that there is a rise in the systemic hormone, cortisol, which may play a role in bone loss in flight. In two flights where bone growth was measured (Skylabs 3 and 4), the crew members had a significant loss of calcium accompanied by a rise in 24 hour urinary cortisol during the entire flight period. In ground-based work on osteoblasts, we have demonstrated that equivalent amounts of glucocorticoids can inhibit osteoblast cell growth. In addition, this laboratory has recently studied gene growth and activation of mouse osteoblasts (MC3T3-E1) during spaceflight. Osteoblast cells were grown on glass coverslips, loaded in the Biorack plunger boxes 18 hours before launch and activated 19 hours after launch in the Biorack incubator under microgravity conditions. The osteoblasts were launched in a serum deprived state, activated and collected in microgravity. Samples were collected at 29 hours after sera activation (0-g, n=4; 1-g, n=4). The osteoblasts were examined for changes in gene expression and cell morphology. Approximately one day after growth activation, remarkable differences were observed in gene expression in 0-g and 1-g flight samples. The 0-g activated cells had increased c-fos mRNA when compared to flight 1-g controls. The message of immediate early growth gene, cox-2 was decreased in the microgravity activated cells when compared to ground or 1-g flight controls. Cox-1 was not detected in any of the samples. There were no significant differences in the expression of actin mRNA between the 0-g and 1-g samples. These data indicate that quiescent osteoblasts are slower to enter the cell cycle in microgravity, suggesting that the force of gravity itself may be a significant factor in bone loss in spaceflight. Preliminary data from our STS 76 flight experiment support our hypothesis that a basic biological response occurs at the tissue, cellular, and molecular level in 0-g. Here we examine ground-based and space flown data on osteoblast growth in ground-based experiments mimicking space flight conditions and in microgravity to simulate lack of gravity stress to help us understand the mechanism of bone loss by experiments.

摘要

过去二十年的太空飞行研究表明,人类在太空飞行期间会发生基本的生理变化。这些变化包括头部体液转移、体液和电解质流失、肌肉质量减少、太空晕动病、贫血、免疫反应降低以及钙和矿化骨流失。这些表现大多的原因尚不清楚,直到最近,一般的方法是研究全身系统变化,而不是对微重力的基本细胞反应。最近分析的1973 - 1974年天空实验室的数据显示,全身激素皮质醇有所上升,这可能在飞行中的骨质流失中起作用。在两次测量骨生长的飞行任务(天空实验室3号和4号)中,机组人员在整个飞行期间钙大量流失,同时24小时尿皮质醇上升。在基于地面的成骨细胞研究中,我们已经证明等量的糖皮质激素可以抑制成骨细胞的生长。此外,该实验室最近研究了太空飞行期间小鼠成骨细胞(MC3T3 - E1)的基因生长和激活情况。成骨细胞在玻璃盖玻片上生长,在发射前18小时装入生物架柱塞盒,并在发射后19小时在微重力条件下的生物架培养箱中激活。成骨细胞在血清剥夺状态下发射,在微重力环境中激活并收集。在血清激活后29小时采集样本(0重力,n = 4;1重力,n = 4)。检查成骨细胞的基因表达和细胞形态变化。生长激活大约一天后,在0重力和1重力飞行样本的基因表达中观察到显著差异。与1重力飞行对照组相比,0重力激活的细胞中c - fos mRNA增加。与地面或1重力飞行对照组相比,微重力激活细胞中即时早期生长基因cox - 2的信息减少。在任何样本中均未检测到Cox - 1。0重力和1重力样本之间肌动蛋白mRNA的表达没有显著差异。这些数据表明,静止的成骨细胞在微重力环境中进入细胞周期的速度较慢,这表明重力本身可能是太空飞行中骨质流失的一个重要因素。我们的STS 76飞行实验的初步数据支持我们的假设,即在0重力环境下,组织、细胞和分子水平会发生基本的生物学反应。在这里,我们通过模拟太空飞行条件的地面实验和成骨细胞在微重力环境中的生长情况来研究地面和太空飞行数据,以模拟缺乏重力应激的情况,通过实验帮助我们了解骨质流失的机制。

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