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通过一种新型氧生物传感器系统在非人灵长类动物和人类胰岛中检测到,对高葡萄糖的反应中氧消耗率增加。

Increased oxygen consumption rates in response to high glucose detected by a novel oxygen biosensor system in non-human primate and human islets.

作者信息

Wang Wenjing, Upshaw Lisa, Strong D Michael, Robertson R Paul, Reems Joanna

机构信息

Islet and Cell Processing Laboratory, Puget Sound Blood Center/Northwest Tissue Center, Seattle, Washington 98104, USA.

出版信息

J Endocrinol. 2005 Jun;185(3):445-55. doi: 10.1677/joe.1.06092.

Abstract

In this study, we investigated the use of a novel oxygen biosensor system to detect changes in oxygen consumption rates (OCRs) by islets in response to glucose. Islets from non-human primate and human pancreata were seeded into an oxygen biosensor system microplate and exposed to basal (2.8 or 5.6 mM) or high (16.7 or 33.3 mM) glucose over either a long-term or a short-term culture. Our data clearly demonstrated that non-human primate islets cultured in high glucose conditions exhibited significant increases in OCRs over a 168 h extended culture period (P<0.05), which indicates an accelerated rate of beta-cell metabolism triggered by glucose over time. Significant increases in OCRs (P<0.01) were also attained in both non-human primate and human islets exposed to high glucose conditions in a 120 min short-term incubation period. OCRs exhibited by human islets exposed to different glucose concentrations correlated with insulin secretion (r(2)=0.7681, P<0.01). Moreover, the OCR stimulation index (i.e. OCR at high glucose/OCR at basal glucose) was significantly greater in human islets displaying high viabilities as opposed to islets exhibiting low viabilities (P<0.05). Together these data demonstrate that this novel oxygen biosensor system documents significant increases in islet oxygen consumption upon acute and chronic exposure to high glucose concentrations. Importantly, this methodology rapidly and robustly detects changes in OCRs by islets in response to high glucose stimulation that correlate well with the metabolic activities and functional viability of islets and clearly delineates significant differences in OCR stimulation index between high and low viability human islets, and therefore may prove to be an effective approach for quickly assessing the functional viability of islets prior to transplantation.

摘要

在本研究中,我们调查了一种新型氧生物传感器系统用于检测胰岛对葡萄糖反应时耗氧率(OCR)变化的情况。将来自非人类灵长类动物和人类胰腺的胰岛接种到氧生物传感器系统微孔板中,并在长期或短期培养过程中使其暴露于基础葡萄糖浓度(2.8或5.6 mM)或高葡萄糖浓度(16.7或33.3 mM)环境下。我们的数据清楚地表明,在高葡萄糖条件下培养的非人类灵长类动物胰岛在168小时的延长培养期内OCR显著增加(P<0.05),这表明随着时间推移,葡萄糖引发β细胞代谢速率加快。在120分钟的短期孵育期内,暴露于高葡萄糖条件下的非人类灵长类动物和人类胰岛的OCR也都显著增加(P<0.01)。暴露于不同葡萄糖浓度下的人类胰岛所表现出的OCR与胰岛素分泌相关(r(2)=0.7681,P<0.01)。此外,与低活力胰岛相比,高活力人类胰岛的OCR刺激指数(即高葡萄糖浓度下的OCR/基础葡萄糖浓度下的OCR)显著更高(P<0.05)。这些数据共同表明,这种新型氧生物传感器系统记录了胰岛在急性和慢性暴露于高葡萄糖浓度时氧消耗的显著增加。重要的是,该方法能够快速、稳健地检测胰岛对高葡萄糖刺激的OCR变化,这些变化与胰岛的代谢活动和功能活力密切相关,并且清楚地界定了高活力和低活力人类胰岛在OCR刺激指数上的显著差异,因此可能被证明是一种在移植前快速评估胰岛功能活力的有效方法。

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