Pye Katherine R, Lantier Louise, Ayala Julio E, Beall Craig, Ellacott Kate L J
bioRxiv. 2024 Sep 19:2024.09.13.612859. doi: 10.1101/2024.09.13.612859.
A glucose tolerance test (GTT) is routinely used to assess glucose homeostasis in clinical settings and in preclinical research studies using rodent models. The procedure assesses the ability of the body to clear glucose from the blood in a defined time after a bolus dose. In the human clinical setting, glucose is ingested via voluntary consumption of a glucose-sweetened drink. Typically, in the rodent GTT oral gavage (gavage-oGTT) or (more commonly) intraperitoneal injection (IPGTT) are used to administer the glucose bolus. Although used less frequently, likely due to investigator technical and experience barriers, the former is the more physiologically relevant as it integrates the gastrointestinal tract (GI), including release of key incretin hormones. However, orally gavaging glucose in the GTT is also not without its limitations: gavaging glucose straight into the stomach bypasses potentially critical early glucose-sensing via the mouth (cephalic phase) and associated physiological responses. Furthermore, gavaging is stressful on mice, and this by itself can increase blood glucose levels. We have developed and validated a refined protocol for mouse oral GTT which uses a voluntary oral glucose dosing method, micropipette-guided drug administration (MDA), without the need for water deprivation. This approach is simple and non-invasive. It is less stressful for the mice, as evidenced by lower circulating corticosterone levels 10 minutes after glucose-dosing compared to oral gavage. This is significant for animal and investigator welfare, and importantly minimising the confounding effect of stress on mouse glucose homeostasis. Using a randomised cross-over design, we have validated the MDA approach in the oGTT against oral gavage in male and female C57BL/6J and C57BL/6N mice. We show the ability of this method to detect changes in glucose tolerance in diet-induced obese animals. Compared to oral gavage there was lower inter-animal variation in the MDA-oGTT. In addition to being more representative of the human procedure, the MDA-oGTT is easy and has lower barriers to adoption than the gavage oGTT as it is non-invasive and requires no specialist equipment or operator training. The MDA-oGTT a more clinically representative, accessible, and refined replacement for the gavage-oGTT for mouse metabolic phenotyping, which is simple yet overcomes significant deficiencies in the current standard experimental approaches.
葡萄糖耐量试验(GTT)通常用于临床环境以及使用啮齿动物模型的临床前研究中评估葡萄糖稳态。该程序评估在给予大剂量葡萄糖后,机体在规定时间内从血液中清除葡萄糖的能力。在人类临床环境中,通过自愿饮用含葡萄糖的饮料来摄入葡萄糖。通常,在啮齿动物的GTT中,口服灌胃(灌胃-oGTT)或(更常见的)腹腔注射(IPGTT)用于给予葡萄糖大剂量。尽管使用频率较低,可能是由于研究人员的技术和经验障碍,但前者在生理上更相关,因为它整合了胃肠道(GI),包括关键肠促胰岛素激素的释放。然而,在GTT中口服灌胃葡萄糖也并非没有局限性:直接将葡萄糖灌胃到胃中绕过了通过口腔(头期)进行的潜在关键早期葡萄糖感知以及相关的生理反应。此外,灌胃对小鼠有压力,而这本身就会增加血糖水平。我们已经开发并验证了一种用于小鼠口服GTT的改进方案,该方案使用自愿口服葡萄糖给药方法,即微量移液器引导药物给药(MDA),无需禁水。这种方法简单且无创。对小鼠的压力较小,与口服灌胃相比,在葡萄糖给药后10分钟循环皮质酮水平较低就证明了这一点。这对动物和研究人员的福利很重要,并且重要的是将压力对小鼠葡萄糖稳态的混杂影响降至最低。使用随机交叉设计,我们已经在雄性和雌性C57BL/6J和C57BL/6N小鼠中针对口服灌胃验证了MDA方法在oGTT中的效果。我们展示了这种方法检测饮食诱导肥胖动物葡萄糖耐量变化的能力。与口服灌胃相比,MDA-oGTT中动物间的变异性更低。除了更能代表人类程序外,MDA-oGTT简单,并且与灌胃oGTT相比采用障碍更低,因为它无创且不需要专业设备或操作人员培训。MDA-oGTT是一种更具临床代表性、更易操作且经过改进的方法,可替代灌胃-oGTT用于小鼠代谢表型分析,它简单却克服了当前标准实验方法中的重大缺陷。
