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首页> 外文期刊>Drug Design, Development and Therapy >Linagliptin: from bench to bedside
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Linagliptin: from bench to bedside

机译:利格列汀:从长凳到床头

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Purpose: The nature of biomedical research affords a broad range of investigational topics at the preclinical stage, not all of which may be explored in subsequent clinical studies. To provide a comprehensive perspective on the physiologic effects of the dipeptidyl peptidase-4 inhibitor linagliptin, this review will discuss the results of both preclinical and clinical research, summarizing data describing outcomes associated with its use.Summary: Clinical studies demonstrate an overall favorable safety profile, low risk for hypoglycemia, weight neutrality, primarily nonrenal clearance, and efficacy for glycosylated hemoglobin reduction, typically ranging from 0.6% to 0.8% depending on baseline levels. In addition to these characteristics, preclinical research on linagliptin has yielded several interesting findings such as improved wound healing, reduced hepatic fat content, decreased infarct size following myocardial infarction or intracranial stroke, and improved vascular function with decreased oxidative stress. In accordance with its preclinical profile, linagliptin is unique among available dipeptidyl peptidase-4 compounds because it does not require dose adjustment when used in patients with renal dysfunction. Reduction of albuminuria with linagliptin on top of inhibitors of the renin–angiotensin–aldosterone system in both preclinical and post hoc clinical analysis serves as the foundation for ongoing clinical trials.Conclusion: In addition to its efficacy for glycemic control, current literature points to other potential opportunities associated with linagliptin therapy. These results warrant further investigation and underscore the importance of translational study based on findings from preclinical research. Moving forward, we can expect that future research on linagliptin and other incretin-based therapies will continue to expand their applications beyond the maintenance of glycemic control in patients with type 2 diabetes.
机译:目的:生物医学研究的性质在临床前阶段提供了广泛的研究主题,在随后的临床研究中可能不会探讨所有这些主题。为了提供有关二肽基肽酶4抑制剂利格列汀的生理作用的全面观点,本综述将讨论临床前和临床研究的结果,并总结描述其使用相关结果的数据。总结:临床研究表明总体安全性良好,低血糖的风险低,体重中和(主要是非肾脏清除)以及糖基化血红蛋白降低的功效,通常在0.6%至0.8%之间,具体取决于基线水平。除这些特征外,对利格列汀的临床前研究还产生了一些有趣的发现,例如伤口愈合改善,肝脂肪含量降低,心肌梗塞或颅内中风后梗塞面积减小,血管功能改善以及氧化应激降低。根据其临床前概况,利格列汀在可用的二肽基肽酶-4化合物中是独特的,因为在用于肾功能不全的患者时不需要调整剂量。在临床前和事后临床分析中,在肾素-血管紧张素-醛固酮系统抑制剂的基础上,用利那列汀减少蛋白尿是正在进行的临床试验的基础。结论:除了其对血糖控制的功效外,目前的文献还指出了其他与利格列汀治疗相关的潜在机会。这些结果值得进一步研究,并强调根据临床前研究结果进行转化研究的重要性。展望未来,我们可以预期,有关利格列汀和其他基于肠降血糖素的疗法的未来研究将继续扩大其应用范围,超越维持2型糖尿病患者的血糖控制。

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