临床前模型中顺铂诱导 AKI 的时程分析:对不同来源 MSC 检测的影响。
Time-course analysis of cisplatin induced AKI in preclinical models: implications for testing different sources of MSCs.
机构信息
Interventional Radiology Innovation at Stanford (IRIS), Department of Radiology, School of Medicine, Stanford University, 3155 Porter Drive, Palo Alto, CA, 94304, USA.
Department of Pathology, Stanford University, Palo Alto, CA, USA.
出版信息
J Transl Med. 2024 Aug 27;22(1):789. doi: 10.1186/s12967-024-05439-6.
BACKGROUND
Kidneys are at risk from drug-induced toxicity, with a significant proportion of acute kidney injury (AKI) linked to medications, particularly cisplatin. Existing cytoprotective drugs for cisplatin-AKI carry side effects, prompting a search for better biological therapies. Mesenchymal Stem Cells (MSCs) are under consideration given their regenerative properties, yet their clinical application has not achieved their full potential, mainly due to variability in the source of MSC tested. In addition, translating treatments from rodent models to humans remains challenging due to a lack of standardized dosing and understanding potential differential responses to cisplatin between animal strains.
METHOD
In the current study, we performed a time-course analysis of the effect of cisplatin across different mouse strains and evaluated gender related differences to create a robust preclinical model that could then be used to explore the therapeutic efficacy of different sources of MSCs for their ability to reverse AKI.
RESULT
Our data indicated that different mouse strains produce differential responses to the same cisplatin dosing regimen. Despite this, we did not observe any gender-related bias towards cisplatin nephrotoxicity. Furthermore, our time-course analysis identified that cisplatin-induced inflammation was driven by a strong CXCL1 response, which was used as a putative biomarker to evaluate the comparative therapeutic efficacy of different MSC sources in reversing AKI. Our data indicates that UC-MSCs have a stronger anti-inflammatory effect compared to BM-MSCs and AD-MSCs, which helped to ameliorate cisplatin-AKI.
CONCLUSION
Overall, our data underscores the importance of using an optimized preclinical model of cisplatin-AKI to test different therapies. We identified CXCL1 as a potential biomarker of cisplatin-AKI and identified the superior efficacy of UC-MSCs in mitigating cisplatin-AKI.
背景
肾脏容易受到药物诱导的毒性影响,其中相当一部分急性肾损伤(AKI)与药物有关,尤其是顺铂。现有的顺铂-AKI 细胞保护药物存在副作用,因此需要寻找更好的生物治疗方法。鉴于间充质干细胞(MSCs)具有再生特性,因此正在考虑使用它们,但由于测试的 MSC 来源存在变异性,其临床应用尚未发挥出全部潜力。此外,由于缺乏标准化的剂量方案以及对不同动物品系中顺铂的潜在差异反应的了解,将治疗方法从啮齿动物模型转化到人类仍然具有挑战性。
方法
在目前的研究中,我们对不同小鼠品系中顺铂的作用进行了时间过程分析,并评估了性别相关差异,以创建一个稳健的临床前模型,然后可以使用该模型来探索不同来源的 MSC 治疗 AKI 的疗效,以评估其逆转 AKI 的能力。
结果
我们的数据表明,不同的小鼠品系对相同的顺铂给药方案产生不同的反应。尽管如此,我们没有观察到顺铂肾毒性与性别相关的任何偏见。此外,我们的时间过程分析表明,顺铂诱导的炎症是由强烈的 CXCL1 反应驱动的,该反应可用作评估不同 MSC 来源逆转 AKI 的相对治疗效果的推定生物标志物。我们的数据表明,UC-MSCs 比 BM-MSCs 和 AD-MSCs 具有更强的抗炎作用,有助于改善顺铂-AKI。
结论
总的来说,我们的数据强调了使用优化的顺铂-AKI 临床前模型来测试不同治疗方法的重要性。我们确定了 CXCL1 作为顺铂-AKI 的潜在生物标志物,并确定了 UC-MSCs 在减轻顺铂-AKI 方面的优越疗效。
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