ProMiFa, Protein Microsequencing Facility, San Raffaele Scientific Institute, Milan, Italy.
Complications of Diabetes Unit, Diabetes Research Institute (DRI), San Raffaele Scientific Institute, Milan, Italy.
J Proteomics. 2019 Feb 20;193:205-216. doi: 10.1016/j.jprot.2018.10.010. Epub 2018 Oct 24.
Despite research progresses, the chance to accurately predict the risk for diabetic nephropathy (DN) is still poor. So far, the first evidence of DN is micro-albuminuria, which is detected only 10-20 years after the onset of diabetes. Our goal is to develop new predictive tools of nephropathy starting from urine, which can be easily obtained using noninvasive procedures and it is directly related to kidney. Since it is reasonable to suppose that, in predisposed patients, the mechanisms leading to nephropathy start acting since the diabetes onset, urine from children with recent diagnosis of type 1 diabetes was subjected to proteomic analysis in comparison to age-matched controls. Targeted confirmation was performed on children with a longer history of diabetes using Western Blotting and applying a urinary lipidomic approach. To definitively understand whether the observed alterations could be related to diabetic nephropathy, urine from diabetic adults with or without albuminuria was also examined. For the first time, lipid metabolisms of prostaglandin and ceramide, which are significantly and specifically modified in association with DN, are shown to be already altered in children with a recent diabetes diagnosis. Future studies on larger cohorts are needed to improve the validity and generalizability of these findings. Data are available via ProteomeXchange with identifier PXD011183 Submission details: Project Name: Urinary proteomics by 2DE and LC-MS/MS. Project accession: PXD011183 Project DOI: https://doi.org/10.6019/PXD011183 SIGNIFICANCE: Nephropathy is a very common diabetic complication. Once established, its progression can only be slowed down but full control or remission is achieved in very few cases, thus posing a large burden on worldwide health. The first evidence of diabetic nephropathy (DN) is micro-albuminuria, but only 30% of patients with micro-albuminuria progress to proteinuria, while in some patients it spontaneously reverts to normo-albuminuria. Thus, there is clear need for biomarkers that can accurately predict the risk to develop DN. Herein, by applying proteomic and lipidomic approaches on urine samples, we show that alteration of prostaglandin and ceramide metabolisms specifically occurs in association with DN. Interestingly, we demonstrate that the modification of these metabolic pathways is an early event in diabetic patients, suggesting the identified changed proteins as possible predictive biomarkers of diabetes-induced renal function decline.
尽管研究取得了进展,但准确预测糖尿病肾病 (DN) 风险的机会仍然很差。到目前为止,DN 的第一个证据是微量白蛋白尿,它仅在糖尿病发病后 10-20 年才被检测到。我们的目标是从尿液中开发新的肾病预测工具,这些工具可以通过非侵入性程序轻松获得,并且与肾脏直接相关。由于可以合理地假设,在易患患者中,导致肾病的机制自糖尿病发病时就开始起作用,因此对最近诊断为 1 型糖尿病的儿童的尿液进行了蛋白质组分析,并与年龄匹配的对照组进行了比较。对糖尿病病史较长的儿童使用 Western Blotting 进行了靶向确认,并应用了尿脂质组学方法。为了明确观察到的改变是否与糖尿病肾病有关,还检查了患有或不患有白蛋白尿的糖尿病成年人的尿液。这是第一次显示,与 DN 显著和特异性相关的前列腺素和神经酰胺的脂质代谢已经在最近被诊断为糖尿病的儿童中发生改变。需要对更大的队列进行进一步的研究,以提高这些发现的有效性和普遍性。数据可通过 ProteomeXchange 获得,标识符为 PXD011183 提交详细信息:项目名称:二维电泳和 LC-MS/MS 尿液蛋白质组学。项目编号:PXD011183 项目 DOI:https://doi.org/10.6019/PXD011183 意义:肾病是一种非常常见的糖尿病并发症。一旦发生,其进展只能减缓,但在极少数情况下可以完全控制或缓解,因此对全球健康造成了很大的负担。糖尿病肾病 (DN) 的第一个证据是微量白蛋白尿,但只有 30%的微量白蛋白尿患者进展为蛋白尿,而在一些患者中,它会自发恢复正常白蛋白尿。因此,非常需要能够准确预测发生 DN 风险的生物标志物。在此,通过对尿液样本进行蛋白质组学和脂质组学方法的应用,我们表明前列腺素和神经酰胺代谢的改变与 DN 特异性相关。有趣的是,我们证明这些代谢途径的修饰是糖尿病患者的早期事件,提示鉴定出的改变蛋白作为糖尿病诱导的肾功能下降的可能预测生物标志物。
