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探索 RBP3 结构与类视黄醇结合以实现眼部活体功能成像:用于糖尿病视网膜病变的新型生物标志物。

Towards a New Biomarker for Diabetic Retinopathy: Exploring RBP3 Structure and Retinoids Binding for Functional Imaging of Eyes In Vivo.

机构信息

Institute of Physical Chemistry, Polish Academy of Sciences, 01-224 Warsaw, Poland.

Integrated Structural Biology Group, International Centre for Translational Eye Research, Institute of Physical Chemistry, Polish Academy of Sciences, 01-224 Warsaw, Poland.

出版信息

Int J Mol Sci. 2023 Feb 23;24(5):4408. doi: 10.3390/ijms24054408.

Abstract

Diabetic retinopathy (DR) is a severe disease with a growing number of afflicted patients, which places a heavy burden on society, both socially and financially. While there are treatments available, they are not always effective and are usually administered when the disease is already at a developed stage with visible clinical manifestation. However, homeostasis at a molecular level is disrupted before visible signs of the disease are evident. Thus, there has been a constant search for effective biomarkers that could signal the onset of DR. There is evidence that early detection and prompt disease control are effective in preventing or slowing DR progression. Here, we review some of the molecular changes that occur before clinical manifestations are observable. As a possible new biomarker, we focus on retinol binding protein 3 (RBP3). We argue that it displays unique features that make it a very good biomarker for non-invasive, early-stage DR detection. Linking chemistry to biological function and focusing on new developments in eye imaging and two-photon technology, we describe a new potential diagnostic tool that would allow rapid and effective quantification of RBP3 in the retina. Moreover, this tool would also be useful in the future to monitor therapeutic effectiveness if levels of RBP3 are elevated by DR treatments.

摘要

糖尿病视网膜病变(DR)是一种严重的疾病,患者数量不断增加,给社会带来了沉重的负担,无论是在社会还是经济方面。虽然有治疗方法,但并不总是有效,而且通常在疾病已经发展到可见临床症状的阶段才进行治疗。然而,在疾病出现明显迹象之前,分子水平的内稳态已经被破坏。因此,一直在寻找有效的生物标志物,以提示 DR 的发生。有证据表明,早期发现和及时控制疾病可以有效预防或减缓 DR 的进展。在这里,我们回顾了一些在可观察到临床症状之前发生的分子变化。作为一种可能的新生物标志物,我们专注于视黄醇结合蛋白 3(RBP3)。我们认为,它具有独特的特征,使其成为一种非常好的非侵入性、早期 DR 检测的生物标志物。我们将化学与生物学功能联系起来,并专注于眼部成像和双光子技术的新发展,描述了一种新的潜在诊断工具,该工具将允许快速有效地定量视网膜中的 RBP3。此外,如果 DR 治疗导致 RBP3 水平升高,该工具在未来也将有助于监测治疗效果。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4d60/10002987/20694d041080/ijms-24-04408-g001.jpg

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