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关于在隐形眼镜上进行荧光捕获免疫测定的可能性。

On the Possibility of Fluorescent Capture Immunoassays on a Contact Lens.

作者信息

Sivashanmugan Kundan, Reece E Albert, Lakowicz Joseph R

机构信息

Center for Fluorescence Spectroscopy, Department of Biochemistry and Molecular Biology, University of Maryland School of Medicine, 721 West Lombard St., Baltimore, MD 21201, USA.

Department of Obstetrics, Gynecology and Reproductive Sciences, University of Maryland School of Medicine, 655 W., Baltimore, MD 21201, USA.

出版信息

Biosensors (Basel). 2025 May 20;15(5):326. doi: 10.3390/bios15050326.

Abstract

Blood samples and testing are routine in healthcare. Presently, there is a growing interest in using tear samples in place of blood. Tear samples can be obtained non-invasively and collection does not require the skills of a trained phlebotomist. Red blood cells and other cells are not present in tears, which avoids centrifugation. Importantly, basal tear samples contain most of the biomarkers present in blood. The difficulty is the small volume of basal tears, which is about 7 μL in each eye. Any contact with the eye results in additional reflex tears with a different chemical composition. The small tear samples are collected with capillary tubes and then sent out for amplified assays, such as enzyme-linked immunosorbent assay (ELISA) or polymerase chain reaction (PCR). The results are not available for several days or a week and, therefore, are less useful in an ophthalmology office. We propose the use of a contact lens that contains bound antibodies for fluorescence immunoassays. The lenses could be removed from the patient for point-of-care measurements at the bedside. To prove that this concept is possible, we performed a three-layer protein capture assay that mimics an immunoassay. For convenience, we used lysozyme (Lys), which spontaneously coats silicon hydrogel (SiHG) contact lenses (CL). Anti-lysozyme IgG was the second layer captured, with anti-lysozyme considered to be the target biomarker. The third layer was rhodamine or Alexa Fluor-labeled Ab against the IgG Fc region, considered to be the detection antibody. The multiple protein layers were stable and did not wash off the SiHG lenses. These results strongly suggest the contact lens can be used for capture immunoassays for a wide variety of biomarkers.

摘要

血液样本采集和检测在医疗保健中很常见。目前,人们越来越有兴趣使用泪液样本替代血液样本。泪液样本采集是非侵入性的,且不需要经过训练的采血技师的技能。泪液中不存在红细胞和其他细胞,因此无需离心。重要的是,基础泪液样本包含血液中存在的大多数生物标志物。困难在于基础泪液的量很少,每只眼睛约为7微升。任何与眼睛的接触都会导致额外的反射泪液,其化学成分不同。小体积的泪液样本用毛细管收集,然后送去进行放大检测,如酶联免疫吸附测定(ELISA)或聚合酶链反应(PCR)。结果要几天或一周后才可得,因此在眼科诊所不太实用。我们建议使用含有结合抗体的隐形眼镜进行荧光免疫测定。这种隐形眼镜可以从患者身上取下,在床边进行即时检测。为了证明这个概念是可行的,我们进行了一项模拟免疫测定的三层蛋白质捕获试验。为方便起见,我们使用了溶菌酶(Lys),它能自发地包被硅水凝胶(SiHG)隐形眼镜(CL)。抗溶菌酶IgG是捕获的第二层,抗溶菌酶被视为目标生物标志物。第三层是针对IgG Fc区域的罗丹明或Alexa Fluor标记的抗体,被视为检测抗体。多层蛋白质在SiHG隐形眼镜上稳定,不会被冲洗掉。这些结果有力地表明,隐形眼镜可用于多种生物标志物的捕获免疫测定。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/211d/12110756/5978fa38a477/biosensors-15-00326-g001.jpg

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