Boronic Acid‐Rich Lanthanide Metal‐Organic Frameworks Enable Deep Proteomics with Ultratrace Biological Samples

材料科学 镧系元素 硼酸 纳米技术 蛋白质组学 金属有机骨架 组合化学 有机化学 生物化学 生物 化学 离子 吸附 基因
作者
Shuang Zhang,Behafarid Ghalandari,Youming Chen,Qingwen Wang,Kun Liu,Xinyi Sun,Xinwen Ding,Sunfengda Song,Lai Jiang,Xianting Ding
出处
期刊:Advanced Materials [Wiley]
卷期号:36 (33) 被引量:1
标识
DOI:10.1002/adma.202401559
摘要

Label-free proteomics is widely used to identify disease mechanism and potential therapeutic targets. However, deep proteomics with ultratrace clinical specimen remains a major technical challenge due to extensive contact loss during complex sample pretreatment. Here, a hybrid of four boronic acid-rich lanthanide metal-organic frameworks (MOFs) with high protein affinity is introduced to capture proteins in ultratrace samples jointly by nitrogen-boronate complexation, cation-π and ionic interactions. A MOFs Aided Sample Preparation (MASP) workflow that shrinks sample volume and integrates lysis, protein capture, protein digestion and peptide collection steps into a single PCR tube to minimize sample loss caused by non-specific absorption, is proposed further. MASP is validated to quantify ≈1800 proteins in 10 HEK-293T cells. MASP is applied to profile cerebrospinal fluid (CSF) proteome from cerebral stroke and brain damaged patients, and identified ≈3700 proteins in 1 µL CSF. MASP is further demonstrated to detect ≈9600 proteins in as few as 50 µg mouse brain tissues. MASP thus enables deep, scalable, and reproducible proteome on precious clinical samples with low abundant proteins.
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