Programming bulk enzyme heterojunctions for biosensor development with tetrahedral DNA framework.
Ping SongJuwen ShenDekai YeBaijun DongFei WangHao PeiJianbang WangJiye ShiLihua WangWei XueYiran HuangGang HuangXiaolei ZuoChun-Hai FanPublished in: Nature communications (2020)
Protein-protein interactions are spatially regulated in living cells to realize high reaction efficiency, as seen in naturally existing electron-transfer chains. Nevertheless, arrangement of chemical/biochemical components at the artificial device interfaces does not possess the same level of control. Here we report a tetrahedral DNA framework-enabled bulk enzyme heterojunction (BEH) strategy to program the multi-enzyme catalytic cascade at the interface of electrochemical biosensors. The construction of interpenetrating network of BEH at the millimeter-scale electrode interface brings enzyme pairs within the critical coupling length (CCL) of ~10 nm, which in turn greatly improve the overall catalytic cascade efficiency by ~10-fold. We demonstrate the BEH generality with a range of enzyme pairs for electrochemically detecting clinically relevant molecular targets. As a proof of concept, a BEH-based sarcosine sensor enables single-step detection of the metabolic biomarker of sarcosine with ultrasensitivity, which hold the potential for precision diagnosis of early-stage prostate cancer.
Keyphrases
- living cells
- electron transfer
- single molecule
- prostate cancer
- early stage
- fluorescent probe
- label free
- circulating tumor
- gold nanoparticles
- photodynamic therapy
- transcription factor
- risk assessment
- radiation therapy
- human health
- ionic liquid
- rectal cancer
- sentinel lymph node
- carbon nanotubes
- drug induced
- solid state
- neoadjuvant chemotherapy
- molecularly imprinted
- loop mediated isothermal amplification
- light emitting