| Id |
Subject |
Object |
Predicate |
Lexical cue |
| T578 |
0-47 |
Sentence |
denotes |
2.2.6 Cell- and molecularly-imprinted polymers |
| T579 |
48-440 |
Sentence |
denotes |
Given traditional biorecognition elements used in biosensing exhibit stability concerns, such as antibodies or aptamers, as discussed in Sections 2.2.1–2.2.4, there have been efforts to create engineered molecular biorecognition elements, such as scFvs. In contrast, materials-based biorecognition elements exploit the principle of target-specific morphology for selective capture (Pan et al. |
| T580 |
441-458 |
Sentence |
denotes |
2018; Zhou et al. |
| T581 |
459-465 |
Sentence |
denotes |
2019). |
| T582 |
466-619 |
Sentence |
denotes |
The most common approach in materials-based biorecognition is based on cell- and molecularly-imprinted polymers (CIPs and MIPs, respectively) (Gui et al. |
| T583 |
620-626 |
Sentence |
denotes |
2018). |
| T584 |
627-782 |
Sentence |
denotes |
CIPs and MIPs have been created using various processes, including bacteria-mediated lithography, micro-contact stamping, and colloid imprints (Chen et al. |
| T585 |
783-800 |
Sentence |
denotes |
2016a; Pan et al. |
| T586 |
801-807 |
Sentence |
denotes |
2018). |
| T587 |
808-1030 |
Sentence |
denotes |
As shown in Fig. 3b, Jafari et al. used imprinted organosilica sol-gel films of tetraethoxysilane and (3-mercaptopropyl)trimethoxysilane (MPTS) for selective detection of E. coli using an impedimetric method (Jafari et al. |
| T588 |
1031-1037 |
Sentence |
denotes |
2019). |
| T589 |
1038-1191 |
Sentence |
denotes |
Similarly, Golabi et al. used imprinted poly(3-aminophenylboronic acid) films for detection of Staphylococcus epidermidis (S. epidermidis) (Golabi et al. |
| T590 |
1192-1198 |
Sentence |
denotes |
2017). |
| T591 |
1199-1405 |
Sentence |
denotes |
Despite the absence of a highly selective molecular biorecognition element, CIPs and MIPs exhibit selectivity when exposed to samples that contain multiple analytes (i.e., non-target species) (Golabi et al. |
| T592 |
1406-1425 |
Sentence |
denotes |
2017; Jafari et al. |
| T593 |
1426-1441 |
Sentence |
denotes |
2019; Qi et al. |
| T594 |
1442-1448 |
Sentence |
denotes |
2013). |
| T595 |
1449-1539 |
Sentence |
denotes |
MIPs and CIPs are also of interest with regard to opportunities in biosensor regeneration. |
| T596 |
1540-1723 |
Sentence |
denotes |
Common adverse effects of regeneration on biosensors that employ molecular biorecognition elements, such as irreversible changes in structure, are less likely to affect MIPs and CIPs. |
| T597 |
1724-1923 |
Sentence |
denotes |
However, it is generally accepted that current CIPs and MIPs exhibit lower selectivity to target species than antibodies and aptamers due to reduction of available chemical selectivity (Cheong et al. |
| T598 |
1924-1975 |
Sentence |
denotes |
2013; Kryscio and Peppas, 2012; Yáñez-Sedeño et al. |
| T599 |
1976-1982 |
Sentence |
denotes |
2017). |
