Affiliation:
1. Department of Biology, Faculty of Basic Science Payame Noor University Tehran Iran
2. Cellular and Molecular Research Center, Research Institute of Cellular and Molecular Sciences in Infectious Diseases Zahedan University of Medical Sciences Zahedan Iran
3. Department of Advanced Sciences and Technologies in Medicine, School of Medicine North Khorasan University of Medical Sciences Bojnurd Iran
4. Natural Products and Medicinal Plants Research Center North Khorasan University of Medical Sciences Bojnurd Iran
5. Department of Chemical Engineering, Faculty of Engineering University of Tehran Tehran Iran
6. Pharmacology Research Center Zahedan University of Medical Sciences Zahedan Iran
7. Department of Biochemistry, Faculty of Biology and Biotechnology University of Warmia and Mazury Olsztyn Poland
8. Department of Physics University of Zabol Zabol Iran
9. Universidad de Alcalá, Facultad de Ciencias Departamento de Quimica Analitica, Quimica Fisica e Ingenieria Quimica Madrid Spain
Abstract
AbstractAptamers (Apts) are synthetic nucleic acid ligands that can be engineered to target various molecules, including amino acids, proteins, and pharmaceuticals. Through a series of adsorption, recovery, and amplification steps, Apts are extracted from combinatorial libraries of synthesized nucleic acids. Using aptasensors in bioanalysis and biomedicine can be improved by combining them with nanomaterials. Moreover, Apt‐associated nanomaterials, including liposomes, polymeric, dendrimers, carbon nanomaterials, silica, nanorods, magnetic NPs, and quantum dots (QDs), have been widely used as promising nanotools in biomedicine. Following surface modifications and conjugation with appropriate functional groups, these nanomaterials can be successfully used in aptasensing. Advanced biological assays can use Apts immobilized on QD surfaces through physical interaction and chemical bonding. Accordingly, modern QD aptasensing platforms rely on interactions between QDs, Apts, and targets to detect them. QD‐Apt conjugates can be used to directly detect prostate, ovarian, colorectal, and lung cancers or simultaneously detect biomarkers associated with these malignancies. Tenascin‐C, mucin 1, prostate‐specific antigen, prostate‐specific membrane antigen, nucleolin, growth factors, and exosomes are among the cancer biomarkers that can be sensitively detected using such bioconjugates. Furthermore, Apt‐conjugated QDs have shown great potential for controlling bacterial infections such as Bacillus thuringiensis, Pseudomonas aeruginosa, Escherichia coli, Acinetobacter baumannii, Campylobacter jejuni, Staphylococcus aureus, and Salmonella typhimurium. This comprehensive review discusses recent advancements in the design of QD‐Apt bioconjugates and their applications in cancer and bacterial theranostics.