A Universal DNA Aptamer that Recognizes Spike Proteins of Diverse SARS‐CoV‐2 Variants of Concern

Zhang, Zijie; Li, Jiuxing; Gu, Jimmy; Amini, Ryan; Stacey, Hannah D.; Ang, Jann C.; White, Dawn; Filipe, Carlos D. M.; Mossman, Karen; Miller, Matthew S.; Salena, Bruno J.; Yamamura, Deborah; Sen, Payel; Soleymani, Leyla; Brennan, John D.; Li, Yingfu

doi:10.1002/chem.202200078

Cited by 48 publications

(63 citation statements)

References 38 publications

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“…For example, the ranking of MSA52R1 increased from 46 th in the WH pool to 14 th in the CA pool, producing a ranking increase of 69.5 %. [38] The results once again confirmed that the members in this family competed well for the binding of all four variants used for selection. Taken together, the sequencing analysis identified MSA52 as a universal aptamer candidate for the S protein.…”

Section: Selection Of Universal Aptamerssupporting

confidence: 62%

“…However, the ranking of MSA52 increased to 24 th , 19 th , 17 th , and 14 th after one‐round selection with the S protein from the UK (UKS), Brazil (BZS), South Africa (SAS), and California (CAS) variants, respectively, but remained largely unchanged (with a ranking of 46 th ) in the pool with the wildtype S protein (WHS). [38] These observations indicate that MSA52 competed favorably for binding all four S protein variants with the top‐ranking sequences established using WHS, pointing to the possibility of this aptamer being the universal aptamer that we were searching for.…”

Section: Selection Of Universal Aptamersmentioning

confidence: 87%

“…This was the foundational hypothesis examined by us in a recent study. [38] To find these aptamers quickly, we carried out five parallel one‐round SELEX experiments with the G13 pool using five different S proteins as the binding targets (Figure 4 A). These variants were: the wildtype S protein plus the S proteins from B.1.1.7 (Alpha, United Kingdom, UK), B.1.351 (Beta, South Africa, SA), P.1 (Gamma, Brazil, BZ) and B.1.429 (Epsilon, California, CA) variants, all of which were commercially available at the time of the experiment.…”

Section: Selection Of Universal Aptamersmentioning

confidence: 99%

“…The amplified DNA pools were then subjected to high‐throughput sequencing, followed by a comparative analysis of abundance changes of the aptamer sequences in these pools. [38] …”

Section: Selection Of Universal Aptamersmentioning

confidence: 99%

“…The sequence and predicted secondary structure of MSA52 were provided in Figure 5 A. [38] MSA52 consists of 79 nucleotides and the overall structure contains 4 pairing arms (P1, P2, P3 and P4) and 7 unpaired elements (SS12, SS23, SS34, SS41, and the loops L2, L3, L4). P1 was the pairing arm that was pre‐designed in the structure of the library (Figure 3 A).…”

Section: Selection Of Universal Aptamersmentioning

confidence: 99%

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One Solution for All: Searching for Universal Aptamers for Constantly Mutating Spike Proteins of SARS‐CoV‐2

Zhang

Amini

et al. 2022

ChemMedChem

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Aptamers that can recognize the spike (S) protein of SARS-CoV-2 with high affinity and specificity are useful molecules towards the development of diagnostics and therapeutics to fight COVID-19. However, this S protein is constantly mutating, producing variants of concern (VoCs) that can significantly weaken the binding by aptamers initially engineered to recognize the S protein of the wildtype virus or a specific VoC. One strategy to overcome this problem is to develop universal aptamers that are insensitive to all or most of the naturally emerging mutations in the protein. We have recently demonstrated this concept by subjecting a pool of S protein-binding DNA aptamers for one-round parallel-SELEX experiments targeting 5 different S protein variants for binding-based sequence enrichment, followed by bioinformatic analysis of the enriched pools. This effort has led to the identification of a universal aptamer that recognizes 8 different variants of the spike protein with equally excellent affinity.

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Section: Selection Of Universal Aptamerssupporting

confidence: 62%

Section: Selection Of Universal Aptamersmentioning

confidence: 87%

Section: Selection Of Universal Aptamersmentioning

confidence: 99%

“…The amplified DNA pools were then subjected to high‐throughput sequencing, followed by a comparative analysis of abundance changes of the aptamer sequences in these pools. [38] …”

Section: Selection Of Universal Aptamersmentioning

confidence: 99%

Section: Selection Of Universal Aptamersmentioning

confidence: 99%

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One Solution for All: Searching for Universal Aptamers for Constantly Mutating Spike Proteins of SARS‐CoV‐2

Zhang

Amini

et al. 2022

ChemMedChem

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A DNA Barcode‐Based Aptasensor Enables Rapid Testing of Porcine Epidemic Diarrhea Viruses in Swine Saliva Using Electrochemical Readout

et al. 2022

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Pen-side testing of farm animals for infectious diseases is critical for preventing transmission in herds and providing timely intervention. However, most existing pathogen tests have to be conducted in centralized labs with sample-to-result times of 2-4 days. Herein we introduce a test that uses a dual-electrode electrochemical chip (DEE-Chip) and a barcode-releasing electroactive aptamer for rapid on-farm detection of porcine epidemic diarrhea viruses (PEDv). The sensor exploits inter-electrode spacing reduction and active field mediated transport to accelerate barcode movement from electroactive aptamers to the detection electrode, thus expediting assay operation. The test yielded a clinically relevant limit-of-detection of 6 nM (0.37 μg mL À 1 ) in saliva-spiked PEDv samples. Clinical evaluation of this biosensor with 12 porcine saliva samples demonstrated a diagnostic sensitivity of 83 % and specificity of 100 % with a concordance value of 92 % at an analysis time of one hour.

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A Colorimetric Biosensing Platform with Aptamers, Rolling Circle Amplification and Urease‐Mediated Litmus Test

Chang,

Li,

Liu

et al. 2023

Angewandte Chemie

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Here we report on an ultra‐sensitive colorimetric sensing platform that takes advantage of both the strong amplification power of rolling circle amplification (RCA) and the high efficiency of a simple urease‐mediated litmus test. The presence of a target triggers the RCA reaction, and urease‐labelled DNA can hybridize to the biotinylated RCA products and be immobilized onto streptavidin‐coated magnetic beads. The urease‐laden beads are then used to hydrolyze urea, leading to an increase in pH that can be detected by a simple litmus test. We show this sensing platform can be easily integrated with aptamers for sensing diverse targets via the detection of human thrombin and platelet‐derived growth factor (PDGF) utilizing structure‐switching aptamers as well as SARS‐CoV‐2 in human saliva using a spike‐binding trimeric DNA aptamer. Furthermore, we demonstrate that this colorimetric sensing platform can be integrated into a simple paper‐based device for sensing applications.

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A Universal DNA Aptamer that Recognizes Spike Proteins of Diverse SARS‐CoV‐2 Variants of Concern

Cited by 48 publications

References 38 publications

One Solution for All: Searching for Universal Aptamers for Constantly Mutating Spike Proteins of SARS‐CoV‐2

One Solution for All: Searching for Universal Aptamers for Constantly Mutating Spike Proteins of SARS‐CoV‐2

A DNA Barcode‐Based Aptasensor Enables Rapid Testing of Porcine Epidemic Diarrhea Viruses in Swine Saliva Using Electrochemical Readout

A Colorimetric Biosensing Platform with Aptamers, Rolling Circle Amplification and Urease‐Mediated Litmus Test

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