Increased Robustness of Single-Molecule Counting with Microfluidics, Digital Isothermal Amplification, and a Mobile Phone versus Real-Time Kinetic Measurements
Abstract
Quantitative bioanalytical measurements are commonly performed in a kinetic format and are known to not be robust to perturbation that affects the kinetics itself or the measurement of kinetics. We hypothesized that the same measurements performed in a "digital" (single-molecule) format would show increased robustness to such perturbations. Here, we investigated the robustness of an amplification reaction (reverse-transcription loop-mediated amplification, RT-LAMP) in the context of fluctuations in temperature and time when this reaction is used for quantitative measurements of HIV-1 RNA molecules under limited-resource settings (LRS). The digital format that counts molecules using dRT-LAMP chemistry detected a 2-fold change in concentration of HIV-1 RNA despite a 6 °C temperature variation (p-value = 6.7 × 10^–7), whereas the traditional kinetic (real-time) format did not (p-value = 0.25). Digital analysis was also robust to a 20 min change in reaction time, to poor imaging conditions obtained with a consumer cell-phone camera, and to automated cloud-based processing of these images (R^2 = 0.9997 vs true counts over a 100-fold dynamic range). Fluorescent output of multiplexed PCR amplification could also be imaged with the cell phone camera using flash as the excitation source. Many nonlinear amplification schemes based on organic, inorganic, and biochemical reactions have been developed, but their robustness is not well understood. This work implies that these chemistries may be significantly more robust in the digital, rather than kinetic, format. It also calls for theoretical studies to predict robustness of these chemistries and, more generally, to design robust reaction architectures. The SlipChip that we used here and other digital microfluidic technologies already exist to enable testing of these predictions. Such work may lead to identification or creation of robust amplification chemistries that enable rapid and precise quantitative molecular measurements under LRS. Furthermore, it may provide more general principles describing robustness of chemical and biological networks in digital formats.
Additional Information
© 2013 American Chemical Society. Received: September 23, 2013; Accepted: October 17, 2013; Published: November 7, 2013. This work was supported in part by DARPA Cooperative Agreement No. HR0011-11-2-0006, NIH grant No. R01EB012946, and NIH grant No. 5DP1OD003584. We thank Whitney Robles for contributions to writing and editing this manuscript. We also thank the five-year-old volunteer for performing the demonstration shown in Video S1.Attached Files
Accepted Version - nihms539046.pdf
Supplemental Material - Single_Molecule_Counting_with_Mobile_Phone_supplementary_information_revised.pdf
Supplemental Material - Video_S1.mpg
Files
Additional details
- PMCID
- PMC3924768
- Eprint ID
- 42341
- DOI
- 10.1021/ac4030413
- Resolver ID
- CaltechAUTHORS:20131108-122433726
- DARPA Cooperative Agreement
- HR0011-11-2-0006
- NIH
- R01EB012946
- NIH Roadmap for Medical Research
- 5DP1OD003584
- Created
-
2013-11-08Created from EPrint's datestamp field
- Updated
-
2021-11-10Created from EPrint's last_modified field