Circulating microRNA Biomarkers as Liquid Biopsy for Cancer Patients: Pros and Cons of Current Assays
Abstract
:1. Introduction
Types of Cancer | Source | Anticoagulant | Volume (mL) | Isolation Method | Controls | Detection Method | References |
---|---|---|---|---|---|---|---|
Diffuse large B-cell lymphoma | Serum | N/A | 2 | TRIzol | miR-16 | RT-qPCR | [24] |
Prostate | Serum/Plasma | EDTA | 10 | mirVana PARIS | Cel-miRs | RT-qPCR pre-amp | [18] |
NSCLC* | Serum/Plasma | Heparin | 0.1 | Total RNA purification kit | Cel-miRs | RT-qPCR | [25] |
NSCLC* | Serum | N/A | 0.5 | mirVana PARIS | dCt matrix | RT-qPCR | [26] |
NSCLC* | Serum | N/A | 50 | TRIzol | Normalization to total RNA | RT-qPCR, sequencing | [27] |
NSCLC* | Plasma EV | U | 3 | Dynabeads mirVana PARIS | miR-142-3p,-30b | RT-qPCR | [28] |
Lung | Plasma | EDTA | 0.2 | mirVana PARIS | RNU-6B | Microarray; RT-qPCR | [29] |
HCC** | Plasma | U | 0.25 | miRNeasy | U6 snRNA; cel-miR-39 | RT-qPCR TLDA cards A and B | [30] |
Head and Neck | Plasma | EDTA | 0.3 | mirVana miRNA isolation kit | Cel-miR-39 | TaqMan Array RT-qPCR | [31] |
Gastric | Plasma | N/A | N/A | miRNeasy Mini kit | Cel-miR-39 | RT-qPCR | [32] |
HCC** | Plasma | N/A | N/A | N/A | miR-1228 | RT-qPCR microarrays | [33] |
RCC*** | Serum | N/A | 0.4 | mirVana PARIS Kit | Cel-miR-39 | RT-qPCR | [34] |
Breast | Serum | N/A | N/A | N/A | miR-16 | RT-qPCR-DS | [35] |
Melanoma | Plasma | Sodium citrate | 0.01 | N/A | N/A | RT-qPCR-DP | [36] |
Multiple myeloma | Serum | N/A | N/A | N/A | N/A | NanoString, RT-qPCR | [37] |
2. Blood Collection and Processing
3. RNA Extraction Methods: Quantity and Quality Assessment of cmiRNA
3.1. RNA Extraction
Kit | Company | Sample Type | Remarks |
---|---|---|---|
mirVana™ PARIS™ Kit | Life technologies (Carlsbad, CA, USA) | Tissues, Cells | Protein can be isolated from the same sample |
miRNeasy® Mini Kit | QIAGEN (Venlo, Limburg, Blegium) | Tissues, Cells | |
miRCURY™ RNA Isolation Kits | EXIQON (Vedbaek, Denmark) | Biofluids, Tissues, Cells, FFPE | Biofluids can be used as sources |
mirPremier™ microRNA Isolation Kit | SIGMA-ALDRICH (St. Louis, MO, USA) | Tissues, Cells | No phenol and chloroform |
miRNA Isolation Kit | FAVORGEN (Ping-Tung, Taiwan) | Tissues, Cells | No large RNA |
MasterPure™ RNA Purification Kit | Epicenter (Madison, WI, USA) | Tissues, Cells | No spin column, No phenol and chloroform |
microRNA Isolation Kit, Human Ago2 | Wako (Osaka, Japan) | Tissues, Cells | IP* with human anti-Ago2 Ab |
miRNA Purification & Isolation Kit | Takara/Clontech (Shiga, Japan) | Tissues, Cells | Protein can be isolated from the same sample. |
3.2. Quantity and Quality Assessment of miRNA
4. Methodological Variations of cmiRNA Detection Profiling
Sensitivity | Specificity | Accuracy | Analysis | Reproducibility | Discovery | |
---|---|---|---|---|---|---|
RT-qPCR | ++++ | ++++ | ++++ | Easy | ++++ | Impossible |
Affymetrix GeneChip miRNA Arrays 4.0 | + | + | + | Moderate | + | Impossible |
Agilent oligonucleotides microarrays | + | + | + | Moderate | + | Impossible |
Exiqon miRCURY LNA microRNA arrays | ++ | ++ | ++ | Moderate | + | Impossible |
µParaflo®Microfluidic Biochip Technology | + | + | + | Moderate | + | Impossible |
3D-Gene® | +++ | +++ | +++ | Moderate | ++ | Impossible |
Next-generation sequencing | ++ | ++ | ++ | Difficult | + | Possible |
4.1. RT-qPCR
4.2. Microarray
Assay | Required Input (ng) | Probe Content |
---|---|---|
Affymetrix GeneChip miRNA Arrays 4.0 | 130 | miRBase v.20 |
Agilent oligonucleotides microarrays | 100 | miRBase v.21 |
Exiqon miRCURY LNA microRNA arrays | 30 | miRBase v.19 |
µParaflo®Microfluidic Biochip Technology | 1000 | miRBase v.21 |
3D-Gene® | 250 | miRBase v.21 |
4.3. Next-Generation Sequencing
5. Discussion
6. Conclusions
Acknowledgments
Author Contributions
Conflicts of Interest
References
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Ono, S.; Lam, S.; Nagahara, M.; Hoon, D.S.B. Circulating microRNA Biomarkers as Liquid Biopsy for Cancer Patients: Pros and Cons of Current Assays. J. Clin. Med. 2015, 4, 1890-1907. https://doi.org/10.3390/jcm4101890
Ono S, Lam S, Nagahara M, Hoon DSB. Circulating microRNA Biomarkers as Liquid Biopsy for Cancer Patients: Pros and Cons of Current Assays. Journal of Clinical Medicine. 2015; 4(10):1890-1907. https://doi.org/10.3390/jcm4101890
Chicago/Turabian StyleOno, Shigeshi, Stella Lam, Makoto Nagahara, and Dave S. B. Hoon. 2015. "Circulating microRNA Biomarkers as Liquid Biopsy for Cancer Patients: Pros and Cons of Current Assays" Journal of Clinical Medicine 4, no. 10: 1890-1907. https://doi.org/10.3390/jcm4101890
APA StyleOno, S., Lam, S., Nagahara, M., & Hoon, D. S. B. (2015). Circulating microRNA Biomarkers as Liquid Biopsy for Cancer Patients: Pros and Cons of Current Assays. Journal of Clinical Medicine, 4(10), 1890-1907. https://doi.org/10.3390/jcm4101890