4.8 Article

The heparinase-linked differential time method allows detection of heparin potency in whole blood with high sensitivity and dynamic range

Journal

BIOSENSORS & BIOELECTRONICS
Volume 198, Issue -, Pages -

Publisher

ELSEVIER ADVANCED TECHNOLOGY
DOI: 10.1016/j.bios.2021.113856

Keywords

Anticoagulation therapy; Heparin potency; Heparinase; Two-zone on one sensor; Thrombin; Biosensor

Funding

  1. National Key R&D Program of China [2021YFB3201202]
  2. National Natural Science Foundation of China [61874133, 61901469, 22005331]
  3. Key Research and Development Program of Jiangsu Province [BE2018080, BE2019684, BE2020768]
  4. Jiangsu Provincial Policy Guidance Program [BZ2019069]
  5. Jihua Laboratory Foundation [X190181TD190]
  6. Youth Innovation Promotion Association CAS [2019322, 2018360, Y201856]
  7. Instrument Developing Project of the Chinese Academy of Sciences [YJKYYQ20190057, YJKYYQ20200046, ZDKYYQ20210004]
  8. Science and Technology Development Program of Suzhou [SYG201907]
  9. Self-deployment Projects of Suzhou Institute of Biomedical Engineering and Technology, CAS [Y851591105]
  10. Tianjin Science and Technology Project [19YFYSQY00040]
  11. Suzhou Science and Technology Program [SLT202005]
  12. Suzhou Municipal Commission of Health and Family Planning [LCZX202031]
  13. Suzhou New District Science and Technology Plan [2019Z009]

Ask authors/readers for more resources

A novel HLDT method was developed using a GR-C sensor to quantitatively evaluate heparin potency in whole blood. The method demonstrated high selectivity for heparin potency in 10 μL of whole blood with a detection limit of 0.1 U/mL.
Anticoagulation therapy with heparin is an effective treatment against thrombosis. Heparin tends to cause spontaneous bleeding and requires regular monitoring during therapy. Most high-sensitivity heparin sensors have focused on the concentration detection in clarified buffer solution. However, the pharmacodynamics of heparin vary depending on individual patient or disease, while potency detection with high sensitivity and dynamic range outperforms concentration detection in clinical diagnosis. In this study, a novel heparinase-linked differential time (HLDT) method was established with a two-zone of Graphene modified Carbon (GR-C) sensor, which was utilized to evaluate heparin potency in whole blood. It was based on electrochemical measurement of clotting time shifting associated with presence or absence of heparinase. Heparinase inhibits the anticoagulant ability of heparin by forming a heparin-antithrombin-thrombin complex during coagulation. And the intensity and peak time of electrochemical current were associated with thrombin activity and clotting on the electrode. The results demonstrated that the sensor had high selectivity for heparin potency in 10 mu L of whole blood with a detection limit of 0.1 U/mL, and the linear detection range was 0.1-5 U/mL. The coefficient of variation (CV) of the peak time was less than 5%, and linear correlation between the GR-C sensor and the TEG-5000 instrument was 0.987. Thus, the HLDT method has better clinical application due to its good repeatability, high sensitivity and wide range in heparin potency evaluation.

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