More than 5 million individuals in the United States have clinically manifest Heart Failure (HF), and that number continues to rise with the country's aging population, contributing to serious strains on our healthcare system and to huge economic costs. Diagnosing and managing the cardiovascular health concerns for such a large population, particularly the elderly who often also suffer from diabetes, has created a growing need for new healthcare technologies that will help: (1) accommodate the physical challenges of aging and diabetic HF patients and (2) lower medical cost and the strain on healthcare resources. Elevated levels of natriuretic peptide biomarkers NT-proBNP and BNP indicate the presence of myocardial stress, and in people with HF, these have been shown to correlate with acute exacerbations of this condition. Quantitation of natriuretic peptide levels is critical to th determination of appropriate emergency and clinical treatment, and currently the only blood-based assay that exists for the diagnosis of myocardial stress and management of HF. Studies where natriuretic peptides were used to guide drug therapies and diagnostics suggest reduced mortality and a significantly lowered number and duration of hospital stays, and that there is additional prognostic value of establishing an individual's baseline level of NT-proBNP. This simple, effective means of monitoring and diagnosis of cardiovascular health, combined with a technologically accurate and demographically relevant means of testing for a robust HF biomarker, presents a simple and compelling opportunity to provide support for the growing population of aging, diabetic HF patients. Our approach to sensor design is somewhat risky, and though our preliminary results are encouraging, we hope to use the R21 mechanism to unambiguously demonstrate quantitative NT-proBNP assay efficacy on an inexpensive electrochemical sensor with an LOD of <1 nM within 5 minutes in buffer (Aim 1). This will be followed in Aim 2 by buffer-based optimization studies with the goal of obtaining a dynamic NT-proBNP detection range of 53 - 212 pM (450 - 1,800 pg/mL). We will also determine coefficients of variation (CVs) and device stability at this stage. Once we are confident of NT-proBNP assay efficacy in buffer, we will then proceed to Aim 3, optimizing the assay in spiked, pooled human plasma and spiked, pooled human whole blood. If this project is successful, we will expand it to a more resource-intensive R01 study that will include: design and development of a reader and patient-user interface, development of data analysis and communication software to transmit results between patient and physician, and conduct of trials to evaluate the effectiveness of the device and its interface. Our ultimate goal is to create a means for HF patients to monitor a key cardiac biomarker at home for the first time. The opportunity to improve clinical decision-making, especially in relation to hospitalization and return to the community, directly addresses the NIH mission to improve quality of care, reduce costs, and to more closely couple physiological changes to medical intervention.

Public Health Relevance

Diagnosing and managing the cardiovascular health for a growing population of patients in the United States, particularly the elderly and those who also suffer from diabetes, has created a growing need for new technologies and processes to help: (1) alleviate stretched healthcare resources and (2) accommodate the physical challenges that these patients face. The proposed research aims to adapt a novel sandwich antibody detection assay for NT-proBNP (an accepted and physiologically robust biomarker for heart failure) to an inexpensive in-home test, the results of which can then be transmitted to the individual's physician for diagnosis and patient care planning. In-home monitoring of cardiovascular health stands the chance of making a real impact on patient quality of life by providing timely individualized care, decreasing the number of ER visits patients must endure, and diminishing the financial strain such visits impose on these patients and on our healthcare system.

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Exploratory/Developmental Grants (R21)
Project #
5R21HL128199-02
Application #
9102226
Study Section
Special Emphasis Panel (ZRG1)
Program Officer
Iturriaga, Erin
Project Start
2015-07-01
Project End
2017-04-30
Budget Start
2016-05-01
Budget End
2017-04-30
Support Year
2
Fiscal Year
2016
Total Cost
Indirect Cost
Name
University of Texas Austin
Department
Chemistry
Type
Schools of Arts and Sciences
DUNS #
170230239
City
Austin
State
TX
Country
United States
Zip Code
78712
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