Abstract

This proposal is in response to """"""""Program Announcement (PA) Number: PA-10-212 issued by the National Insti- tute of Allergy and Infectious Diseases (NIAID), National Institutes of Health (NIH), which solicits grant applications from institutions/organizations that propose to develop improved HIV incidence assays with increased specificity and reliability for distinguishing incident from chronic HIV infections."""""""" The stated motivation is to improve the ability to estimate the incidence of HIV infection in order to better control the epidemic. Our proposed method focuses on addressing three important shortcomings associated with current measuring methods: low specificity, low sensitivity and sampling bias. To address these shortcomings, we first introduce a novel entropy measure associated with the viral genome, which will distinguish between recent and long term infections among seropos- itive individuals who test negative on the BED HIV-1 Capture EIA assay, or the best available screening assay. This will increase the overall specificity of the assay. Second, we propose a pooling strategy to lower the cost and increase the accuracy of directly identifying individuals in the critical acute phase of the incidence curve, thus increasing the efficiency and sensitivity of the overall procedure, especially during the period when the anti- body assays have extremely low (or even zero) sensitivity for detecting infection. And third, we propose a way to take advantage of the anonymity afforded by pooled testing to overcome a high non-consent-to-testing rate and its concomitant bias-a non-consent rate that in some studies is sufficiently high to make those survey results suspect. Combining these three proposed advances provides a principled testing method for a cross-sectional estimator of incidence that is cost-effective, timely and reliable. Moreover, in addition to the direct response to the PA we propose a method for estimating the instantaneous incidence curve-rather than a single number-that provides a superior perspective of the progressing epidemic. Because our proposed methods all employ existing technologies in a novel way and do not require any new technological breakthroughs, they offer a high probability of success with only a minimal risk of failure.

Public Health Relevance

Our project takes aim at three serious shortcomings of the existing cross-sectional incidence estimators [1]: 1. the lack of long-term specificity associated with properly classifying seropositive individuals who test negative on the BED HIV-1 Capture EIA assay;2. the lack of sensitivity and the high costs associated with finding patients in the acute phase of infection;and, 3. the potentially sizable sampling bias introduced by individuals who withhold consent for HIV testing. By basing our cross-sectional method on both a measure of entropy associated with the viral genome so as to age the infection and on pooling methods that target the additional shortcomings, our resultant estimator is not only cost-effective and timely but also principled and reliable, uniquely correcting on multiple levels a number of current deficiencies. Our methods attempt to be cost-effective particularly to be implementable in economically constrained countries.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI097015-03
Application #
8616714
Study Section
AIDS Clinical Studies and Epidemiology Study Section (ACE)
Program Officer
Sharma, Usha K
Project Start
2012-03-01
Project End
2016-02-28
Budget Start
2014-03-01
Budget End
2015-02-28
Support Year
3
Fiscal Year
2014
Total Cost
$408,430
Indirect Cost
$158,430

  Institution

Name
Harvard University
Department
Biostatistics & Other Math Sci
Type
Schools of Public Health
DUNS #
149617367
City
Boston
State
MA
Country
United States
Zip Code
02115

  Publications

Marino, Miguel; Pagano, Marcello (2018) Role of survey response rates on valid inference: an application to HIV prevalence estimates. Emerg Themes Epidemiol 15:6
Finucane, Mariel M; Rowley, Christopher F; Paciorek, Christopher J et al. (2016) Estimating the prevalence of transmitted HIV drug resistance using pooled samples. Stat Methods Med Res 25:917-35
Hund, Lauren; Bedrick, Edward J; Pagano, Marcello (2015) Choosing a Cluster Sampling Design for Lot Quality Assurance Sampling Surveys. PLoS One 10:e0129564
Wu, Julia Wei; Patterson-Lomba, Oscar; Novitsky, Vladimir et al. (2015) A Generalized Entropy Measure of Within-Host Viral Diversity for Identifying Recent HIV-1 Infections. Medicine (Baltimore) 94:e1865
Patterson-Lomba, Oscar; Wu, Julia W; Pagano, Marcello (2015) Assessing Biases in the Evaluation of Classification Assays for HIV Infection Recency. PLoS One 10:e0139735
Jenkins, Helen E; Tolman, Arielle W; Yuen, Courtney M et al. (2014) Incidence of multidrug-resistant tuberculosis disease in children: systematic review and global estimates. Lancet 383:1572-9
Olives, Casey; Valadez, Joseph J; Pagano, Marcello (2014) Estimation after classification using lot quality assurance sampling: corrections for curtailed sampling with application to evaluating polio vaccination campaigns. Trop Med Int Health 19:321-330
Hund, Lauren; Pagano, Marcello (2014) Extending cluster lot quality assurance sampling designs for surveillance programs. Stat Med 33:2746-57
Gabaitiri, Lesego; Mwambi, Henry G; Lagakos, Stephen W et al. (2013) A likelihood estimation of HIV incidence incorporating information on past prevalence. S Afr Stat J 47:15-31
Hund, Lauren; Pagano, Marcello (2013) Estimating HIV prevalence from surveys with low individual consent rates: annealing individual and pooled samples. Emerg Themes Epidemiol 10:2

Showing the most recent 10 out of 12 publications