Abstract

Early diagnosis of systemic infection in humans and prediction of clinical outcome both remain elusive, despite the critical need for both. The two basic approaches for diagnosis and prognosis, direct identification of the infectious agent and measurement of host response features, have been limited by reliance on cultivation, pre-test assumptions about specific agents, limited breadth of coverage, and an insufficient signal-to-noise ratio. Recent advances in DNA sequencing technology and computational tools for data analysis provide new opportunities for characterizing complex mixtures of DNA and RNA molecules in a minimally-biased fashion, and for detecting rare sequences of interest in clinical specimens. The goals of this project are to characterize microbial and viral genomic sequences in the peripheral blood of healthy subjects, as well as subjects with fever (and in some cases, known causative infectious agents) at the time of clinical presentation, to characterize human genome-wide RNA patterns in peripheral blood, and then to integrate these complementary forms of data so as to derive putative diagnostic and prognostic signatures for systemic infection. We propose three aims; (1) characterize microbial and viral sequences and host RNAs in peripheral blood of non-febrile, healthy subjects; (2) characterize microbial and viral sequences and host RNAs in human blood during febrile illness; and (3) identify and validate diagnostic and prognostic biomarkers during early stages of febrile illness based on microbial and viral sequences, host RNAs, and clinical features. Our long-term objectives are to validate novel early diagnostic and prognostic signatures for several classes and species of pathogens and their related clinical syndromes, with attention to early predictors of subsequent critical illness requiring intensive care. Sequence-based signatures will serve as the basis for the design of probes on CMOS electrochemical-based active microarrays and other technologies, so that they can be exploited and deployed at the point-of-care in an easy-to-use format.

Public Health Relevance

Early diagnosis of systemic infection in humans and prediction of clinical outcome both remain elusive, despite the critical need for both. We propose to employ state of the art techniques for characterizing microbial and viral DNA and RNA in human blood, as well as host molecules that are expressed early during the course of infection, in order to identify and then validate genetic signatures. These signatures will serve as the basis for tests that reveal the nature of the causative agent as well as the likely outcome of the disease early, when opportunities for beneficial intervention are greatest.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program--Cooperative Agreements (U19)
Project #
5U19AI109761-03
Application #
9010918
Study Section
Special Emphasis Panel (ZAI1-LR-M)
Project Start
Project End
Budget Start
2016-03-01
Budget End
2017-02-28
Support Year
3
Fiscal Year
2016
Total Cost
$850,040
Indirect Cost
$60,298

  Institution

Name
Columbia University (N.Y.)
Department
Type
DUNS #
621889815
City
New York
State
NY
Country
United States
Zip Code
10032

  Publications

Tokarz, Rafal; Mishra, Nischay; Tagliafierro, Teresa et al. (2018) A multiplex serologic platform for diagnosis of tick-borne diseases. Sci Rep 8:3158
Johnson, Bryan A; Graham, Rachel L; Menachery, Vineet D (2018) Viral metagenomics, protein structure, and reverse genetics: Key strategies for investigating coronaviruses. Virology 517:30-37
Gunn, Bronwyn M; Jones, Jennifer E; Shabman, Reed S et al. (2018) Ross River virus envelope glycans contribute to disease through activation of the host complement system. Virology 515:250-260
Mishra, Nischay; Caciula, Adrian; Price, Adam et al. (2018) Diagnosis of Zika Virus Infection by Peptide Array and Enzyme-Linked Immunosorbent Assay. MBio 9:
Cockrell, Adam S; Johnson, Joshua C; Moore, Ian N et al. (2018) A spike-modified Middle East respiratory syndrome coronavirus (MERS-CoV) infectious clone elicits mild respiratory disease in infected rhesus macaques. Sci Rep 8:10727
Lindesmith, Lisa C; Brewer-Jensen, Paul D; Mallory, Michael L et al. (2018) Antigenic Characterization of a Novel Recombinant GII.P16-GII.4 Sydney Norovirus Strain With Minor Sequence Variation Leading to Antibody Escape. J Infect Dis 217:1145-1152
Allicock, Orchid M; Guo, Cheng; Uhlemann, Anne-Catrin et al. (2018) BacCapSeq: a Platform for Diagnosis and Characterization of Bacterial Infections. MBio 9:
Williams, Simon H; Che, Xiaoyu; Garcia, Joel A et al. (2018) Viral Diversity of House Mice in New York City. MBio 9:
Gralinski, Lisa E; Sheahan, Timothy P; Morrison, Thomas E et al. (2018) Complement Activation Contributes to Severe Acute Respiratory Syndrome Coronavirus Pathogenesis. MBio 9:
Williams, Simon H; Cordey, Samuel; Bhuva, Nishit et al. (2018) Investigation of the Plasma Virome from Cases of Unexplained Febrile Illness in Tanzania from 2013 to 2014: a Comparative Analysis between Unbiased and VirCapSeq-VERT High-Throughput Sequencing Approaches. mSphere 3:

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