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J Transl Med. 2015 Nov 4;13:346. doi: 10.1186/s12967-015-0701-z.

Application of Nanotrap technology for high sensitivity measurement of urinary outer surface protein A carboxyl-terminus domain in early stage Lyme borreliosis.

Author information

1
George Mason University, Manassas, VA, USA. rmagni@gmu.edu.
2
University of Milan, Milan, Italy. rmagni@gmu.edu.
3
Ceres Nanosciences, Manassas, VA, USA. bespina@ceresnano.com.
4
Ceres Nanosciences, Manassas, VA, USA. kshah@ceresnano.com.
5
Ceres Nanosciences, Manassas, VA, USA. blepene@ceresnano.com.
6
George Mason University, Manassas, VA, USA. 2014cmayuga@gmail.com.
7
George Mason University, Manassas, VA, USA. tdouglas91@gmail.com.
8
George Mason University, Manassas, VA, USA. vespina@gmu.edu.
9
George Mason University, Manassas, VA, USA. srucker@gmu.edu.
10
Ceres Nanosciences, Manassas, VA, USA. rdunlap@ceresnano.com.
11
George Mason University, Manassas, VA, USA. epetrico@gmu.edu.
12
Frekko Primary Care, Gaithersburg, MD, USA. Frekkomi@aol.com.
13
Care ID, Annandale, VA, USA. donald2750@aol.com.
14
Novant Health, Manassas, VA, USA. irwinmed@aol.com.
15
Internal Medicine of Northern Virginia, Reston, VA, USA. samshor@yahoo.com.
16
George Mason University, Manassas, VA, USA. lliotta@gmu.edu.
17
George Mason University, Manassas, VA, USA. aluchini@gmu.edu.

Abstract

OBJECTIVES:

Prompt antibiotic treatment of early stage Lyme borreliosis (LB) prevents progression to severe multisystem disease. There is a clinical need to improve the diagnostic specificity of early stage Lyme assays in the period prior to the mounting of a robust serology response. Using a novel analyte harvesting nanotechnology, Nanotrap particles, we evaluated urinary Borrelia Outer surface protein A (OspA) C-terminus peptide in early stage LB before and after treatment, and in patients suspected of late stage disseminated LB.

METHOD:

We employed Nanotrap particles to concentrate urinary OspA and used a highly specific anti-OspA monoclonal antibody (mAb) as a detector of the C-terminus peptides. We mapped the mAb epitope to a narrow specific OspA C-terminal domain OspA236-239 conserved across infectious Borrelia species but with no homology to human proteins and no cross-reactivity with relevant viral and non-Borrelia bacterial proteins. 268 urine samples from patients being evaluated for all categories of LB were collected in a LB endemic area. The urinary OspA assay, blinded to outcome, utilized Nanotrap particle pre-processing, western blotting to evaluate the OspA molecular size, and OspA peptide competition for confirmation.

RESULTS:

OspA test characteristics: sensitivity 1.7 pg/mL (lowest limit of detection), % coefficient of variation (CV) = 8 %, dynamic range 1.7-30 pg/mL. Pre-treatment, 24/24 newly diagnosed patients with an erythema migrans (EM) rash were positive for urinary OspA while false positives for asymptomatic patients were 0/117 (Chi squared p < 10(-6)). For 10 patients who exhibited persistence of the EM rash during the course of antibiotic therapy, 10/10 were positive for urinary OspA. Urinary OspA of 8/8 patients switched from detectable to undetectable following symptom resolution post-treatment. Specificity of the urinary OspA test for the clinical symptoms was 40/40. Specificity of the urinary OspA antigen test for later serology outcome was 87.5 % (21 urinary OspA positive/24 serology positive, Chi squared p = 4.072e(-15)). 41 of 100 patients under surveillance for persistent LB in an endemic area were positive for urinary OspA protein.

CONCLUSIONS:

OspA urinary shedding was strongly linked to concurrent active symptoms (e.g. EM rash and arthritis), while resolution of these symptoms after therapy correlated with urinary conversion to OspA negative.

PMID:
26537892
PMCID:
PMC4634744
DOI:
10.1186/s12967-015-0701-z
[Indexed for MEDLINE]
Free PMC Article

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