Serodiagnosis and Therapeutic Monitoring of New-World Tegumentary Leishmaniasis Using Synthetic Type-2 Glycoinositolphospholipid-based Neoglycoproteins

Overview

Journal Emerg Microbes Infect

Specialty Infectious Diseases

Date 2022 Aug 30

PMID 36039908

Authors

Sayonara M Viana

Alba L Montoya

Augusto M Carvalho

Brunele S de Mendonca

Susana Portillo

Janet J Olivas

Nasim H Karimi

Igor L Estevao

Uriel Ortega-Rodriguez

Edgar M Carvalho

Walderez O Dutra

Rosa A Maldonaldo

Katja Michael

Camila I de Oliveira

Igor C Almeida

Affiliations

Soon will be listed here.

Abstract

American tegumentary leishmaniasis (TL) caused by is characterized by a spectrum of clinical presentations, ranging from localized cutaneous ulcers (CL), mucosal (ML), or disseminated (DL) disease, to a subclinical (SC) asymptomatic form. Current diagnosis based on parasite culture and/or microscopy lacks sensitivity and specificity. Previous studies showed that patients with CL and ML have very high levels of -specific anti-α-Gal antibodies. However, the native parasite α-Gal glycotope(s) is(are) still elusive, thus they have not yet been explored for a more accurate TL diagnosis. Using a chemiluminescent immunoassay, we evaluated the seroreactivity of TL patients across its clinical spectrum, and of endemic (EC) and nonendemic healthy controls (NEC) against three synthetic neoglycoproteins (NGP29b, NGP30b, and NGP28b), respectively comprising the derived type-2 glycoinositolphospholipid (GIPL)-1 (Galβ1,3Manα), GIPL-2 (Galα1,3Galβ1,3Manα), and GIPL-3 (Galα1,6Galα1,3Galβ) glycotopes. Contrary to NGP29b and NGP30b, NGP28b exhibited high sensitivity and specificity to a CL serum pool. More importantly, NGP28b reacted strongly and specifically with individual sera from distinct clinical forms of TL, especially with SC sera, with 94% sensitivity and 97% specificity, by post-two-graph receiver-operating characteristic curve analysis. Contrary to NGP29b, NGP28b showed low cross-reactivity with Chagas disease and control (NEC/EC) sera. Additionally, seroreactivity of CL patients against NGP28b was significantly decreased after successful chemotherapy, indicating that -specific anti-α-Gal antibodies may serve as an early biomarker of cure in CL. Our data also points towards the applicability of type-2 GIPL-3-derived Galα1,6Galα1,3Galβ glycotope for the serological diagnosis of American TL, particularly of the subclinical form.

Citing Articles

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