A real-time PCR assay for quantification of parasite burden in murine models of leishmaniasis

A real-time PCR assay for quantification of parasite burden in murine models of leishmaniasis

Eukaryotic parasites in the genus Leishmania place approximately 350 million people per year at risk of disease. In addition to their global health significance, Leishmania spp. have served as an important model for delineating basic concepts in immunology such as T-helper cell polarization. There h...

Full description

Bibliographic Details
Main Authors: Alejandro L. Antonia, Liuyang Wang, Dennis C. Ko
Format: Article
Language:English
Published: PeerJ Inc. 2018-11-01
Series:PeerJ
Subjects:
Quantitative real-time PCR
Leishmania
Leishmaniasis
DRBD3
Mouse
Parasite burden
Online Access:https://peerj.com/articles/5905.pdf
id doaj-12f51684ffd54af6bf5a297a535ceb65
record_format Article
spelling doaj-12f51684ffd54af6bf5a297a535ceb652020-11-25T02:17:15ZengPeerJ Inc.PeerJ2167-83592018-11-016e590510.7717/peerj.5905A real-time PCR assay for quantification of parasite burden in murine models of leishmaniasisAlejandro L. Antonia0Liuyang Wang1Dennis C. Ko2Department of Molecular Genetics and Microbiology, Duke University, Durham, NC, USADepartment of Molecular Genetics and Microbiology, Duke University, Durham, NC, USADepartment of Molecular Genetics and Microbiology, Duke University, Durham, NC, USAEukaryotic parasites in the genus Leishmania place approximately 350 million people per year at risk of disease. In addition to their global health significance, Leishmania spp. have served as an important model for delineating basic concepts in immunology such as T-helper cell polarization. There have been many qPCR-based assays reported for measuring parasite burden in humans and animals. However, these are largely optimized for use in clinical diagnosis and not specifically for animal models. This has led several of these assays to have suboptimal characteristics for use in animal models. For example, multi-copy number genes have been frequently used to increase sensitivity but are subject to greater plasticity within the genome and thus may confound effects of experimental manipulations in animal models. In this study, we developed a sybr-green based quantitative touchdown PCR assay for a highly conserved and single-copy putative RNA-binding protein, DRBD3. With primers that share greater than 90% sequence identity across all sequenced Leishmania spp., we demonstrate that this assay has a lower limit of detection of 100 fg of parasite DNA for Leishmania major, L. donovani, L. venezuelensis, and L. panamensis. Using C57BL6/J mice, we used this assay to monitor parasite burden over 1 month of infection with two strains of L. major (Seidman and Friedlin), and L. venezeuelensis. These characteristics rival the sensitivity of previously reported qPCR based methods of parasite quantitation while amplifying a stable, single copy gene. Use of this protocol in the future will lead to improved accuracy in animal based models and help to tease apart differences in biology of host-parasite interactions.https://peerj.com/articles/5905.pdfQuantitative real-time PCRLeishmaniaLeishmaniasisDRBD3MouseParasite burden
collection DOAJ
language English
format Article
sources DOAJ
author Alejandro L. Antonia
Liuyang Wang
Dennis C. Ko
spellingShingle Alejandro L. Antonia
Liuyang Wang
Dennis C. Ko
A real-time PCR assay for quantification of parasite burden in murine models of leishmaniasis
PeerJ
Quantitative real-time PCR
Leishmania
Leishmaniasis
DRBD3
Mouse
Parasite burden
author_facet Alejandro L. Antonia
Liuyang Wang
Dennis C. Ko
author_sort Alejandro L. Antonia
title A real-time PCR assay for quantification of parasite burden in murine models of leishmaniasis
title_short A real-time PCR assay for quantification of parasite burden in murine models of leishmaniasis
title_full A real-time PCR assay for quantification of parasite burden in murine models of leishmaniasis
title_fullStr A real-time PCR assay for quantification of parasite burden in murine models of leishmaniasis
title_full_unstemmed A real-time PCR assay for quantification of parasite burden in murine models of leishmaniasis
title_sort real-time pcr assay for quantification of parasite burden in murine models of leishmaniasis
publisher PeerJ Inc.
series PeerJ
issn 2167-8359
publishDate 2018-11-01
description Eukaryotic parasites in the genus Leishmania place approximately 350 million people per year at risk of disease. In addition to their global health significance, Leishmania spp. have served as an important model for delineating basic concepts in immunology such as T-helper cell polarization. There have been many qPCR-based assays reported for measuring parasite burden in humans and animals. However, these are largely optimized for use in clinical diagnosis and not specifically for animal models. This has led several of these assays to have suboptimal characteristics for use in animal models. For example, multi-copy number genes have been frequently used to increase sensitivity but are subject to greater plasticity within the genome and thus may confound effects of experimental manipulations in animal models. In this study, we developed a sybr-green based quantitative touchdown PCR assay for a highly conserved and single-copy putative RNA-binding protein, DRBD3. With primers that share greater than 90% sequence identity across all sequenced Leishmania spp., we demonstrate that this assay has a lower limit of detection of 100 fg of parasite DNA for Leishmania major, L. donovani, L. venezuelensis, and L. panamensis. Using C57BL6/J mice, we used this assay to monitor parasite burden over 1 month of infection with two strains of L. major (Seidman and Friedlin), and L. venezeuelensis. These characteristics rival the sensitivity of previously reported qPCR based methods of parasite quantitation while amplifying a stable, single copy gene. Use of this protocol in the future will lead to improved accuracy in animal based models and help to tease apart differences in biology of host-parasite interactions.
topic Quantitative real-time PCR
Leishmania
Leishmaniasis
DRBD3
Mouse
Parasite burden
url https://peerj.com/articles/5905.pdf
work_keys_str_mv AT alejandrolantonia arealtimepcrassayforquantificationofparasiteburdeninmurinemodelsofleishmaniasis
AT liuyangwang arealtimepcrassayforquantificationofparasiteburdeninmurinemodelsofleishmaniasis
AT denniscko arealtimepcrassayforquantificationofparasiteburdeninmurinemodelsofleishmaniasis
AT alejandrolantonia realtimepcrassayforquantificationofparasiteburdeninmurinemodelsofleishmaniasis
AT liuyangwang realtimepcrassayforquantificationofparasiteburdeninmurinemodelsofleishmaniasis
AT denniscko realtimepcrassayforquantificationofparasiteburdeninmurinemodelsofleishmaniasis
_version_ 1724887432750432256

Similar Items