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Transcriptional alterations of virulence factors in Leishmania major clinical isolates harboring Leishmania RNA virus 2 (LRV2)
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Transcriptional alterations of virulence factors in Leishmania major clinical isolates harboring Leishmania RNA virus 2 (LRV2)
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Journal Article
Transcriptional alterations of virulence factors in Leishmania major clinical isolates harboring Leishmania RNA virus 2 (LRV2)
2025
Overview
Background
Leishmaniasis is a parasitic disease caused by an intracellular protozoan,
Leishmania
. Various factors, including host immunity and the
Leishmania
species, influence the manifestation and severity of the disease. Recent investigations have shed light on the potentially significant role of
Leishmania
RNA virus (LRV) in the clinical prognosis of leishmaniasis. This study aims to investigate the influence of LRV2 + on various pathogenic genes of
Leishmania
.
Materials and methods
In this study, 35
Leishmania
isolates were obtained from patients diagnosed with cutaneous leishmaniasis (CL).
Leishmania
species and the presence of LRV2 + were identified with the PCR-RFLP and semi-nested PCR methods, respectively. Additionally, the RNA expression levels of cysteine protease (CP), heat shock protein 70 (HSP70), heat shock protein 83 (HSP83), glycoprotein 63 (GP63), and mannose phosphate isomerase (MPI) were assessed in LRV2 + and LRV2-
Leishmania
clinical isolates using RT-qPCR.
Results
Out of the 35 isolates, 20 were selected from CL patients, all confirmed as
Leishmania major
. These isolates were divided into two groups, LRV2 + and LRV2-, with 10 isolates in each group. RT-qPCR analysis revealed that HSP83, MPI, and GP63 gene expression levels were statistically upregulated in LRV2 + isolates compared to LRV2- isolates (
P
< 0.05). Although
HSP70
and
CP
genes showed slight up-regulation in LRV2 + isolates, it was not statistically significant compared to LRV2- isolates.
Conclusion
The notable increase in gene expression levels, particularly for
GP63
,
HSP83
, and
MPI
genes, suggests that the presence of LRV2 + may significantly influence the expression of these factors in
L. major
clinical isolates.
Clinical trial number
Not applicable.
Publisher
BioMed Central,BioMed Central Ltd,Springer Nature B.V,BMC
Subject
/ Control
/ Female
/ Genes
/ GP63
/ Heat-Shock Proteins - genetics
/ HSP70
/ HSP70 Heat-Shock Proteins - genetics
/ HSP83
/ Humans
/ Identification and classification
/ Leishmania major - isolation & purification
/ Leishmania major - pathogenicity
/ Leishmaniasis, Cutaneous - parasitology
/ Leishmaniavirus - isolation & purification
/ Mannose
/ Medicine
/ MPI
/ Proteins
/ Protozoa
/ Protozoan Proteins - genetics
/ Restriction fragment length polymorphism
/ RNA
