Coadminstration of L. major amastigote class I nuclease (rLmaCIN) with LPD nanoparticles delays the progression of skin lesion and the L. major dissemination to the spleen in BALB/c mice-based experimental setting

Fatemeh Fakhraee; Ali Badiee; Seyedeh Hoda Alavizadeh; Seyed Amir Jalali; Omid Chavoshian; Ali Khamesipour; Fereidoun Mahboudi; Mahmoud Reza Jaafari

doi:10.1016/j.actatropica.2016.04.004

Coadminstration of L. major amastigote class I nuclease (rLmaCIN) with LPD nanoparticles delays the progression of skin lesion and the L. major dissemination to the spleen in BALB/c mice-based experimental setting

Acta Trop. 2016 Jul:159:211-8. doi: 10.1016/j.actatropica.2016.04.004. Epub 2016 Apr 6.

Authors

Fatemeh Fakhraee¹, Ali Badiee², Seyedeh Hoda Alavizadeh¹, Seyed Amir Jalali³, Omid Chavoshian¹, Ali Khamesipour⁴, Fereidoun Mahboudi⁵, Mahmoud Reza Jaafari⁶

Affiliations

¹ Nanotechnology Research Center, School of Pharmacy, Mashhad University of Medical Sciences, Mashhad, Iran.
² Nanotechnology Research Center, School of Pharmacy, Mashhad University of Medical Sciences, Mashhad, Iran. Electronic address: Badieea@mums.ac.ir.
³ Department of Immunology, Medical School, Shahid Beheshti University of Medical Sciences, Tehran, Iran.
⁴ Center for Research and Training in Skin Diseases and Leprosy, Tehran University of Medical Sciences, Tehran, Iran.
⁵ Biotechnology Department, Pasteur Institute of Iran, Tehran, Iran. Electronic address: Mahboudi@institute.pasteur.ac.ir.
⁶ Biotechnology Research Center, Nanotechnology Research Center, School of Pharmacy, Mashhad University of Medical Sciences, Mashhad, Iran. Electronic address: Jafarimr@mums.ac.ir.

PMID: 27060774
DOI: 10.1016/j.actatropica.2016.04.004

Abstract

Human cutaneous leishmaniasis is a disease caused by eukaryotic single-celled Leishmania species, the developmental program of which relies upon blood-feeding adult female sand flies and their dominant mammal blood sources, namely wild rodents in area where human beings exert more or less transient activities. The recourse to model rodents - namely laboratory mice such as C57BL/6 mice - has allowed extracted the immune signatures that account for the healing of the transient cutaneous lesion that develops at the site where Leishmania major promastigotes were delivered. Indeed, if the latter mice are exposed to a second inoculum of L. major promastigotes, no lesion will develop in the secondary skin site remodeled as a niche for a low size intracellular L. major amastigote population. Moreover, IFN-γ dominates over IL-10 in the supernatant of cultures of PBMCs -prepared from blood sampled from human beings who healed from a cutaneous lesion- and incubated with L. major class I Nuclease LmaCIN, a protein highly expressed in the cell-cycling amastigote population which is dominant by macrophages. Altogether, these datasets were strong incentive to promote research aimed to design and monitor efficacy of L. major amastigote protein-based vaccines in pre-clinical settings. Using L. major enzyme class I nuclease (LmaCIN) expressed in the L. major cell-cycling amastigote population hosted by macrophages, BALB/c mice were immunized three times with either rLmaCIN plus LPD nanoparticles (LPD-rLmaCIN), or rLmaCIN-CpG DNA or free rLmaCIN and dextrose. The following parameters: footpad swelling, splenic L. major load, L. major binding IgGs and cytokine profiles of rLmaCIN- reactive T lymphocytes were then compared. Once coadminstered with LPD, rLmaCIN allow BALB/c mice to display delayed onset of skin lesion at the challenge inoculation site and delayed L. major dissemination from the challenged site to the spleen. Thus, the LPD-rLmaCIN is shown to display some promising features out of three formulations inoculated to the BALB/c mouse immunization.

Keywords: CpG DNA; Experimental leishmaniasis; LPD nanoparticles; Vaccine; rLmaCIN.

MeSH terms

Animals
Female
Humans
Immunization
Interleukin-10 / therapeutic use*
Leishmania major / immunology*
Leishmaniasis, Cutaneous / drug therapy*
Leishmaniasis, Cutaneous / immunology*
Liposomes / therapeutic use*
Membrane Proteins / therapeutic use*
Mice
Mice, Inbred BALB C
Mice, Inbred C57BL
Nanoparticles / therapeutic use
Neuraminidase / therapeutic use*
Psychodidae / immunology
Spleen / immunology*

Substances

IL10 protein, human
Liposomes
Membrane Proteins
Interleukin-10
amastigote surface protein-1
Neuraminidase