<i>Leishmania (L.) amazonensis</i> LaLRR17 increases parasite entry in macrophage by a mechanism dependent on GRP78

Peña, Mauricio S.; Tang, Fenny Hui Fen; Franco, Fernando Alves de Lima; Rodrigues, Agatha Sacramento; Carrara, Guilherme Moreira Paiva; Araujo, Thaís L.S.; Giordano, Ricardo J.; Palmisano, Giuseppe; Camargo, Maristela Martins de; Uliana, Sílvia Reni Bortolin; Stolf, Beatriz S.

doi:10.1017/s0031182023000720

Parasitology

2023

DOI: 10.1017/s0031182023000720

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Leishmania (L.) amazonensis LaLRR17 increases parasite entry in macrophage by a mechanism dependent on GRP78

Mauricio S. Peña

Fenny Hui Fen Tang

Fernando Alves de Lima Franco

et al.

Abstract: Leishmaniases affect 12 million people worldwide. They are caused by Leishmania spp., protozoan parasites transmitted to mammals by female phlebotomine flies. During the life cycle, promastigote forms of the parasite live in the gut of infected sandflies and convert into amastigotes inside the vertebrate macrophages. The parasite evades macrophage's microbicidal responses due to virulence factors that affect parasite phagocytosis, survival and/or proliferation. The interaction between Leishmania and macrophage… Show more

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2024

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FVB/NJ strain as a mouse model for cutaneous leishmaniasis by Leishmania (L.) amazonensis

Carrara,

Stolf

2024

Mem. Inst. Oswaldo Cruz

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BACKGROUND Leishmaniases encompass a spectrum of neglected diseases caused by parasites of the genus Leishmania, grouped in two forms: tegumentary and visceral leishmaniasis.OBJECTIVES In this study, we propose Friend Virus B NIH Jackson (FVB/NJ) mouse strain as a new experimental model of infection with Leishmania (Leishmania) amazonensis, the second most prevalent agent of tegumentary leishmaniasis in Brazil. METHODS AND FINDINGSWe performed in vitro infections of FVB/NJ macrophages and compared them with BALB/c macrophages, showing that BALB/c cells have higher infection percentages and a higher number of amastigotes/cell. Phagocytosis assays indicated that BALB/c and FVB/NJ macrophages have similar capacity to uptake parasites after 5 min incubations. We also investigated promastigotes' resistance to sera from FVB/NJ and BALB/c and observed no difference between the two sera, even though FVB/NJ has a deficiency in complement components. Finally, we subcutaneously infected FVB/NJ and BALB/c mice with 2 × 10 6 parasites expressing luciferase. Analysis of lesion development for 12 weeks showed that FVB/NJ and BALB/c mice have similar lesion profiles and parasite burdens.MAIN CONCLUSIONS This work characterises for the first time the FVB/NJ mouse as a new model for tegumentary leishmaniasis caused by Leishmania (L.) amazonensis.

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FVB/NJ strain as a mouse model for cutaneous leishmaniasis by Leishmania (L.) amazonensis

Carrara,

Stolf

2024

Mem. Inst. Oswaldo Cruz

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Leishmania (L.) amazonensis LaLRR17 increases parasite entry in macrophage by a mechanism dependent on GRP78

Cited by 1 publication

References 74 publications

FVB/NJ strain as a mouse model for cutaneous leishmaniasis by Leishmania (L.) amazonensis

FVB/NJ strain as a mouse model for cutaneous leishmaniasis by Leishmania (L.) amazonensis

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