Leishmania infection modulates beta-1 integrin activation and alters the kinetics of monocyte spreading over fibronectin

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Cláudio Pereira Figueira
Djalma Gomes Ferrão Carvalhal
Rafaela Andrade Almeida
Micely d’ El-Rei Hermida
Dominique Touchard
Phillipe Robert
Anne Pierres
Pierre Bongrand
Washington LC dos-Santos
机构
[1] Fundação Oswaldo Cruz-Bahia,
[2] Centro de Pesquisas Gonçalo Moniz,undefined
[3] Brazilian Ministry of Health,undefined
[4] Universidade do Estado da Bahia,undefined
[5] Laboratoire Adhésion Cellulaire et Inflammation,undefined
[6] Parc Scientifique de Luminy,undefined
[7] Aix-Marseille Université,undefined
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Contact with Leishmania leads to a decreases in mononuclear phagocyte adherence to connective tissue. In this work, we studied the early stages of bond formation between VLA4 and fibronectin, measured the kinetics of membrane alignment and the monocyte cytoplasm spreading area over a fibronectin-coated surface and studied the expression of high affinity integrin epitope in uninfected and Leishmania-infected human monocytes. Our results show that the initial VLA4-mediated interaction of Leishmania-infected monocyte with a fibronectin-coated surface is preserved, however, the later stage, leukocyte spreading over the substrate is abrogated in Leishmania-infected cells. The median of spreading area was 72 [55–89] μm2 for uninfected and 41 [34–51] μm2 for Leishmania-infected monocyte. This cytoplasm spread was inhibited using an anti-VLA4 blocking antibody. After the initial contact with the fibronectrin-coated surface, uninfected monocyte quickly spread the cytoplasm at a 15 μm2 s−1 ratio whilst Leishmania-infected monocytes only made small contacts at a 5.5 μm2 s−1 ratio. The expression of high affinity epitope by VLA4 (from 39 ± 21% to 14 ± 3%); and LFA1 (from 37 ± 32% to 18 ± 16%) molecules was reduced in Leishmania-infected monocytes. These changes in phagocyte function may be important for parasite dissemination and distribution of lesions in leishmaniasis.
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