Circadian Regulation of Leishmania Parasite Internalisation in Macrophages and Downstream Cellular Events

Author:

Carvalho Cabral Priscilla1,Stegeman Sophia K.1,Olivier Martin2,Cermakian Nicolas1ORCID

Affiliation:

1. Douglas Research Centre McGill University Montreal Quebec Canada

2. Research Institute of the McGill University Health Centre McGill University Montreal Quebec Canada

Abstract

ABSTRACTLeishmania spp. parasites use macrophages as a host cell during infection. As a result, macrophages have a dual role: clearing the parasite as well as acting as host cells. Recently, studies have shown that macrophages harbour circadian clocks, which affect many of their functions such as phagocytosis, receptor expression and cytokine release. Interestingly, Leishmania major infection in hosts was also shown to be under circadian control. Therefore, we decided to investigate what underlies the rhythms of L. major infection within macrophages. Using a culture model of infection of bone marrow–derived macrophages with L. major promastigotes, we show that the parasites are internalised into macrophages with a 24‐h variation dependent on a functional circadian clock in the cells. This was associated with a variation in the number of parasites per macrophage. The cell surface expression of parasite receptors was not controlled by the cells' circadian clock. In contrast, the expression of the components of the endocytic pathway, EEA1 and LC3b, varied according to the time of infection. This was paralleled by variations in parasite‐induced ROS production as well as cytokine tumour necrosis factor α. In summary, we have uncovered a time‐dependent regulation of the internalisation of L. major promastigotes in macrophages, controlled by the circadian clock in these cells, as well as subsequent cellular events in the endocytic pathway, intracellular signalling and cytokine production.

Funder

Faculty of Medicine, McGill University

Canadian Institutes of Health Research

Fonds de Recherche du Québec - Santé

Publisher

Wiley

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