Last Updated: 04/12/2025

Molecular mechanisms of bone-specific immunopathology during malaria

Objectives

*Original title and text were machine translated from Japanese

This project investigated possible negative impact of malaria infection on bone remodeling and growth.

Principal Institution

Osaka University (OU), Japan

Principal Investigators / Focal Persons

Cevayir Coban

Partner Investigators

Ken J. Ishii
Shizuo Akira

Rationale and Abstract

Malaria has deadly complications; however, the long term pathological consequences of chronic malaria infection are poorly understood. It is suspected that there is an association between growth retardation and malaria infection. Using mouse models mimicking chronic and self-clearing Plasmodium infection we showed that infection causes significant and long term bone loss in adult mice and growth retardation in young mice. Bone remodeling is completely suppressed during the acute phase of infection, but is highly activated immediately after the clearance of parasites, with increased osteoclastic activity skewing the balance toward bone resorption. Osteoclasts are activated by the key osteclastogenic cytokine RANKL, which was upregulated in osteoblasts through MyD88-dependent inflammation, triggered by the accumulation and long term persistence of parasite products in the bone marrow.

External reference

Project details

Themes

Basic Science

Date

Apr 2016 — Mar 2019

Total Project Funding

$158,891

Funding Details

Japan Society for the Promotion of Science (JSPS), Japan

Grant ID: 16H05181

JPY 17.55M