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Traffic-related diesel pollution particles impair the lysosomal functions of human iPSC-derived microglia

Publiceringsår

2025

Upphovspersoner

Ohtonen, Sohvi; Jäntti, Henna; Giudice, Luca; Mohamed, Ahmed; Shakirzyanova, Anastasia; Závodná, Táňa; Belevich, Ilya; Yan, Hong; Sabogal-Guáqueta, Angélica María; Saveleva, Liudmila; Väänänen, Mari-Anna; Rillo-Albert, Ashley; Perciballi, Elisa; Ferrari, Daniela; Tervo, Minna-Mari; Gómez-Budia, Mireia; Krejčík, Zdeněk; Aakko-Saksa, Päivi; Koistinaho, Jari; Lehtonen, Šárka; Kanninen, Katja M.; Topinka, Jan; Jokitalo, Eija; Sierra, Alejandra; Schmidt, Martina; Dolga, Amalia M.; Jalava, Pasi I.; Korhonen, Paula; Malm, Tarja
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Abstrakt

<p>Exposure to air pollution is associated with neurological diseases. Traffic is a major source of air pollution, consisting of a complex mixture of ultrafine particles, that can invade the brain and induce a microglia-mediated inflammatory response. However, the exact mechanisms of how traffic-related particles impact human microglia remain poorly understood. This study investigates the effects of diesel exhaust particles (DEPs) on human induced pluripotent stem cell-derived microglia-like cells (iMGL). We exposed iMGLs to three different DEPs and studied the impact on the iMGL transcriptome and functionality, focusing on cytokine secretion, mitochondrial respiration, lysosomal function, and phagocytosis. A20 particles were collected from a heavy-duty engine run with petroleum diesel. For A0, the same engine was run with renewable diesel. E6 was produced with a modern 2019 model diesel passenger car run with renewable diesel. RNAseq revealed activation of the cytokine storm pathway and inhibition of the autophagy pathway in iMGLs after exposure to particles derived from older diesel emission technology (A20, A0). Particles from the modern diesel engine technology (E6) did not alter microglial transcriptome after 24 h exposure. A20 and A0 exposure led to impaired lysosomal functions in iMGLs. In contrast, E6 did not cause major alterations in microglia functions. In addition, we show that response to particles is more pronounced in human iMGLs compared to mouse primary microglia. To conclude, particles from older emission technology impair phago-lysosomal functions of iMGLs, but modern alternatives with filtration do not induce drastic changes in the functionality of iMGLs.</p>
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Organisationer och upphovspersoner

Helsingfors universitet

Jokitalo Eija

Belevich Ilya

Koistinaho Jari

Östra Finlands universitet

Jalava Pasi Ilari

Mohamed Ahmed Mohamed Ibrahim Mohamed

Sierra Lopez Alejandra

Shakirzyanova Anastasia Orcid -palvelun logo

Jäntti Henna Johanna

Kanninen Katja Marika

Saveleva Liudmila Orcid -palvelun logo

Giudice Luca Orcid -palvelun logo

Väänänen Mari-Anna

Tervo Minna-Mari

Gomez Budia Mireia

Korhonen Paula Karoliina

Lehtonen Sarka Orcid -palvelun logo

Ohtonen Sohvi Salome

Malm Tarja Maarit

Publikationstyp

Publikationsform

Artikel

Moderpublikationens typ

Tidning

Artikelstyp

En originalartikel

Målgrupp

Vetenskaplig

Kollegialt utvärderad

Kollegialt utvärderad

UKM:s publikationstyp

A1 Originalartikel i en vetenskaplig tidskrift

Publikationskanalens uppgifter

Moderpublikationens namn

Environment International

Volym

199

Artikelnummer

109467

Publikationsforum

55330

Publikationsforumsnivå

3

Öppen tillgång

Öppen tillgänglighet i förläggarens tjänst

Ja

Öppen tillgång till publikationskanalen

Delvis öppen publikationskanal

Licens för förläggarens version

CC BY

Parallellsparad

Nej

Övriga uppgifter

Vetenskapsområden

Miljövetenskap; Folkhälsovetenskap, miljö och arbetshälsa

Nyckelord

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Förlagets internationalitet

Internationell

Språk

engelska

Internationell sampublikation

Ja

Sampublikation med ett företag

Nej

DOI

10.1016/j.envint.2025.109467

Publikationen ingår i undervisnings- och kulturministeriets datainsamling

Ja