Overexpression of PEX14 results in mistargeting to mitochondria, accompanied by organelle fragmentation and clustering in human embryonic kidney cells

Renate L. M. Jansen, Rinse de Boer, Eline M. F. de Lange, Janet Koster, Rifka Vlijm, Hans R. Waterham, Ida J. van der Klei*

*Corresponding author voor dit werk

Onderzoeksoutput: ArticleAcademicpeer review

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Samenvatting

Peroxisome biogenesis disorders are caused by pathogenic variants in genes involved in biogenesis and maintenance of peroxisomes. However, mitochondria are also often affected in these diseases. Peroxisomal membrane proteins, including PEX14, have been found to mislocalise to mitochondria in cells lacking peroxisomes. Recent studies indicated that this mislocalisation contributes to mitochondrial abnormalities in PEX3-deficient patient fibroblasts cells. Here, we studied whether mitochondrial morphology is also affected in PEX3-deficient HEK293 cells and whether PEX14 mislocalises to mitochondria in these cells. Using high-resolution imaging techniques, we show that although endogenous PEX14 mislocalises to mitochondria, mitochondrial morphology was normal in PEX3-KO HEK293 cells. However, we discovered that overexpression of tagged PEX14 in wild-type HEK293 cells resulted in its mitochondrial localisation, accompanied by altered mitochondrial morphology. Our data indicate that overexpression of tagged PEX14 alone directly or indirectly cause mitochondrial abnormalities in cells containing peroxisomes.

Originele taal-2English
Artikelnummer119754
Aantal pagina's12
TijdschriftBiochimica et Biophysica Acta - Molecular Cell Research
Volume1871
Nummer van het tijdschrift6
Vroegere onlinedatum23-mei-2024
DOI's
StatusPublished - aug.-2024

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