Loss of HSPA9 induces peroxisomal degradation by increasing pexophagy

Doo Sin Jo; So Jung Park; Ae Kyeong Kim; Na Yeon Park; Joon Bum Kim; Ji Eun Bae; Hyun Jun Park; Ji Hyun Shin; Jong Wook Chang; Peter K. Kim; Yong Keun Jung; Jae Young Koh; Seong Kyu Choe; Kyu Sun Lee; Dong Hyung Cho

doi:10.1080/15548627.2020.1712812

Loss of HSPA9 induces peroxisomal degradation by increasing pexophagy

Doo Sin Jo, So Jung Park, Ae Kyeong Kim, Na Yeon Park, Joon Bum Kim, Ji Eun Bae, Hyun Jun Park, Ji Hyun Shin, Jong Wook Chang, Peter K. Kim, Yong Keun Jung, Jae Young Koh, Seong Kyu Choe, Kyu Sun Lee, Dong Hyung Cho

Research output: Contribution to journal › Article › peer-review

43 Scopus citations

Abstract

Quality control of peroxisomes is essential for cellular homeostasis. However, the mechanism underlying pexophagy is largely unknown. In this study, we identified HSPA9 as a novel pexophagy regulator. Downregulation of HSPA9 increased macroautophagy/autophagy but decreased the number of peroxisomes in vitro and in vivo. The loss of peroxisomes by HSPA9 depletion was attenuated in SQSTM1-deficient cells. In HSPA9-deficient cells, the level of peroxisomal reactive oxygen species (ROS) increased, while inhibition of ROS blocked pexophagy in HeLa and SH-SY5Y cells. Importantly, reconstitution of HSPA9 mutants found in Parkinson disease failed to rescue the loss of peroxisomes, whereas reconstitution with wild type inhibited pexophagy in HSPA9-depleted cells. Knockdown of Hsc70-5 decreased peroxisomes in Drosophila, and the HSPA9 mutants failed to rescue the loss of peroxisomes in Hsc70-5-depleted flies. Taken together, our findings suggest that the loss of HSPA9 enhances peroxisomal degradation by pexophagy.

Original language	English
Pages (from-to)	1989-2003
Number of pages	15
Journal	Autophagy
Volume	16
Issue number	11
DOIs	https://doi.org/10.1080/15548627.2020.1712812
State	Published - 1 Nov 2020

Keywords

Drosophila
HSPA9
Parkinson disease
peroxisome
pexophagy
ROS

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title = "Loss of HSPA9 induces peroxisomal degradation by increasing pexophagy",

abstract = "Quality control of peroxisomes is essential for cellular homeostasis. However, the mechanism underlying pexophagy is largely unknown. In this study, we identified HSPA9 as a novel pexophagy regulator. Downregulation of HSPA9 increased macroautophagy/autophagy but decreased the number of peroxisomes in vitro and in vivo. The loss of peroxisomes by HSPA9 depletion was attenuated in SQSTM1-deficient cells. In HSPA9-deficient cells, the level of peroxisomal reactive oxygen species (ROS) increased, while inhibition of ROS blocked pexophagy in HeLa and SH-SY5Y cells. Importantly, reconstitution of HSPA9 mutants found in Parkinson disease failed to rescue the loss of peroxisomes, whereas reconstitution with wild type inhibited pexophagy in HSPA9-depleted cells. Knockdown of Hsc70-5 decreased peroxisomes in Drosophila, and the HSPA9 mutants failed to rescue the loss of peroxisomes in Hsc70-5-depleted flies. Taken together, our findings suggest that the loss of HSPA9 enhances peroxisomal degradation by pexophagy.",

keywords = "Drosophila, HSPA9, Parkinson disease, peroxisome, pexophagy, ROS",

author = "Jo, {Doo Sin} and Park, {So Jung} and Kim, {Ae Kyeong} and Park, {Na Yeon} and Kim, {Joon Bum} and Bae, {Ji Eun} and Park, {Hyun Jun} and Shin, {Ji Hyun} and Chang, {Jong Wook} and Kim, {Peter K.} and Jung, {Yong Keun} and Koh, {Jae Young} and Choe, {Seong Kyu} and Lee, {Kyu Sun} and Cho, {Dong Hyung}",

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AU - Bae, Ji Eun

AU - Park, Hyun Jun

AU - Shin, Ji Hyun

AU - Chang, Jong Wook

AU - Kim, Peter K.

AU - Jung, Yong Keun

AU - Koh, Jae Young

AU - Choe, Seong Kyu

AU - Lee, Kyu Sun

AU - Cho, Dong Hyung

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N2 - Quality control of peroxisomes is essential for cellular homeostasis. However, the mechanism underlying pexophagy is largely unknown. In this study, we identified HSPA9 as a novel pexophagy regulator. Downregulation of HSPA9 increased macroautophagy/autophagy but decreased the number of peroxisomes in vitro and in vivo. The loss of peroxisomes by HSPA9 depletion was attenuated in SQSTM1-deficient cells. In HSPA9-deficient cells, the level of peroxisomal reactive oxygen species (ROS) increased, while inhibition of ROS blocked pexophagy in HeLa and SH-SY5Y cells. Importantly, reconstitution of HSPA9 mutants found in Parkinson disease failed to rescue the loss of peroxisomes, whereas reconstitution with wild type inhibited pexophagy in HSPA9-depleted cells. Knockdown of Hsc70-5 decreased peroxisomes in Drosophila, and the HSPA9 mutants failed to rescue the loss of peroxisomes in Hsc70-5-depleted flies. Taken together, our findings suggest that the loss of HSPA9 enhances peroxisomal degradation by pexophagy.

AB - Quality control of peroxisomes is essential for cellular homeostasis. However, the mechanism underlying pexophagy is largely unknown. In this study, we identified HSPA9 as a novel pexophagy regulator. Downregulation of HSPA9 increased macroautophagy/autophagy but decreased the number of peroxisomes in vitro and in vivo. The loss of peroxisomes by HSPA9 depletion was attenuated in SQSTM1-deficient cells. In HSPA9-deficient cells, the level of peroxisomal reactive oxygen species (ROS) increased, while inhibition of ROS blocked pexophagy in HeLa and SH-SY5Y cells. Importantly, reconstitution of HSPA9 mutants found in Parkinson disease failed to rescue the loss of peroxisomes, whereas reconstitution with wild type inhibited pexophagy in HSPA9-depleted cells. Knockdown of Hsc70-5 decreased peroxisomes in Drosophila, and the HSPA9 mutants failed to rescue the loss of peroxisomes in Hsc70-5-depleted flies. Taken together, our findings suggest that the loss of HSPA9 enhances peroxisomal degradation by pexophagy.

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Loss of HSPA9 induces peroxisomal degradation by increasing pexophagy

Abstract

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