HIF-2α drives hepatic Kupffer cell death and proinflammatory recruited macrophage activation in nonalcoholic steatohepatitis

Ishtiaq Jeelani; Jae Su Moon; Flavia Franco da Cunha; Chanond A. Nasamran; Seokhyun Jeon; Xinhang Zhang; Gautam K. Bandyopadhyay; Katarzyna Dobaczewska; Zbigniew Mikulski; Mojgan Hosseini; Xiao Liu; Tatiana Kisseleva; David A. Brenner; Seema Singh; Rohit Loomba; Minkyu Kim; Yun Sok Lee

doi:10.1126/scitranslmed.adi0284

HIF-2α drives hepatic Kupffer cell death and proinflammatory recruited macrophage activation in nonalcoholic steatohepatitis

Ishtiaq Jeelani
, Jae Su Moon
, Flavia Franco da Cunha
, Chanond A. Nasamran
, Seokhyun Jeon
, Xinhang Zhang
, Gautam K. Bandyopadhyay
, Katarzyna Dobaczewska
, Zbigniew Mikulski
, Mojgan Hosseini
, Xiao Liu
, Tatiana Kisseleva
, David A. Brenner
, Seema Singh
, Rohit Loomba
, Minkyu Kim
, Yun Sok Lee

Department of Biochemistry & Structural Biology

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

34 Scopus citations

Abstract

Proinflammatory hepatic macrophage activation plays a key role in the development of nonalcoholic steatohepatitis (NASH). This involves increased embryonic hepatic Kupffer cell (KC) death, facilitating the replacement of KCs with bone marrow–derived recruited hepatic macrophages (RHMs) that highly express proinflammatory genes. Moreover, phago/efferocytic activity of KCs is diminished in NASH, enhancing liver inflammation. However, the molecular mechanisms underlying these changes in KCs are not known. Here, we show that hypoxia-inducible factor 2α (HIF-2α) mediates NASH-associated decreased KC growth and efferocytosis by enhancing lysosomal stress. At the molecular level, HIF-2α stimulated mammalian target of rapamycin (mTOR)– and extracellular signal–regulated kinase-dependent inhibitory transcription factor EB (TFEB) phosphorylation, leading to decreased lysosomal and phagocytic gene expression. With increased metabolic stress and phago/efferocytic burden in NASH, these changes were sufficient to increase lysosomal stress, causing decreased efferocytosis and lysosomal cell death. Of interest, HIF-2α–dependent TFEB regulation only occurred in KCs but not RHMs. Instead, in RHMs, HIF-2α promoted mitochondrial reactive oxygen species production and proinflammatory activation by increasing ANT2 expression and mitochondrial permeability transition. Consequently, myeloid lineage–specific or KC-specific HIF-2α depletion or the inhibition of mTOR-dependent TFEB inhibition using antisense oligonucleotide treatment protected against the development of NASH in mice. Moreover, treatment with an HIF-2α–specific inhibitor reduced inflammatory and fibrogenic gene expression in human liver spheroids cultured under a NASH-like condition. Together, our results suggest that macrophage subtype–specific effects of HIF-2α collectively contribute to the proinflammatory activation of liver macrophages, leading to the development of NASH.

Original language	English (US)
Article number	eadi0284
Journal	Science translational medicine
Volume	16
Issue number	764
DOIs	https://doi.org/10.1126/scitranslmed.adi0284
State	Published - Sep 11 2024

ASJC Scopus subject areas

General Medicine

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10.1126/scitranslmed.adi0284

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Jeelani, I., Moon, J. S., da Cunha, F. F., Nasamran, C. A., Jeon, S., Zhang, X., Bandyopadhyay, G. K., Dobaczewska, K., Mikulski, Z., Hosseini, M., Liu, X., Kisseleva, T., Brenner, D. A., Singh, S., Loomba, R., Kim, M., & Lee, Y. S. (2024). HIF-2α drives hepatic Kupffer cell death and proinflammatory recruited macrophage activation in nonalcoholic steatohepatitis. Science translational medicine, 16(764), Article eadi0284. https://doi.org/10.1126/scitranslmed.adi0284

Jeelani, I, Moon, JS, da Cunha, FF, Nasamran, CA, Jeon, S, Zhang, X, Bandyopadhyay, GK, Dobaczewska, K, Mikulski, Z, Hosseini, M, Liu, X, Kisseleva, T, Brenner, DA, Singh, S, Loomba, R, Kim, M & Lee, YS 2024, 'HIF-2α drives hepatic Kupffer cell death and proinflammatory recruited macrophage activation in nonalcoholic steatohepatitis', Science translational medicine, vol. 16, no. 764, eadi0284. https://doi.org/10.1126/scitranslmed.adi0284

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title = "HIF-2α drives hepatic Kupffer cell death and proinflammatory recruited macrophage activation in nonalcoholic steatohepatitis",

abstract = "Proinflammatory hepatic macrophage activation plays a key role in the development of nonalcoholic steatohepatitis (NASH). This involves increased embryonic hepatic Kupffer cell (KC) death, facilitating the replacement of KCs with bone marrow–derived recruited hepatic macrophages (RHMs) that highly express proinflammatory genes. Moreover, phago/efferocytic activity of KCs is diminished in NASH, enhancing liver inflammation. However, the molecular mechanisms underlying these changes in KCs are not known. Here, we show that hypoxia-inducible factor 2α (HIF-2α) mediates NASH-associated decreased KC growth and efferocytosis by enhancing lysosomal stress. At the molecular level, HIF-2α stimulated mammalian target of rapamycin (mTOR)– and extracellular signal–regulated kinase-dependent inhibitory transcription factor EB (TFEB) phosphorylation, leading to decreased lysosomal and phagocytic gene expression. With increased metabolic stress and phago/efferocytic burden in NASH, these changes were sufficient to increase lysosomal stress, causing decreased efferocytosis and lysosomal cell death. Of interest, HIF-2α–dependent TFEB regulation only occurred in KCs but not RHMs. Instead, in RHMs, HIF-2α promoted mitochondrial reactive oxygen species production and proinflammatory activation by increasing ANT2 expression and mitochondrial permeability transition. Consequently, myeloid lineage–specific or KC-specific HIF-2α depletion or the inhibition of mTOR-dependent TFEB inhibition using antisense oligonucleotide treatment protected against the development of NASH in mice. Moreover, treatment with an HIF-2α–specific inhibitor reduced inflammatory and fibrogenic gene expression in human liver spheroids cultured under a NASH-like condition. Together, our results suggest that macrophage subtype–specific effects of HIF-2α collectively contribute to the proinflammatory activation of liver macrophages, leading to the development of NASH.",

author = "Ishtiaq Jeelani and Moon, \{Jae Su\} and \{da Cunha\}, \{Flavia Franco\} and Nasamran, \{Chanond A.\} and Seokhyun Jeon and Xinhang Zhang and Bandyopadhyay, \{Gautam K.\} and Katarzyna Dobaczewska and Zbigniew Mikulski and Mojgan Hosseini and Xiao Liu and Tatiana Kisseleva and Brenner, \{David A.\} and Seema Singh and Rohit Loomba and Minkyu Kim and Lee, \{Yun Sok\}",

year = "2024",

month = sep,

day = "11",

doi = "10.1126/scitranslmed.adi0284",

language = "English (US)",

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T1 - HIF-2α drives hepatic Kupffer cell death and proinflammatory recruited macrophage activation in nonalcoholic steatohepatitis

AU - Jeelani, Ishtiaq

AU - Moon, Jae Su

AU - da Cunha, Flavia Franco

AU - Nasamran, Chanond A.

AU - Jeon, Seokhyun

AU - Zhang, Xinhang

AU - Bandyopadhyay, Gautam K.

AU - Dobaczewska, Katarzyna

AU - Mikulski, Zbigniew

AU - Hosseini, Mojgan

AU - Liu, Xiao

AU - Kisseleva, Tatiana

AU - Brenner, David A.

AU - Singh, Seema

AU - Loomba, Rohit

AU - Kim, Minkyu

AU - Lee, Yun Sok

PY - 2024/9/11

Y1 - 2024/9/11

N2 - Proinflammatory hepatic macrophage activation plays a key role in the development of nonalcoholic steatohepatitis (NASH). This involves increased embryonic hepatic Kupffer cell (KC) death, facilitating the replacement of KCs with bone marrow–derived recruited hepatic macrophages (RHMs) that highly express proinflammatory genes. Moreover, phago/efferocytic activity of KCs is diminished in NASH, enhancing liver inflammation. However, the molecular mechanisms underlying these changes in KCs are not known. Here, we show that hypoxia-inducible factor 2α (HIF-2α) mediates NASH-associated decreased KC growth and efferocytosis by enhancing lysosomal stress. At the molecular level, HIF-2α stimulated mammalian target of rapamycin (mTOR)– and extracellular signal–regulated kinase-dependent inhibitory transcription factor EB (TFEB) phosphorylation, leading to decreased lysosomal and phagocytic gene expression. With increased metabolic stress and phago/efferocytic burden in NASH, these changes were sufficient to increase lysosomal stress, causing decreased efferocytosis and lysosomal cell death. Of interest, HIF-2α–dependent TFEB regulation only occurred in KCs but not RHMs. Instead, in RHMs, HIF-2α promoted mitochondrial reactive oxygen species production and proinflammatory activation by increasing ANT2 expression and mitochondrial permeability transition. Consequently, myeloid lineage–specific or KC-specific HIF-2α depletion or the inhibition of mTOR-dependent TFEB inhibition using antisense oligonucleotide treatment protected against the development of NASH in mice. Moreover, treatment with an HIF-2α–specific inhibitor reduced inflammatory and fibrogenic gene expression in human liver spheroids cultured under a NASH-like condition. Together, our results suggest that macrophage subtype–specific effects of HIF-2α collectively contribute to the proinflammatory activation of liver macrophages, leading to the development of NASH.

AB - Proinflammatory hepatic macrophage activation plays a key role in the development of nonalcoholic steatohepatitis (NASH). This involves increased embryonic hepatic Kupffer cell (KC) death, facilitating the replacement of KCs with bone marrow–derived recruited hepatic macrophages (RHMs) that highly express proinflammatory genes. Moreover, phago/efferocytic activity of KCs is diminished in NASH, enhancing liver inflammation. However, the molecular mechanisms underlying these changes in KCs are not known. Here, we show that hypoxia-inducible factor 2α (HIF-2α) mediates NASH-associated decreased KC growth and efferocytosis by enhancing lysosomal stress. At the molecular level, HIF-2α stimulated mammalian target of rapamycin (mTOR)– and extracellular signal–regulated kinase-dependent inhibitory transcription factor EB (TFEB) phosphorylation, leading to decreased lysosomal and phagocytic gene expression. With increased metabolic stress and phago/efferocytic burden in NASH, these changes were sufficient to increase lysosomal stress, causing decreased efferocytosis and lysosomal cell death. Of interest, HIF-2α–dependent TFEB regulation only occurred in KCs but not RHMs. Instead, in RHMs, HIF-2α promoted mitochondrial reactive oxygen species production and proinflammatory activation by increasing ANT2 expression and mitochondrial permeability transition. Consequently, myeloid lineage–specific or KC-specific HIF-2α depletion or the inhibition of mTOR-dependent TFEB inhibition using antisense oligonucleotide treatment protected against the development of NASH in mice. Moreover, treatment with an HIF-2α–specific inhibitor reduced inflammatory and fibrogenic gene expression in human liver spheroids cultured under a NASH-like condition. Together, our results suggest that macrophage subtype–specific effects of HIF-2α collectively contribute to the proinflammatory activation of liver macrophages, leading to the development of NASH.

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UR - https://www.scopus.com/pages/publications/85204087274#tab=citedBy

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JO - Science translational medicine

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ER -

HIF-2α drives hepatic Kupffer cell death and proinflammatory recruited macrophage activation in nonalcoholic steatohepatitis

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