Chop Deficiency Protects Mice Against Bleomycin-induced Pulmonary Fibrosis by Attenuating M2 Macrophage Production

Yao, Yingying; Wang, Yi; Zhang, Zhijun; He, Liangmei; Zhu, Jianghui; Zhang, Meng; He, Xiaoyu; Cheng, Zhenshun; Ao, Qilin; Cao, Yong; Yang, Ping; Su, Yunchao; Zhao, Jianping; Zhang, Shu; Yu, Qilin; Ning, Qin; Xiang, Xudong; Xiong, Weining; Wang, Cong Yi; Xu, Yongjian

doi:10.1038/mt.2016.36

Cited by 176 publications

(169 citation statements)

References 39 publications

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“…ER stress develops in airway cells in this model and is exacerbated by viral infection, and the UPR has been associated with the differentiation status of macrophages, and intrinsic ER stress within macrophages also occurs 16, 71, 75, 83, 84, 85, 86…”

Section: Oxidative and Er Stress In Chronic Inflammatory And Mucopurumentioning

confidence: 88%

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Oxidative and endoplasmic reticulum stress in respiratory disease

2018

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Oxidative stress and endoplasmic reticulum (ER) stress are related states that can occur in cells as part of normal physiology but occur frequently in diseases involving inflammation. In this article, we review recent findings relating to the role of oxidative and ER stress in the pathophysiology of acute and chronic nonmalignant diseases of the lung, including infections, cystic fibrosis, idiopathic pulmonary fibrosis and asthma. We also explore the potential of drugs targeting oxidative and ER stress pathways to alleviate disease.

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Section: Oxidative and Er Stress In Chronic Inflammatory And Mucopurumentioning

confidence: 88%

“…). Evidence for ER stress in human respiratory epithelial cells, particularly in type II pneumocytes, includes high expression of CHOP,71 activation of ATF6, XBP1 and ATF4 14. Activation of the UPR has been found in both inherited and sporadic IPF and associated with viral infection 13.…”

Section: Oxidative and Er Stress In Chronic Inflammatory And Mucopurumentioning

confidence: 99%

Oxidative and endoplasmic reticulum stress in respiratory disease

2018

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“…Changes in proteostasis lead to an increase of nonfunctional proteins, accumulation of cytotoxic proteins, and/or aggregation of misfolded proteins. In IPF lungs, evidence of altered proteostasis has been found at different levels, including protein misfolding, markers of ER stress (99)(100)(101)(102), defective autophagy, and impaired proteasome activity (103,104) (Table 4). For instance, familial pulmonary fibrosis is associated with several mutations in surfactant A and C genes (105)(106)(107)(108).…”

Section: Cellular Perturbations In the Ipf Lungmentioning

confidence: 99%

Mitochondria in the spotlight of aging and idiopathic pulmonary fibrosis

Mora¹,

Bueno²,

Rojas³

2017

Journal of Clinical Investigation

176

169

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One of the most remarkable medical accomplishments in the last century has been the increasing longevity of the human population. A decrease in birth rates, accompanied by a reduction in mortality among the elderly population, has collectively increased the percentage of the aged population, particularly in developed countries. Globally, it is estimated that the proportion of the population over the age of 60 will increase from 11% to 22% by 2050, and 28% by 2100. Currently, 18% of the US population is over 60 years of age (57 million), which is predicted to rise to 27% (107 million) in 2050 and up to 31% (149 million) by 2100 (1). The aging population has propelled an increase in the overall prevalence of chronic conditions. Several lung diseases, including acute lung injury and asthma, and some infectious diseases, such as pneumonia, increase in severity and mortality with age. Additionally, there has been a significant increase in incidence of chronic lung diseases -including chronic obstructive pulmonary disease, most forms of lung cancer, and idiopathic pulmonary fibrosis (IPF) -resulting in aging-related increases in prevalence.IPF is the most common form of idiopathic interstitial lung diseases. Its overall incidence in the US is 7 to 17 per 100,000 persons with a prevalence between 13.2 and 63 per 100,000 persons (2). A 1996 study initially demonstrated a higher incidence and prevalence of IPF in patients over 65 (3). These observations were confirmed more recently by Raghu et al. (4) and others, using both broad and narrow case-finding criteria for IPF diagnosis. These studies estimated that in the US, the prevalence of IPF increases with age, ranging from 4 per 100,000 for population aged between 18 and 34 years old to 227.2 per 100,000 among those 75 or older (4). This aging-related increase in cumulative incidence and prevalence of IPF has been corroborated by several studies that include populations in Europe and Asia (5-9). Accordingly, the median age at diagnosis of sporadic IPF ranges between 50 and 85 years old, and patients younger than 50 are more commonly associated with familial, rather than sporadic, forms of the disease (2). Mortality rates from IPF are steadily increasing worldwide, and a positive association has also been observed with advanced age (10). Examination of US government health insurance data for people aged 65 and older shows an increasing prevalence of IPF among older age groups (11). These studies confirm the growing concern that aging, and consequently age-related diseases, will drive up health care expenditures. As the elderly population in developed countries is expected to double in the next 25 years, there is an urgent need to understand the pathogenesis of IPF and develop interventions to attenuate or reverse lung fibrosis. The physiology of aging and the lungEvolutionary theories of aging include the concept of selection shadow that permits the accumulation of mutations with late deleterious effects, and the theory of antagonistic pleiotropy, which supports the sele...

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“…Mutation of the COPA gene, which encodes a protein involved in Golgi-to-ER retrieval was found to cause autoimmune arthritis and pulmonary interstitial lung disease, but although UPR activation was detected in the lung epithelium the mutation caused a multisystem disorder of altered immune function [15]. In two separate studies, the UPR transcription factor CHOP has been identified as a potential driver of fibrosis [16,61]. Deletion of Chop in mice reduced alveolar epithelial apoptosis following bleomycin treatment, but in one of the studies adoptive transfer of wildtype macrophages restored normal levels of pulmonary fibrosis [16].…”

Section: Pulmonary Fibrosismentioning

confidence: 99%

“…In two separate studies, the UPR transcription factor CHOP has been identified as a potential driver of fibrosis [16,61]. Deletion of Chop in mice reduced alveolar epithelial apoptosis following bleomycin treatment, but in one of the studies adoptive transfer of wildtype macrophages restored normal levels of pulmonary fibrosis [16]. This suggests that modulation of the innate immune response by CHOP in the macrophage may play an important role, at least in the bleomycin model of fibrosis.…”

Section: Pulmonary Fibrosismentioning

confidence: 99%

Endoplasmic reticulum stress in lung disease

Marciniak

2017

Eur Respir Rev

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Exposure to inhaled pollutants, including fine particulates and cigarette smoke is a major cause of lung disease in Europe. While it is established that inhaled pollutants have devastating effects on the genome, it is now recognised that additional effects on protein folding also drive the development of lung disease. Protein misfolding in the endoplasmic reticulum affects the pathogenesis of many diseases, ranging from pulmonary fibrosis to cancer. It is therefore important to understand how cells respond to endoplasmic reticulum stress and how this affects pulmonary tissues in disease. These insights may offer opportunities to manipulate such endoplasmic reticulum stress pathways and thereby cure lung disease.

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Chop Deficiency Protects Mice Against Bleomycin-induced Pulmonary Fibrosis by Attenuating M2 Macrophage Production

Cited by 176 publications

References 39 publications

Oxidative and endoplasmic reticulum stress in respiratory disease

Oxidative and endoplasmic reticulum stress in respiratory disease

Mitochondria in the spotlight of aging and idiopathic pulmonary fibrosis

Endoplasmic reticulum stress in lung disease

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