The Lipid Mediator Protectin D1 Inhibits Influenza Virus Replication and Improves Severe Influenza

Morita, Masayuki; Kuba, Keiji; Ichikawa, Akihiko; Nakayama, Mizuho; Katahira, Jun; Iwamoto, Ryo; Watanebe, Tokiko; Sakabe, Saori; Daidoji, Tomo; Nakamura, Shota; Kadowaki, Ayumi; Ohto, Takayo; Nakanishi, Hiroki; Taguchi, Ryo; Nakaya, Takaaki; Murakami, Makoto; Yoneda, Yoshihiro; Arai, Hiroyuki; Kawaoka, Yoshihiro; Penninger, Josef; Arita, Makoto; Imai, Yumiko

doi:10.1016/j.cell.2013.02.027

Cited by 406 publications

(421 citation statements)

References 60 publications

Supporting

Mentioning

404

Contrasting

Unclassified

Order By: Relevance

“…Consistent with impaired peroxisomal ␤ -oxidation, we observed an enrichment in C26:0 but a decrease in C24:1 fatty acids in SPL species ( Fig. 1G ) (25)(26)(27); this provided further support for an important role of fatty acyl metabolism during infl uenza infection ( 15,16 ).…”

Section: D609 and Gw7647 Treatment Of Infl Uenza Virus-infected Cellssupporting

confidence: 58%

“…Host cell lipid metabolism and plasma membrane microdomains are implicated in the biogenesis of virus envelopes. Several studies have dissected the lipid inventory of purifi ed infl uenza virions ( 9, 10 ), whereas others have demonstrated the requirements for de novo fatty acid and sphingolipid biosynthesis and unique cholesterol compositions for virus production at budding sites (11)(12)(13)(14).In addition to the importance of host cell lipid metabolism for the biogenesis of infl uenza virus envelopes, recent fi ndings suggest a major role for soluble lipid mediators in antiviral responses against infl uenza virus infection in vivo ( 15,16 ). These soluble lipid mediators originate from membrane glycerophospholipids (GPLs) via phospholipase activity, and (to some extent), are metabolized in peroxisomes.…”

mentioning

confidence: 99%

“…In addition to the importance of host cell lipid metabolism for the biogenesis of infl uenza virus envelopes, recent fi ndings suggest a major role for soluble lipid mediators in antiviral responses against infl uenza virus infection in vivo ( 15,16 ). These soluble lipid mediators originate from membrane glycerophospholipids (GPLs) via phospholipase activity, and (to some extent), are metabolized in peroxisomes.…”

mentioning

confidence: 99%

“…These soluble lipid mediators originate from membrane glycerophospholipids (GPLs) via phospholipase activity, and (to some extent), are metabolized in peroxisomes. For example, ␤ -oxidation in the peroxisome is crucial for the retroconversion of DHA, the precursor of the lipid mediator protectin D1, which prevents nuclear export of infl uenza virus RNAs; protectin D1 production is directly inhibited by infl uenza virus ( 15 ). The role of peroxisomes during infl uenza virus replication is further evident by interaction between infl uenza virus nonstructural protein 1 (NS1) and multifunctional protein 2 (MFP2/HSD17B4), an antiviral protein essential for peroxisomal ␤ -oxidation ( 17 ).…”

mentioning

confidence: 99%

See 3 more Smart Citations

Lipidomics identifies a requirement for peroxisomal function during influenza virus replication

Tanner

Chng

Guan

et al. 2014

Journal of Lipid Research

View full text Add to dashboard Cite

for virus production. Host cell lipid metabolism and plasma membrane microdomains are implicated in the biogenesis of virus envelopes. Several studies have dissected the lipid inventory of purifi ed infl uenza virions ( 9, 10 ), whereas others have demonstrated the requirements for de novo fatty acid and sphingolipid biosynthesis and unique cholesterol compositions for virus production at budding sites (11)(12)(13)(14).In addition to the importance of host cell lipid metabolism for the biogenesis of infl uenza virus envelopes, recent fi ndings suggest a major role for soluble lipid mediators in antiviral responses against infl uenza virus infection in vivo ( 15,16 ). These soluble lipid mediators originate from membrane glycerophospholipids (GPLs) via phospholipase activity, and (to some extent), are metabolized in peroxisomes. For example, ␤ -oxidation in the peroxisome is crucial for the retroconversion of DHA, the precursor of the lipid mediator protectin D1, which prevents nuclear export of infl uenza virus RNAs; protectin D1 production is directly inhibited by infl uenza virus ( 15 ). The role of peroxisomes during infl uenza virus replication is further evident by interaction between infl uenza virus nonstructural protein 1 (NS1) and multifunctional protein 2 (MFP2/HSD17B4), an antiviral protein essential for peroxisomal ␤ -oxidation ( 17 ). Therefore, the collective literature indicates an apparent role for peroxisomes as the initial sites of antiviral signaling ( 18 ). Infl uenza viruses hijack host cell machineries for efficient replication and acquire a host-derived lipid envelope during budding. Recent systems-scale studies have primarily addressed the individual roles of genes ( 1-5 ) and proteins ( 6-8 ) in this process, yet have failed to illustrate how they function together to generate macromolecular precursors Abstract

show abstract

Section: D609 and Gw7647 Treatment Of Infl Uenza Virus-infected Cellssupporting

confidence: 58%

mentioning

confidence: 99%

mentioning

confidence: 99%

mentioning

confidence: 99%

See 2 more Smart Citations

Lipidomics identifies a requirement for peroxisomal function during influenza virus replication

Tanner

Chng

Guan

et al. 2014

Journal of Lipid Research

View full text Add to dashboard Cite

show abstract

“…Similarly, strategies that promote immune resolution or tissue regeneration, e.g. inhibitors of T-cell co-stimulators, resolvins, lipoxins, inhibitors of the CD200 receptor and immunomodulatory antibiotics or glitazones [93,99,[199][200][201] may accelerate regeneration in patients with severe disease. Further research is needed to identify cells and pathways that can be specifically targeted over the course of the infection and to develop clinically useful biomarkers that can identify the subset of patients in whom these targeted therapies will be most effective.…”

Section: Discussionmentioning

confidence: 99%

Influenza virus-induced lung injury: pathogenesis and implications for treatment

et al. 2015

View full text Add to dashboard Cite

The influenza viruses are some of the most important human pathogens, causing substantial seasonal and pandemic morbidity and mortality. In humans, infection of the lower respiratory tract of can result in flooding of the alveolar compartment, development of acute respiratory distress syndrome and death from respiratory failure. Influenza-mediated damage of the airway, alveolar epithelium and alveolar endothelium results from a combination of: 1) intrinsic viral pathogenicity, attributable to its tropism for host airway and alveolar epithelial cells; and 2) a robust host innate immune response, which, while contributing to viral clearance, can worsen the severity of lung injury. In this review, we summarise the molecular events at the virus-host interface during influenza virus infection, highlighting some of the important cellular responses. We discuss immune-mediated viral clearance, the mechanisms promoting or perpetuating lung injury, lung regeneration after influenza-induced injury, and recent advances in influenza prevention and therapy. @ERSpublications We discuss novel aspects of virus-and immune-mediated lung injury and repair after influenza infection

show abstract

Neuroprotectin/protectin D1 protects against neuropathic pain in mice after nerve trauma

Liu

Berta

et al. 2013

Annals of Neurology

107

127

View full text Add to dashboard Cite

Prevalence of neuropathic pain is high after major surgeries. However, effective treatment for preventing neuropathic pain is lacking. Here we report that peri-surgical treatment of Neuroprotectin D1/protectin D1 (NPD1/PD1), derived from docosahexaenoic acid, prevents nerve injury-induced mechanical allodynia and ongoing pain in mice. Intrathecal post-treatment of NPD1/PD1 also effectively reduces established neuropathic pain and produces no apparent signs of analgesic tolerance. Mechanistically, NPD1/PD1 treatment blocks nerve injury-induced long-term potentiation, glial reaction, inflammatory responses, and reverses synaptic plasticity in the spinal cord. Thus, NPD1/PD1 and related mimetics might serve as a new class of analgesics for preventing and treating neuropathic pain.

show abstract

The Lipid Mediator Protectin D1 Inhibits Influenza Virus Replication and Improves Severe Influenza

Cited by 406 publications

References 60 publications

Lipidomics identifies a requirement for peroxisomal function during influenza virus replication

Lipidomics identifies a requirement for peroxisomal function during influenza virus replication

Influenza virus-induced lung injury: pathogenesis and implications for treatment

Neuroprotectin/protectin D1 protects against neuropathic pain in mice after nerve trauma

Contact Info

Product

Resources

About