Lipocalin 2: An Emerging Player in Iron Homeostasis and Inflammation

Xiao, Xia; Yeoh, Beng San

doi:10.1146/annurev-nutr-071816-064559

Cited by 243 publications

(191 citation statements)

References 200 publications

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“…The higher levels of plasma lipocalin-2 seen in preclinical AD are consistent with prior studies implicating lipocalin-2 in AD pathobiology [9,23]. Lipocalin-2 has been hypothesized to be an important modulator of inflammation, neurotoxicity, and brain iron homeostasis, which may all contribute directly to AD pathogenesis [7,8]. However, whether lipocalin-2 plays a significant role in AD pathogenesis is controversial.…”

Section: Discussionsupporting

confidence: 79%

“…Although experimental models support a direct role for central lipocalin-2 in various aspects of AD pathogenesis [9,23], the contribution, if any, of peripheral lipocalin-2 to AD pathogenesis is not clear. Because peripheral lipocalin-2 has been shown to cross the blood-brain barrier to modulate central pathways such as by activating hypothalamic neurons to decrease appetite [20], it is plausible for circu-lating lipocalin-2 to act on central processes involved early in AD pathogenesis including neuroinflammation, systemic metabolism, and brain iron homeostasis [7,8]. As there was a lack of association between plasma lipocalin-2 and BMI in our cohort, the results from our study do not support peripheral lipocalin-2 contributing to the early dysregulation of body weight seen in preclinical AD [6].…”

Section: Discussionmentioning

confidence: 99%

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Plasma lipocalin‐2 levels in the preclinical stage of Alzheimer's disease

Eruysal

Ravdin

Kamel

et al. 2019

Alz & Dem Diag Ass & Dis Mo

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Introduction Lipocalin‐2 is an acute‐phase protein with pleotropic functions that has been implicated in several diseases including Alzheimer's disease (AD). However, it is unknown if circulating lipocalin‐2 levels are altered in the preclinical stage of AD, where AD pathology has accumulated but cognition remains relatively intact. Methods In this cross‐sectional study, we used an immunoassay to measure plasma lipocalin‐2 levels in cognitively normal (Clinical Dementia Rating 0) elderly individuals. 38 of 156 subjects were classified as preclinical AD by cerebrospinal fluid criteria. Results Plasma lipocalin‐2 levels were higher in preclinical AD compared with control subjects and associated with cerebrospinal fluid amyloid‐beta42 levels but not cerebrospinal fluid tau or phosphorylated‐tau181 levels. Exploratory analyses revealed that plasma lipocalin‐2 was associated with executive function but not episodic memory. Discussion Collectively, these results raise the possibility that circulating lipocalin‐2 is involved early in AD pathogenesis and may represent an early blood biomarker of amyloid‐beta pathology.

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Section: Discussionsupporting

confidence: 79%

Section: Discussionmentioning

confidence: 99%

Plasma lipocalin‐2 levels in the preclinical stage of Alzheimer's disease

Eruysal

Ravdin

Kamel

et al. 2019

Alz & Dem Diag Ass & Dis Mo

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“…Gut microbiota‐derived ligands/metabolites are known to directly modulate inflammatory responses in liver‐residing cells, such as the synthesis of proinflammatory cytokines and acute‐phase reactants . LCN2, an iron‐sequestering antimicrobial peptide, is synthesized by the liver as an acute‐phase reactant . Microbe ligand recognition and inflammation upregulate the synthesis of LCN2 .…”

Section: Discussionmentioning

confidence: 99%

“…(79)(80)(81)(82)(83) LCN2, an iron-sequestering antimicrobial peptide, is synthesized by the liver as an acute-phase reactant. (117)(118)(119)(120)(121) Microbe ligand recognition and inflammation upregulate the synthesis of LCN2. (118)(119)(120)122) Central to the current investigation, findings that LCN2 is upregulated in the liver and serum, but not in the gut and skeletal tissues of MPF versus EF mice, demonstrate a novel immunoregulatory mechanism driven by SFB within the commensal gut microbiota.…”

Section: Discussionmentioning

confidence: 99%

Specific Commensal Bacterium Critically Regulates Gut Microbiota Osteoimmunomodulatory Actions During Normal Postpubertal Skeletal Growth and Maturation

et al. 2020

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The commensal gut microbiota critically regulates immunomodulatory processes that influence normal skeletal growth and maturation. However, the influence of specific microbes on commensal gut microbiota osteoimmunoregulatory actions is unknown. We have shown previously that the commensal gut microbiota enhances TH17/IL17A immune response effects in marrow and liver that have procatabolic/antianabolic actions in the skeleton. Segmented filamentous bacteria (SFB), a specific commensal gut bacterium within phylum Firmicutes, potently induces TH17/IL17A‐mediated immunity. The study purpose was to delineate the influence of SFB on commensal gut microbiota immunomodulatory actions regulating normal postpubertal skeletal development. Two murine models were utilized: SFB‐monoassociated mice versus germ‐free (GF) mice and specific‐pathogen‐free (SPF) mice +/− SFB. SFB colonization was validated by 16S rDNA analysis, and SFB‐induced TH17/IL17A immunity was confirmed by upregulation of Il17a in ileum and IL17A in serum. SFB‐colonized mice had an osteopenic trabecular bone phenotype, which was attributed to SFB actions suppressing osteoblastogenesis and enhancing osteoclastogenesis. Intriguingly, SFB‐colonized mice had increased expression of proinflammatory chemokines and acute‐phase reactants in the liver. Lipocalin‐2 (LCN2), an acute‐phase reactant and antimicrobial peptide, was substantially elevated in the liver and serum of SFB‐colonized mice, which supports the notion that SFB regulation of commensal gut microbiota osteoimmunomodulatory actions are mediated in part through a gut–liver–bone axis. Proinflammatory TH17 and TH1 cells were increased in liver‐draining lymph nodes of SFB‐colonized mice, which further substantiates that SFB osteoimmune‐response effects may be mediated through the liver. SFB‐induction of Il17a in the gut and Lcn2 in the liver resulted in increased circulating levels of IL17A and LCN2. Recognizing that IL17A and LCN2 support osteoclastogenesis/suppress osteoblastogenesis, SFB actions impairing postpubertal skeletal development appear to be mediated through immunomodulatory effects in both the gut and liver. This research reveals that specific microbes critically impact commensal gut microbiota immunomodulatory actions regulating normal postpubertal skeletal growth and maturation. © 2020 The Authors. JBMR Plus published by Wiley Periodicals, Inc. on behalf of American Society for Bone and Mineral Research.

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“…Lipocalin‐2 (LCN2), also known as neutrophil gelatinase‐associated lipocalin (NGAL; human ortholog of the mouse Lcn2 gene), is one of the most extensively investigated acute‐phase proteins because its levels are highly elevated (up to ∼6 μg/mL in the serum) under all inflammatory conditions including in liver disease . It is well documented that LCN2 plays a critical role in host defense against bacterial infection by sequestering iron‐containing siderophores .…”

mentioning

confidence: 99%