Effect of hypoxia on release of IL-1 and TNF by human alveolar macrophages.

Hempel, S. L.; Monick, Martha M.; Hunninghake, Gary W.

doi:10.1165/ajrcmb.14.2.8630267

Cited by 97 publications

(85 citation statements)

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“…Hypoxaemia per se modifies muscle mass through a sharp decline in protein synthesis so that oxygen supply can adapt to demand [18]. Hypoxaemia may also act through a release of pro-inflammatory cytokines [19]. An important factor related to nutritional depletion is the level of systemic inflammation [20,21].…”

Section: Discussionmentioning

confidence: 99%

Prevalence and consequences of nutritional depletion in lung transplant candidates

Schwebel

Pin²,

Barnoud³

et al. 2000

Eur Respir J

107

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Nutritional status was studied in lung transplant (LT) candidates. The hypotheses were that nutritional depletion was highly prevalent and lean body mass depletion was a risk factor for a higher mortality both before and after LT.Of 78 consecutive patients listed for LT, 16 (21%) died while on the waiting list, eight (10%) were alive awaiting LT, and 54 (69%) received a graft. Mean age was 42.3 4.4 (mean SD). Thirty-eight per cent had a diagnosis of bronchiectasis or cystic fibrosis (BRO/CF), 33% of emphysema, 20% of idiopathic pulmonary fibrosis (IPF) and 8% of primary pulmonary hypertension. Body mass index (BMI) was 20.4 4.3 kg . m 2 , weight was 87.9 16.6% of ideal body weight (IBW).Patients were classed into four nutritional groups according to IBW and creatinine height index (CHI): I: weight <90% IBW and CHI <60% of predicted (28% of cases); II: weight <90% IBW and CHI $60% (27%); III: weight $90% IBW and CHI <60% (17%); IV: weight $90% IBW and CHI $60% (28%). Overall, 72% were depleted corresponding to groups I, II and III. Lean body mass depletion occurred despite normal weight in 17% of the cases (group III). Subjects with BRO/CF were mostly in groups I, II, III whereas IPF were concentrated in group III. Lean body mass depletion was associated with more severe hypoxaemia, reduced 6-minute walking distance and a higher mortality while awaiting. After LT, duration of mechanical ventilation, time spent in intensive care unit (ICU) was related to initial body composition. Survival after LT was lowest in group III.To conclude, nutritional depletion in lung transplant candidates is highly prevalent and should be more precisely assessed with a special reference to lean body mass since it has specific consequences both while awaiting and after lung transplant. Attempts should be made to increase lean body mass before lung transplant. Eur Respir J 2000; 16: 1050±1055.

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Section: Discussionmentioning

confidence: 99%

Prevalence and consequences of nutritional depletion in lung transplant candidates

Schwebel

Pin²,

Barnoud³

et al. 2000

Eur Respir J

107

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“…Hypoxia-induced secretion of proinflammatory cytokines, TNF-a and IL-1, has been found in human alveolar macrophages, blood monocytes and human monocytic cell lines. [73][74][75] Since these proinflammatory cytokines can themselves stimulate VEGF production, 76,77 TNF-a and IL-1 may serve to perpetuate the proangiogenic cytokine milieu in hypoxic areas. Other notable cytokines that appear to be upregulated by hypoxic macrophages include macrophage inhibitory factor (MIF) a cytokine known to be involved in facilitating growth factor-induced tumor and endothelial cell proliferation; 78 and interleukin-18 binding protein, which is known to inactivate the angiostatic factor, interleukin-18.…”

Section: Tam Gene Expression In Response To Tumor Hypoxiamentioning

confidence: 99%

Macrophage migration and gene expression in response to tumor hypoxia

Murdoch

Lewis

2005

Intl Journal of Cancer

183

143

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Monocytes are recruited into tumors from the circulation along defined chemotactic gradients and they then differentiate into tumor-associated macrophages (TAMs). Recent evidence has shown that large numbers of TAMs are attracted to and retained in avascular and necrotic areas, where they are exposed to tumor hypoxia. At these sites, TAMs appear to undergo marked phenotypic changes with activation of hypoxia-inducible transcription factors, dramatically upregulating the expression of a large number of genes encoding mitogenic, proangiogenic and prometastatic cytokines and enzymes. As a consequence, high TAMs density has been correlated with increased tumor growth and angiogenesis in various tumor types. Since hypoxia is a hallmark feature of malignant tumors and hypoxic tumor cells are relatively resistant to radio-and chemotherapy, these areas have become a target for novel forms of anticancer therapy. These include hypoxiatargeted gene therapy in which macrophages are armed with therapeutic genes that are activated by hypoxia-responsive promoter elements. This restricts transgene expression to hypoxic areas, where the gene product is then released and acts on neighboring hypoxic tumor cells or proliferating blood vessels. In this way, the responses of macrophages to tumor hypoxia can be exploited to deliver potent antitumor agents to these poorly vascularized, and thus largely inaccessible, areas of tumors. ' 2005 Wiley-Liss, Inc.

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“…Individuals with sleep apnea show increased circulating markers of oxidative stress and inflammation (Montplaisir et al, 1992). In addition, hypoxia causes macrophages to elaborate proinflammatory cytokines, especially IL-1␤ (Hempel et al, 1996), and hypoxia boosts microglial expression of IL-1␤ (Kim et al, 2003).…”

Section: Introductionmentioning

confidence: 99%

Acute Hypoxia Activates the Neuroimmune System, Which Diabetes Exacerbates

Johnson¹,

O’Connor²,

Hartman³

et al. 2007

J. Neurosci.

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Acute hypoxia is experienced in an array of ailments and conditions, including asthma, chronic obstructive pulmonary disease, heart failure, sleep apnea, acute hypotension, and blast lung injury. Classically, infection activates the neuroimmune system, causing loss of interest in the social environment. We report that the non-infectious stimulus acute hypoxia triggers neuroimmune system activation (NSA), causing loss of interest in the social environment, and that recovery from hypoxia-induced NSA is impaired in a mouse model of type 2 diabetes. Importantly, recovery from the behavioral consequences of hypoxia-induced NSA was nearly ablated in MyD88 (myeloid differentiation factor 88) knock-out mice and in mice intracerebroventricularly administered the caspase-1 inhibitor ac-YVAD-CMK (ac-Tyr-Val-Asp-2,6-dimethylbenzoyloxymethylketone). Diabetic mice had prolonged recovery from NSA that could be halved by administration of subcutaneous interleukin-1 (IL-1) receptor antagonist (RA). These results show that acute hypoxia activates the IL-1␤ arm of the neuroimmune system, which diabetes exacerbates and treatment with IL-1RA ameliorates.

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Effect of hypoxia on release of IL-1 and TNF by human alveolar macrophages.

Cited by 97 publications

References 0 publications

Prevalence and consequences of nutritional depletion in lung transplant candidates

Prevalence and consequences of nutritional depletion in lung transplant candidates

Macrophage migration and gene expression in response to tumor hypoxia

Acute Hypoxia Activates the Neuroimmune System, Which Diabetes Exacerbates

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